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Sickle cell trait skews common diabetes test – Reuters

February 8th, 2017 5:44 am

(Reuters Health) - A genetic trait that affects red blood cells and is fairly common among African Americans and Hispanic Americans can cause an important blood sugar test to miss signs of diabetes, researchers say.

The test known as hemoglobin A1c (HbA1c) estimates long-term blood sugar levels by measuring the amount of glucose sticking to red blood cells, but blood cells from people with sickle cell trait don't live as long, so they have less time to collect glucose.

When lead author Mary Elizabeth Lacy from Brown University School of Public Health in Providence, Rhode Island, and her colleagues used standard HbA1c cutoffs to screen for diabetes, we identified 40 percent fewer cases of prediabetes and 48 percent fewer cases of diabetes in individuals with sickle cell trait than in those without sickle cell trait, she told Reuters Health by email.

Sickle cell disease is a serious condition that occurs when a person has two copies of a defective gene responsible for making part of the hemoglobin molecule in red blood cells. Hemoglobin allows the cells to carry oxygen to the tissues that need it, but in people with two copies of the faulty gene, blood cells can turn sickle-shaped, causing painful crises and even death.

People with only one copy of the defective gene are said to have sickle cell trait, and most have no symptoms of sickle cell disease. The gene is most common among people with ancestry in sub-Saharan Africa, Central America and South America, Saudi Arabia, India, Turkey, Greece and Italy.

The U.S. Centers for Disease Control and Prevention estimates that 1 in 13 African American babies are born with sickle cell trait.

In their study of 4,620 African Americans, including 367 with sickle cell trait, Lacys team found that HbA1c levels were 0.3 percent lower in those with the trait than in those without it, even though they had similar blood sugar levels.

While 0.3 percent may seem small, Lacy said, a difference of 0.3 percentage points in HbA1c could be the difference between being identified as high-risk (and being targeted for more frequent monitoring as well as additional diabetes prevention efforts) or not, or receiving a diagnosis of diabetes or not.

Among individuals with no history of diabetes and not taking diabetes medications, testing blood sugar directly detected pre-diabetic elevated blood sugar levels or full-fledged diabetes in equal numbers of people, regardless of whether they had sickle cell trait, the researchers report in JAMA.

But if HbA1c was used instead of blood sugar testing, pre-diabetic elevated blood sugar would be diagnosed in about 29 percent of those with sickle cell trait compared to 49 percent of those without the trait. Similarly, the HbA1c test would identify diabetes in about 4 percent of those with sickle cell trait and about 7 percent of those without the trait.

The results of HbA1c testing need to be interpreted with caution in patients with sickle cell trait, Lacy concludes. These findings were based on one method of HbA1c measurement. While it is approved for use in those with sickle cell trait, we are unable to say whether our findings are due to assay interference or a biological phenomenon in those with sickle cell trait.

Doctors should consider using a glucose tolerance test if they suspect diabetes in people with SCT whose HbA1c is close to the cutoff level, said Dr. Anthony J. Bleyer from Wake Forest School of Medicine in Winston-Salem, North Carolina, who coauthored a related editorial.

I think there needs to be more research in this area. The HbA1c is a really important test that we use all the time. We need to make sure it is accurate for individuals of all races and ethnicities, Bleyer said by email.

Approximately 10 percent of African American patients have sickle cell trait. It is prudent to test African American patients for hemoglobinopathy (sickle cell trait) before relying on HbA1c for diagnosis diabetes/prediabetes and before using HbA1c to monitor blood sugar control, Dr. Kristina Behan from the University of West Florida in Pensacola, who was not involved in the study, said by email.

SOURCE: bit.ly/2ln3Rap and bit.ly/2kovj9m JAMA, online February 7, 2017.

The U.S. Food and Drug Administration has approved Amgen Inc's treatment for secondary hyperparathyroidism in adult patients with chronic kidney disease undergoing dialysis, the U.S. biotech company said on Tuesday.

WASHINGTON The U.S. Federal Trade Commission filed a complaint against Shire ViroPharma on Tuesday, accusing it of abusing government processes in order to fend off generic competition to its antibiotic Vancocin HCl, the agency said in a statement.

VATICAN CITY Beijing's top official on transplants said on Tuesday Beijing was "mending its ways" from a murky past when organs were taken from detained or executed prisoners.

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Cancer stem cell – Wikipedia

February 8th, 2017 5:42 am

Cancer stem cells (CSCs) are cancer cells (found within tumors or hematological cancers) that possess characteristics associated with normal stem cells, specifically the ability to give rise to all cell types found in a particular cancer sample. CSCs are therefore tumorigenic (tumor-forming), perhaps in contrast to other non-tumorigenic cancer cells. CSCs may generate tumors through the stem cell processes of self-renewal and differentiation into multiple cell types. Such cells are hypothesized to persist in tumors as a distinct population and cause relapse and metastasis by giving rise to new tumors. Therefore, development of specific therapies targeted at CSCs holds hope for improvement of survival and quality of life of cancer patients, especially for patients with metastatic disease.

Existing cancer treatments have mostly been developed based on animal models, where therapies able to promote tumor shrinkage were deemed effective. However, animals do not provide a complete model of human disease. In particular, in mice, whose life spans do not exceed two years, tumor relapse is difficult to study.

The efficacy of cancer treatments is, in the initial stages of testing, often measured by the ablation fraction of tumor mass (fractional kill). As CSCs form a small proportion of the tumor, this may not necessarily select for drugs that act specifically on the stem cells. The theory suggests that conventional chemotherapies kill differentiated or differentiating cells, which form the bulk of the tumor but do not generate new cells. A population of CSCs, which gave rise to it, could remain untouched and cause relapse.

Cancer stem cells were first identified by John Dick in acute myeloid leukemia in the late 1990s. Since the early 2000s they have been an intense cancer research focus.[1]

In different tumor subtypes, cells within the tumor population exhibit functional heterogeneity and tumors are formed from cells with various proliferative and differentiation capacities.[2] This functional heterogeneity among cancer cells has led to the creation of multiple propagation models to account for heterogeneity and differences in tumor-regenerative capacity: the cancer stem cell (CSC) and stochastic model.

The Cancer Stem Cell Model, also known as the Hierarchical Model proposes that tumors are hierarchically organized (CSCs lying at the apex[3] (Fig. 3).) Within the cancer population of the tumors there are cancer stem cells (CSC) that are tumorigenic cells and are biologically distinct from other subpopulations[4] They have two defining features: their long-term ability to self-renew and their capacity to differentiate into progeny that is non-tumorigenic but still contributes to the growth of the tumor. This model suggests that only certain subpopulations of cancer stem cells have the ability to drive the progression of cancer, meaning that there are specific (intrinsic) characteristics that can be identified and then targeted to destroy a tumor long-term without the need to battle the whole tumor [5]

In order for a cell to become cancerous it must undergo a significant number of alterations to its DNA sequence. This cell model suggests these mutations could occur to any cell in the body resulting in a cancer. Essentially this theory proposes that all cells have the ability to be tumorigenic making all tumor cells equipotent with the ability to self-renew or differentiate, leading to tumor heterogeneity while others can differentiate into non-CSCs [4][6] The cell's potential can be influenced by unpredicted genetic or epigenetic factors, resulting in phenotypically diverse cells in both the tumorigenic and non-tumorigenic cells that compose the tumor.[7]

These mutations could progressively accumulate and enhance the resistance and fitness of cells that allow them to outcompete other tumor cells, better known as the somatic evolution model.[4] The clonal evolution model, which occurs in both the CSC model and stochastic model, postulates that mutant tumor cells with a growth advantage outproliferate others. Cells in the dominant population have a similar potential for initiating tumor growth[8] (Fig. 4).

[9] These two models are not mutually exclusive, as CSCs themselves undergo clonal evolution. Thus, the secondary more dominant CSCs may emerge, if a mutation confers more aggressive properties[10] (Fig. 5).

A study in 2014 argues the gap between these two controversial models can be bridged by providing an alternative explanation of tumor heterogeneity. They demonstrate a model that includes aspects of both the Stochastic and CSC models.[6] They examined cancer stem cell plasticity in which cancer stem cells can transition between non-cancer stem cells (Non-CSC) and CSC via in situ supporting a more Stochastic model.[6][11] But the existence of both biologically distinct non-CSC and CSC populations supports a more CSC model, proposing that both models may play a vital role in tumor heterogeneity.[6]

The existence of CSCs is under debate, because many studies found no cells with their specific characteristics.[12] Cancer cells must be capable of continuous proliferation and self-renewal to retain the many mutations required for carcinogenesis and to sustain the growth of a tumor, since differentiated cells (constrained by the Hayflick Limit[13]) cannot divide indefinitely. If most tumor cells are endowed with stem cell properties, targeting tumor size directly is a valid strategy. If they are a small minority, targeting them may be more effective. Another debate is over the origin of CSCs - whether from disregulation of normal stem cells or from a more specialized population that acquired the ability to self-renew (which is related to the issue of stem cell plasticity).

The first conclusive evidence for CSCs came in 1997. Bonnet and Dick isolated a subpopulation of leukemia cells that expressed surface marker CD34, but not CD38.[14] The authors established that the CD34+/CD38 subpopulation is capable of initiating tumors in NOD/SCID mice that were histologically similar to the donor. The first evidence of a solid tumor cancer stem-like cell followed in 2002 with the discovery of a clonogenic, sphere-forming cell isolated and characterized from human brain gliomas. Human cortical glial tumors contain neural stem-like cells expressing astroglial and neuronal markers in vitro.[15]

In cancer research experiments, tumor cells are sometimes injected into an experimental animal to establish a tumor. Disease progression is then followed in time and novel drugs can be tested for their efficacy. Tumor formation requires thousands or tens of thousands of cells to be introduced. Classically, this was explained by poor methodology (i.e., the tumor cells lose their viability during transfer) or the critical importance of the microenvironment, the particular biochemical surroundings of the injected cells. Supporters of the CSC paradigm argue that only a small fraction of the injected cells, the CSCs, have the potential to generate a tumor. In human acute myeloid leukemia the frequency of these cells is less than 1 in 10,000.[14]

Further evidence comes from histology. Many tumors are heterogeneous and contain multiple cell types native to the host organ. Heterogeneity is commonly retained by tumor metastases. This suggests that the cell that produced them had the capacity to generate multiple cell types, a classical hallmark of stem cells.[14]

The existence of leukemia stem cells prompted research into other cancers. CSCs have recently been identified in several solid tumors, including:

Once the pathways to cancer are hypothesized, it is possible to develop predictive mathematical models,[33] e.g., based on the cell compartment method. For instance, the growths of abnormal cells can be denoted with specific mutation probabilities. Such a model predicted that repeated insult to mature cells increases the formation of abnormal progeny and the risk of cancer.[34] The clinical efficacy of such models[35] remains unestablished.

The origin of CSCs is an active research area. The answer may depend on the tumor type and phenotype. So far the hypothesis that tumors originate from a single "cell of origin" has not been demonstrated using the cancer stem cell model. This is because cancer stem cells are not present in end-stage tumors.

Origin hypotheses include mutants in developing stem or progenitor cells, mutants in adult stem cells or adult progenitor cells and mutant, differentiated cells that acquire stem-like attributes. These theories often focus on a tumor's "cell of origin".

The "mutation in stem cell niche populations during development" hypothesis claims that these developing stem populations are mutated and then reproduce so that the mutation is shared by many descendants. These daughter cells are much closer to becoming tumors and their numbers increase the chance of a cancerous mutation.[36]

Another theory associates adult stem cells (ASC) with tumor formation. This is most often associated with tissues with a high rate of cell turnover (such as the skin or gut). In these tissues, ASCs are candidates because of their frequent cell divisions (compared to most ASCs) in conjunction with the long lifespan of ASCs. This combination creates the ideal set of circumstances for mutations to accumulate: mutation accumulation is the primary factor that drives cancer initiation. Evidence shows that the association represents an actual phenomenon, although specific cancers have been linked to a specific cause.[37][38]

De-differentiation of mutated cells may create stem cell-like characteristics, suggesting that any cell might become a cancer stem cell. In other words, a fully differentiated cell undergoes several mutations that drive it back to a stem-like state.

The concept of tumor hierarchy claims that a tumor is a heterogeneous population of mutant cells, all of which share some mutations, but vary in specific phenotype. A tumor hosts several types of stem cells, one optimal to the specific environment and other less successful lines. These secondary lines may be more successful in other environments, allowing the tumor to adapt, including adaptation to therapeutic intervention. If correct, this concept impacts cancer stem cell-specific treatment regimes.[39] Such a hierarchy would complicate attempts to pinpoint the origin.

CSCs, now reported in most human tumors, are commonly identified and enriched using strategies for identifying normal stem cells that are similar across studies.[40] These procedures include fluorescence-activated cell sorting (FACS), with antibodies directed at cell-surface markers and functional approaches including side population assay or Aldefluor assay.[41] The CSC-enriched result is then implanted, at various doses, in immune-deficient mice to assess its tumor development capacity. This in vivo assay is called a limiting dilution assay. The tumor cell subsets that can initiate tumor development at low cell numbers are further tested for self-renewal capacity in serial tumor studies.[42]

CSC can also be identified by efflux of incorporated Hoechst dyes via multidrug resistance (MDR) and ATP-binding cassette (ABC) Transporters.[41]

Another approach is sphere-forming assays. Many normal stem cells such as hematopoietics or stem cells from tissues, under special culture conditions, form three-dimensional spheres that can differentiate. As with normal stem cells, the CSCs isolated from brain or prostate tumors also have the ability to form anchor-independent spheres.[43]

CSCs have been identified in various solid tumors. Markers specific for normal stem cells are commonly used for isolating CSCs from solid and hematological tumors. Cell surface markers have proved useful for isolation of CSC-enriched populations including CD133 (also known as PROM1), CD44, CD24, EpCAM (epithelial cell adhesion molecule, also known as epithelial specific antigen, ESA), THY1, ATP-binding cassette B5 (ABCB5),[44] and CD200.

CD133 (prominin 1) is a five-transmembrane domain glycoprotein expressed on CD34+ stem and progenitor cells, in endothelial precursors and fetal neural stem cells. It has been detected using its glycosylated epitope known as AC133.

EpCAM (epithelial cell adhesion molecule, ESA, TROP1) is hemophilic Ca2+-independent cell adhesion molecule expressed on the basolateral surface of most epithelial cells.

CD90 (THY1) is a glycosylphosphatidylinositol glycoprotein anchored in the plasma membrane and involved in signal transduction. It may also mediate adhesion between thymocytes and thymic stroma.

CD44 (PGP1) is an adhesion molecule that has pleiotropic roles in cell signaling, migration and homing. It has multiple isoforms, including CD44H, which exhibits high affinity for hyaluronate and CD44V which has metastatic properties.

CD24 (HSA) is a glycosylated glycosylphosphatidylinositol-anchored adhesion molecule, which has co-stimulatory role in B and T cells.

CD200 (OX-2) is a type 1 membrane glycoprotein, which delivers an inhibitory signal to immune cells including T cells, natural killer cells and macrophages.

ALDH is a ubiquitous aldehyde dehydrogenase family of enzymes, which catalyzes the oxidation of aromatic aldehydes to carboxyl acids. For instance, it has a role in conversion of retinol to retinoic acid, which is essential for survival.[45][46]

The first solid malignancy from which CSCs were isolated and identified was breast cancer and they are the most intensely studied. Breast CSCs have been enriched in CD44+CD24/low,[44] SP[47] and ALDH+ subpopulations.[48][49] Breast CSCs are apparently phenotypically diverse. CSC marker expression in breast cancer cells is apparently heterogeneous and breast CSC populations vary across tumors.[50] Both CD44+CD24 and CD44+CD24+ cell populations are tumor initiating cells; however, CSC are most highly enriched using the marker profile CD44+CD49fhiCD133/2hi.[51]

CSCs have been reported in many brain tumors. Stem-like tumor cells have been identified using cell surface markers including CD133,[52] SSEA-1 (stage-specific embryonic antigen-1),[53]EGFR[54] and CD44.[55] The use of CD133 for identification of brain tumor stem-like cells may be problematic because tumorigenic cells are found in both CD133+ and CD133 cells in some gliomas and some CD133+ brain tumor cells may not possess tumor-initiating capacity.[54]

CSCs were reported in human colon cancer.[56] For their identification, cell surface markers such as CD133,[56] CD44[57] and ABCB5,[58] functional analysis including clonal analysis [59] and Aldefluor assay were used.[60] Using CD133 as a positive marker for colon CSCs generated conflicting results. The AC133 epitope, but not the CD133 protein, is specifically expressed in colon CSCs and its expression is lost upon differentiation.[61] In addition, CD44+ colon cancer cells and additional sub-fractionation of CD44+EpCAM+ cell population with CD166 enhance the success of tumor engraftments.[57]

Multiple CSCs have been reported in prostate,[62]lung and many other organs, including liver, pancreas, kidney or ovary.[45][63] In prostate cancer, the tumor-initiating cells have been identified in CD44+[64] cell subset as CD44+21+,[65] TRA-1-60+CD151+CD166+[66] or ALDH+[67] cell populations. Putative markers for lung CSCs have been reported, including CD133+,[68] ALDH+,[69] CD44+[70] and oncofetal protein 5T4+.[71]

Metastasis is the major cause of tumor lethality. However, not every tumor cell can metastasize. This potential depends on factors that determine growth, angiogenesis, invasion and other basic processes.

In epithelial tumors, the epithelial-mesenchymal transition (EMT) is considered to be a crucial event.[72] EMT and the reverse transition from mesenchymal to an epithelial phenotype (MET) are involved in embryonic development, which involves disruption of epithelial cell homeostasis and the acquisition of a migratory mesenchymal phenotype.[73] EMT appears to be controlled by canonical pathways such as WNT and transforming growth factor .[74]

EMT's important feature is the loss of membrane E-cadherin in adherens junctions, where -catenin may play a significant role. Translocation of -catenin from adherens junctions to the nucleus may lead to a loss of E-cadherin and subsequently to EMT. Nuclear -catenin apparently can directly, transcriptionally activate EMT-associated target genes, such as the E-cadherin gene repressor SLUG (also known as SNAI2).[75] Mechanical properties of the tumor microenvironment, such as hypoxia, can contribute to CSC survival and metastatic potential through stabilization of hypoxia inducible factors through interactions with ROS (reactive oxygen species).[76][77]

Tumor cells undergoing an EMT may be precursors for metastatic cancer cells, or even metastatic CSCs.[78] In the invasive edge of pancreatic carcinoma, a subset of CD133+CXCR4+ (receptor for CXCL12 chemokine also known as a SDF1 ligand) cells was defined. These cells exhibited significantly stronger migratory activity than their counterpart CD133+CXCR4 cells, but both showed similar tumor development capacity.[79] Moreover, inhibition of the CXCR4 receptor reduced metastatic potential without altering tumorigenic capacity.[80]

In breast cancer CD44+CD24/low cells are detectable in metastatic pleural effusions.[44] By contrast, an increased number of CD24+ cells have been identified in distant metastases in breast cancer patients.[81] It is possible that CD44+CD24/low cells initially metastasize and in the new site change their phenotype and undergo limited differentiation.[82] The two-phase expression pattern hypothesis proposes two forms of cancer stem cells - stationary (SCS) and mobile (MCS). SCS are embedded in tissue and persist in differentiated areas throughout tumor progression. MCS are located at the tumor-host interface. These cells are apparently derived from SCS through the acquisition of transient EMT (Figure 7).[83]

CSCs have implications for cancer therapy, including for disease identification, selective drug targets, prevention of metastasis and intervention strategies.

Somatic stem cells are naturally resistant to chemotherapeutic agents. They produce various pumps (such as MDR[citation needed]) that pump out drugs and DNA repair proteins. They have a slow rate of cell turnover (chemotherapeutic agents naturally target rapidly replicating cells).[citation needed] CSCs that develop from normal stem cells may also produce these proteins, which could increase their resistance towards chemotherapy. The surviving CSCs then repopulate the tumor, causing a relapse.[84]

Selectively targeting CSCs may allow treatment of aggressive, non-resectable tumors, as well as prevent metastasis and relapse.[84] The hypothesis suggests that upon CSC elimination, cancer could regress due to differentiation and/or cell death.[citation needed] The fraction of tumor cells that are CSCs and therefore need to be eliminated is unclear.[85]

Studies looked for specific markers[17] and for proteomic and genomic tumor signatures that distinguish CSCs from others.[86] In 2009, scientists identified the compound salinomycin, which selectively reduces the proportion of breast CSCs in mice by more than 100-fold relative to Paclitaxel, a commonly used chemotherapeutic agent.[87] Some types of cancer cells can survive treatment with salinomycin through autophagy,[88] whereby cells use acidic organelles such as lysosomes to degrade and recycle certain types of proteins. The use of autophagy inhibitors can kill cancer stem cells that survive by autophagy.[89]

The cell surface receptor interleukin-3 receptor-alpha (CD123) is overexpressed on CD34+CD38- leukemic stem cells (LSCs) in acute myelogenous leukemia (AML) but not on normal CD34+CD38- bone marrow cells.[90] Treating AML-engrafted NOD/SCID mice with a CD123-specific monoclonal antibody impaired LSCs homing to the bone marrow and reduced overall AML cell repopulation including the proportion of LSCs in secondary mouse recipients.[91]

A 2015 study packaged nanoparticles with miR-34a and ammonium bicarbonate and delivered them to prostate CSCs in a mouse model. Then they irradiated the area with near-infrared laser light. This caused the nanoparticles to swell three times or more in size bursting the endosomes and dispersing the RNA in the cell. miR-34a can lower the levels of CD44.[92][93]

The design of new drugs for targeting CSCs requires understanding the cellular mechanisms that regulate cell proliferation. The first advances in this area were made with hematopoietic stem cells (HSCs) and their transformed counterparts in leukemia, the disease for which the origin of CSCs is best understood. Stem cells of many organs share the same cellular pathways as leukemia-derived HSCs.

A normal stem cell may be transformed into a CSC through disregulation of the proliferation and differentiation pathways controlling it or by inducing oncoprotein activity.

The Polycomb group transcriptional repressor Bmi-1 was discovered as a common oncogene activated in lymphoma[94] and later shown to regulate HSCs.[95] The role of Bmi-1 has been illustrated in neural stem cells.[96] The pathway appears to be active in CSCs of pediatric brain tumors.[97]

The Notch pathway plays a role in controlling stem cell proliferation for several cell types including hematopoietic, neural and mammary[98] SCs. Components of this pathway have been proposed to act as oncogenes in mammary[99] and other tumors.

A branch of the Notch signaling pathway that involves the transcription factor Hes3 regulates a number of cultured cells with CSC characteristics obtained from glioblastoma patients.[100]

These developmental pathways are SC regulators.[101] Both Sonic hedgehog (SHH) and Wnt pathways are commonly hyperactivated in tumors and are necessary to sustain tumor growth. However, the Gli transcription factors that are regulated by SHH take their name from gliomas, where they are highly expressed. A degree of crosstalk exists between the two pathways and they are commonly activated together.[102] By contrast, in colon cancer hedgehog signalling appears to antagonise Wnt.[103]

Sonic hedgehog blockers are available, such as cyclopamine. A water-soluble cyclopamine may be more effective in cancer treatment. DMAPT, a water-soluble derivative of parthenolide, induces oxidative stress and inhibits NF-B signaling[104] for AML (leukemia) and possibly myeloma and prostate cancer. Telomerase is a study subject in CSC physiology.[105] GRN163L (Imetelstat) was recently started in trials to target myeloma stem cells.

Wnt signaling can become independent of regular stimuli, through mutations in downstream oncogenes and tumor suppressor genes that become permanently activated even though the normal receptor has not received a signal. -catenin binds to transcription factors such as the protein TCF4 and in combination the molecules activate the necessary genes. LF3 strongly inhibits this binding in vitro, in cell lines and reduced tumor growth in mouse models. It prevented replication and reduced their ability to migrate, all without affecting healthy cells. No cancer stem cells remained after treatment. The discovery was the product of "rational drug design", involving AlphaScreens and ELISA technologies.[106]

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Study: Strong link between sense of smell and death – wwlp.com

February 8th, 2017 5:42 am

wwlp.com
Study: Strong link between sense of smell and death
wwlp.com
Dr. Sprehe says the olfactory system depends on stem cell turnover and when it loses function, it could be a warning sign for degenerative diseases like Parkinson's, Alzheimer's, dementia, even certain viral illnesses. It appears to be a degeneration ...

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Three technologies improving quality of life for those with low vision, blindness – Bel Marra Health

February 8th, 2017 5:42 am

Home Eye Health Three technologies improving quality of life for those with low vision, blindness

February is National Low Vision Awareness Month, and the National Eye Institute is outlining five new technologies currently in development to make life for those with low vision or blindness easier.

Low vision is characterized by difficulty performing daily tasks even after receiving treatment in the form of glasses or contacts, medications, or surgery. The type of vision loss can vary based on the cause and can affect different aspects of an individuals life.

For example, the loss of peripheral vision may be due to glaucoma and can impact your ability to walk and drive, while central vision loss can occur because of age-related macular degeneration and make tasks like reading difficult. To help those living with low vision and blindness, researchers are currently developing technologies that can be used to make some of these tasks easier. Continue reading to learn more about these new innovations.

Co-Robotic Cane: A co-robotic cane is currently being developed by Dr. Chang Ye of the University of Arkansas, Little Rock to aid those with low vision in maneuvering indoors. There is existing GPS-based technology available to help people find a location, such as a building, but it isnt useful for finding and navigating specific rooms within a structure. The cane functions by providing feedback about the users environment, using a 3D camera and a motorized roller tip to drive the cane forward for the user to follow. The cane also stores preloaded floor plans that can be accessed through voice recognition, though Ye hopes to have the cane capable of downloading a buildings floor plans through Wi-Fi upon entry.

Robotic Glove: Dr. Ye is also working on a robotic glove to help the user locate and use small objects and doorknobs. The fingerless glove uses a camera and speech recognition to identify an object, then guides the hands movements through tactile prompts. For example, the user could say the word mug, and the glove would stimulate the nerves in the hand in a distinct pattern to guide their hand towards the mug and help them pick it up correctly.

Low vision and blindness affect 4.1 million Americans, and these new technologies are just three of the many in the works to help them accomplished daily tasks safely. While these tools require further testing and development, they provide hope that tasks such as crossing the road, navigating a room, and opening a door will be able to be accomplished much quicker by those affected by low vision and blindness.

Related: Natural ways to improve night vision (night blindness)

Related Reading:

Night blindness (nyctalopia) treatment: Options to improve night vision

Red bloodshot eyes: Causes and cures

https://nei.nih.gov/news/briefs/five-innovations-harness-new-technologies-people-visual-impairment-blindness

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Will Biotechnology Regulations Squelch Food and Farming Innovation? – Genetic Literacy Project

February 8th, 2017 5:41 am

Jon Entine, Executive Director, Genetic Literacy Project,oversaw the assignments and the editing of this series

INTRODUCTION:

Genetically engineered crops and animals (GMOs) have been a controversial public issue since the first products were introduced in the 1990s. They have posed unique challenges for governments to regulate. Although most working scientists in the field hold the opinion that genetic engineering, for the most part, is part of a continuum of the human manipulation of our food supply thats gone on for thousands of years, critics contend differently.

Many crop biotechnology skeptics frame their concerns in quasi-religious terms, as a violation of nature or fears that the increased use of GE foods will lead to a corporate takeover of our seed and food systems, and the adoption of an ecologically destructive industrialized agriculture system. GMOs have become a symbol of the battle over what our global, regional and local food systems should look like going forward.

The clout of the food movement that vocally rejects many aspects of conventional farming has exponentially increased since then, promoted by mainstream journalists, scientists and non-profit groups from Michael Pollan to Consumers Union to the Environmental Working Group. Organic leaders and lobbyists, such as Gary Hirshberg, founder of Stonyfield Organics and Just Label It, openly demonize conventional food and farming in defiance of their commitments agreed to in the 1990s that organic food would not be promoted at the expense of conventional agriculture. Attempts to reign in the unchecked influence of the conventional food critics have repeatedly failed; over much of the past decade, theyve had a sympathetic ear in Washington. Partly in response to the prevailing winds, the USDA has evolved increasingly byzantine regulatory structures when it comes to new GE products.

The Genetic Literacy Project 10-part series Beyond the Science II (Beyond the Science I can be viewed here) commences with this introductory article. Leading scientists, journalists and social scientists explore the ramifications of genetic engineering and so-called new breeding technologies (NBTs), specifically gene-editing technologies such as CRISPR. We will post two articles each week, on Tuesday and Wednesday, over the next 5 weeks.

Regulation is at the heart of this ongoing debate. Many scientists and entrepreneurs have come to view the two key agencies regulating GE in the United States the Food and Drug Administration and Department of Agriculture as places where innovation goes to die. Thats an exaggeration, but not without some truth; regulations are inherently political, and the winds have been blowing against technological breakthroughs in agriculture for much of the last decade. On average, it takes upwards of $125 million and 7-10 years for the Agriculture Department to approve a trait, exhausting almost half of a new products 20-year patent protection. No wonder the agricultural sector is consolidating, and most new products are innovated by larger corporations.

The regulatory climate may be changing, perhaps radically, in the United States and possibly in the United Kingdom, as the result of recent elections.

Many of the old rules and regulations regulating GE crops were set up in the 1980s and early 1990s. They are arguably creaky, overly-restrictive and do not account for dramatic increases in our understanding of how genetic engineering works and the now clear consensus on their safety.

Now with NBTs, which are largely unregulated since the techniques were not foreseen 30 years ago when regulations were first formulated, agricultural genetic research is at an inflection point: Will governments make the same mistake that they did previously and regulate innovation almost out of existence, or will they incorporate reasonable risk-risk and risk-benefit calculations in evaluating which technological advances should proceed with limited regulations?

Decisions on these issues will shape not only food and farming in Europe, North America and the industrialized nations, but the food insecure developing world, which looks to the West for regulatory guidance.

Gene Editing and Animals

The second article in our series, by University of California animal geneticist Alison Van Eenennaam, addresses the challenges of regulating genetically engineered animals. She focuses on dehorned cows, which have been developed without gene editing over many years with, at times, less than optimal results. Should gene editing be evaluated on a case-by-case basis triggered by the novelty of the traits, or should the entire process be heavily regulated the general approach favored by the European Union in regulating more conventional genetic engineering?

Pesticide Debate: How Should Agricultural Chemicals Be Regulated to Encourage Sustainability?

Dave Walton, an Iowa farmer, discusses the brouhaha that has erupted in recent years over the use of glyphosate, the active ingredient in the weed killer originally developed under patent by Monsanto. Many GMO critics are now expressing concerns over pesticide use in conventional agriculture, using glyphosate as a proxy for attacking the technology. Are their concerns appropriate? Walton, who grows both GE and non-GE crops and is director of the Iowa Soybean Association, has used glyphosate on his farm since the introduction of herbicide resistant crops in 1996. He uses on average a soda-sized cup of glyphosate per acre, and the use of the herbicide has allowed him to switch from more toxic chemicals. Most strikingly he discusses the sustainability impact if a glyphosate ban is imposed, as many activists are calling for.

Plant pathologist Steve Savage challenges us to think in a more nuanced way about a popular belief that organic farming is ecologically superior to conventional agriculture. The Agricultural Department has been a fractious mess in recent years in its efforts to oversee and encourage new breeding technologies. When the Clinton administration oversaw the founding of the National Organics Standards Board in 1995, USDA officials extracted the commitment from organic industry that the alternative farming system would not be promoted at the expense of conventional agriculture. After all, study after study, then and now, has established that organic farming offers no safety nor clear ecological benefits.

Let me be clear about one thing, said former Secretary of Agriculture Dan Glickman in December 2000. The organic label is not a statement about food safety, nor is organic a value judgment about nutrition or quality.

But thats not whats happened.

Regulations and the NGO Problem in Africa and Asia

While GE crops were pioneered in the United States and embraced in other western coun- tries outside of Europe, there has been resistance in regions of the world where these innovations could arguably bring the most impact: Africa and poorer sections of Asia. Ma- haletchumy Arujanan, executive director of Malaysian Biotechnology Information Centre and editor-in-chief of The Petri Dish, the first science newspaper in Malaysia, takes on the emerging Asian food security crisis posed by a parallel rise in population and living (and food consumption) standards. She reviews the successes and failures in various countries, and the effective campaigns by anti-GMO NGOs, mostly European funded, to block further biotech innovation.

Margaret Karembu, director of International Service for the Acquisition of Agribiotech Applications, Africa regional office (ISSSA) AfriCenter based in Nairobi, has found a similar pattern of mostly European-funded NGOs attempting to sabotage research and spread misinformation about the basic science of crop biotechnology. Africa is the ultimate organic experiment, and farmers have failed miserably using family agro-ecology techniques for decades. Cracks are beginning to form in the anti-GMO wall erected across the continent and there are hopes that young people will be attracted to farming, lured by the introduction of GE crops and other innovations.

Public Opinion and GMOs

Brandon McFadden, assistant professor in the Food and Resource Economics Department, University of Florida, addresses the complex views of consumers regarding innovation and GE foods. The public has a widely distorted perception of what genetic engineering entails, which helps explain why consumers remain so skeptical about technological innovation in farming.

Julie Kelly, a contributing writer to numerous publications including the Wall Street Journal, National Review and the GLP, takes on Hollywood in her analysis of the celebrity embrace of the anti-GMO movement. Who are the movers and shakers manipulating public opinion in favor of the organic movement and against conventional agriculture? Is the celebrity-backed science misinformation campaign working?

Future of GM Research and How the Public Debate May Evolve

Paul Vincelli, extension professor and Provosts Distinguished Service Professor at the University of Kentucky, has been perturbed about the attack on independent university researchers for working with the biotechnology industry over the years. By law, land grant university scientists are required to work with all stakeholders, particularly corporations who are developing the products used by farmers, including organic farmers. No, scientists who partner with corporations in research and product development are not shills. He rejects the knee jerk belief, advanced by many activist critics of GE crops, that corporate funding necessarily corruptsscience and should be banned.

Finally, risk expert David Ropeik has an optimistic take on the future. He believes 2016 may have been a turning point in the debate over GE foods. Technology rejectionists, from Greenpeace to labeling activists, are sounding increasingly shrill and less scientific. Gene editing, he believes, could undercut claims that GE foods are unsafe because they are unnatural. He is convinced, perhaps optimistically, that GE opponents will soon be viewed as science denialists.

We will see.

Anti-GMO critics cite opinion polls and the votes of anti-GMO legislators in Europe and elsewhere as proof that genetic engineering should be curtailed and more heavily regulated. Thats a rickety platform if one believes in science, however; science is not a popularity contest.

The Genetic Literacy Project is a 501(c)(3) non profit dedicated to helping the public, journalists, policy makers and scientists better communicate the advances and ethical and technological challenges ushered in by the biotechnology and genetics revolution, addressing both human genetics and food and farming. We are one of two websites overseen by the Science Literacy Project; our sister site, the Epigenetics Literacy Project, addresses the challenges surrounding emerging data-rich technologies.Jon Entineis the founder of the Science Literacy Project.

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Insider Selling: Puma Biotechnology Inc (PBYI) Insider Sells … – Sports Perspectives

February 8th, 2017 5:41 am
Insider Selling: Puma Biotechnology Inc (PBYI) Insider Sells ...
Sports Perspectives
Puma Biotechnology Inc (NYSE:PBYI) insider Robert Charnas sold 3008 shares of the firm's stock in a transaction that occurred on Wednesday, February 1st.
Puma Biotechnology Inc Risk Points versus Health Care - CMLvizCML News
The Puma Biotechnology Inc (PBYI) Insider Sells $95744.64 in StockDailyQuint
Robert Charnas Sells 3008 Shares of Puma Biotechnology Inc (PBYI) StockCommunity Financial News

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‘Lifestyle is important in treating arthritis’ | Ahmedabad News – Times … – Times of India

February 8th, 2017 5:41 am

AHMEDABAD: City-based rheumatologist Dr Vishnu Sharma, at a press meet on Tuesday, spoke about an alarming increase in incidence of arthritis in people, especially younger people, and how a lack of awareness is causing health problems and deformities."There are as many as a hundred types of arthritis, of which more than 90% are curable if diagnosed on time. Some 80% to 90% of patients respond positively to treatment. We want to improve these results and hence want to raise awareness about rheumatology," Dr Sharma said. Dr Sharma then shed more light on 'inflammatory arthritis', the type more prevalent among young and middle-aged people. According to Dr Sharma, inflammatory arthritis has two causes, the first is a genetic tendency and the second is environmental factors like simple viral infections or physical and mental stress. About the influence of lifestyle on arthritis, Dr Sharma said: "Experts have found significant correlation between smoking and arthritis.Arthritis, conventionally a problem for old people and women, is increasing in male patients and the severity is greater in men who are frequent smokers." Dr Sharma said that as part of healthy lifestyle, the patient should have minimal stress levels, a high protein diet and should engage in exercise and yoga.

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What to Know About the Link Between Vitamin D and Psoriatic Arthritis – Health.com

February 8th, 2017 5:41 am

If you have psoriatic arthritis, you may have heard that people withthe conditionwhich causes painful, swollen, stiff jointsoften havelow levels ofvitamin D.In a 2015 study published in Arthritis Research & Therapy, researchers found that 40.9% of participants with psoriatic arthritis had a vitamin D deficiency, compared to 26.7% of control participants.Other autoimmune diseases have also been linked to low levels of the sunshine vitamin (so-called because the body produces vitamin D when it's exposed to sunlightyou can also get some vitamin Dfrom food, but sunshine is the main source). In the same study as above, 40.5% of rheumatoid arthritis patients were found to havea deficiency, as did 57.8% of psoriasis patients in earlier research from the British Journal of Dermatology.

Experts believe inflammation may have something to do with this.Autoimmune diseases like psoriatic arthritis and psoriasisinvolve an inflammation process,explainsWaseem Mir, MD, a rheumatologist at Lenox Hill Hospital in New York City."We think that inflammation causes a decrease in vitamin D," he told Health."[Its] not because [people] dont have enough vitamin D in their body, but theyre not processing it correctly."

It makes sense. The body needs vitamin D to absorb calcium. Both calcium and vitamin D work to promotehealthy bones, and vitamin D also seems to be involved in proper functioning of the immune system. And the bones and immune systemare both compromised in people who have psoriatic arthritis.

RELATED: 31 Ways to Manage Your Psoriatic Arthritis

Dr. Mir points out that there's been some research to suggest that vitamin D treatment may help ease joint pain in certain people with psoriatic arthritis. One such treatment is vitamin D supplements.If you have psoriatic arthritis, speak to your doctor about your vitamin D levels to find out if supplements are right for you.

Another treatment is phototherapy (careful exposure to ultraviolet rays), but there isn't enough research to recommend this for psoriatic arthritis patients.And although you can feel free to add morevitamin D-rich foods to your plate (think: fatty fish like salmon and tuna, certain kinds of mushrooms, and fortified milk) it's unlikely that you'd be able to reverse a true deficiency through diet alone.

In his own practice, Dr. Mir usually prescribes liquid vitamin D to patients, which he says helps get a better response.

"That is the most effective," he says. "A lot of it is absorbed through the mouth."

However, it is possible to get too much vitamin D, which can result in a build-up of calcium in the bloodand possibly lead to nausea, vomiting, and kidney problems.Speak to your doctor before adding any new supplements to your diet.

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Yes there’s hope, but treating spinal injuries with stem cells is not a … – The Conversation AU

February 7th, 2017 2:55 am

The Conversation AU
Yes there's hope, but treating spinal injuries with stem cells is not a ...
The Conversation AU
Claims that stem cell treatments can repair spinal injuries right now are overblown. But it's not for lack of trying, and the science is certainly progressing.

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Finding her way Student excels in goalball, life despite visual impairment – Daily Herald

February 7th, 2017 2:54 am

Elizabeth Chantry winds up the ball to throw as her two teammates flank her on either side, poised in their ready positions. As the three-pound goalball, which is much like a heavy basketball, shoots from Chantrys hands the bells embedded inside the ball ring out into the silence of the gym. The three players on the opposite end of the court dive with their arms and legs extended in an attempt to stop the rolling ball from passing their goal line. One opposing player, after stopping the ball, then stands and rolls it back at Elizabeth and her teammates in an attempt to score.

This goes on until time runs out and the team with the most goals wins. However theres one catch, none of the players can see a thing.

Goalball is a Paralympic sport for blind athletes. Though, its not the lack of eyesight that keeps the players from seeing, but rather the blacked-out eyeshades (essentially taped-over ski-goggles) that allows partially-sighted players and totally-blind players to play equally. Players navigate the court on their hands and knees by feeling strands of taped-over twine that outline the boundaries and positions for each of the players. Six hash marks in the lines allow players to orient themselves to make sure theyre in position and facing the correct way.

Despite playing without any vision, the game moves along in a quick and orderly fashion. Its a rhythm Elizabeth Chantry has become accustomed to through several years of playing.

Now a sophomore at Timpanogos High School, Elizabeth began playing goalball in fifth grade. She was hooked on the sport from the start.

As she put it simply with a laugh, Its really fun to throw a ball at people. I know that sounds really bad, but its satisfying to throw stuff at people and have it be OK.

Elizabeth was diagnosed with dominant optic nerve atrophy at four years old. The condition results in a breakdown in communication between the optic nerve and the brain, resulting in blindness. Elizabeth is legally blind, but still has some sight.

Like many things, eyesight is a spectrum. 20/20 vision is considered perfect eyesight, and anything below 20/200 vision is considered legally blind a person with perfect vision can see at 200 feet what a person with 20/200 vision can only make out at 20 feet. Elizabeth has approximately 20/400 vision.

I didnt really comprehend that I actually had a visual impairment, Elizabeth said. I knew it was there, I knew that I needed to do stuff, but I didnt really comprehend it until third grade.

Throughout Elizabeths schooling, she has had vision teachers. These teachers have helped her to learn effectively with her visual impairment. Elizabeth can read, but the letters need to be extremely close or especially large for her to make out each word.

Sometimes the print will be really small, or really annoying, or really cursive, and for that I have some magnifiers that I carry around with me that can make it bigger, she explained.

Despite these added challenges, Elizabeth doesnt feel disadvantaged or frustrated.

She just dives into it and is happy to try something new, so that makes it easy, said her mother, Jennifer Chantry.

Jennifer also has dominant optic nerve atrophy.

The condition is hereditary and affects each family member on Jennifers side of the family differently. Growing up with about 20/200 vision herself, Jennifer knew the sort of challenges her daughter would face. I think that since we had a good understand of what was going on that it made things easier, explained Jennifer.

My mom tells stories about when we were little and shed point out animals in the fields as we drove by, but she didnt realize we couldnt really see the animals, recounted Jennifer.

For a fifth grader working hard to overcome her visual impairment, goalball was a fun outlet.

As I got more and more into goalball, it was kind of a confidence boost, said Elizabeth. It was something I could do.

That winter in fifth grade began building Elizabeths devotion to the sport. I started to see it as a bigger thing. She said. I could get really good at it and I could like, do stuff that is cool.

Each year after that, she became more and more invested throughout the January through March season. At the end of the season when Elizabeth was in eighth grade, she was invited to join the state high school goalball team: the Utah Rage.

This accomplishment resulted in even more focused practices in the fall of her freshman year of high school to prepare for the winter season. It was pretty intense, simply stated her mother.

The Utah Rage took Elizabeth to her first national tournament that fall in Florida. The Utah Rage did so again this year, but this time earned a bronze medal, and Elizabeth was named one of six All-Americans in the girls division.

Aside from practicing the sport herself, Elizabeth also helps teach younger and less-experienced players how to play goalball.

Last year, I asked Elizabeth to come help me at goalball practices with the younger kids in Orem, said Jalayne Engberg, a teacher for the blind and visually impaired with Alpine School District.

With 23 years of goalball experience, Engberg explained, I have been doing coaching for a long time and the best thing I can do is find older goalball players to carry on the goalball sport in Utah.

Engberg and her colleague Tony Jepson have been instrumental in developing goalball in Utah. I am proud of Elizabeth for helping teach the sport to younger kids. She doesnt just teach it to visually impaired students, she shares it with her church youth group, too.

Elizabeths time spent on the court also yielded many new friends with similar visual impairments. Although, she has had no shortage of friends whether it be on a goalball court or at school (where she even plays flute in the schools band). Theres not a big difference between my friends at school and my friends at goalball, she explained.

Despite their visual shortcomings, goalball practice allows for everyone to make light of their lack of sight through their mutual experiences with visual impairments.

We make a ton of blind jokes, laughed Elizabeth. None of us can see, and so its kind of nice. Its like whats over there? I dont know, can anyone else tell? she recounted with more laughter.

The fun environment allows for players with visual impairments and their families to come together under a common bond. Its like a family in a lot of ways, Jennifer explained. You get to know other peoples kids, and other moms and dad, and its really kind of unique.

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Blind woman’s sight restored – St. Charbel’s relic brings slew of miraculous healings – Catholic Online

February 7th, 2017 2:54 am

'God gave me my vision back for a reason.'

Dafne Gutierrez was legally blind and doctors told her she would never see again. With help from St. Charbel, Gutierrez proved those doctors wrong.

Gutierrez prayed on the St. Charbel relic. Days later, her vision was restored.

LOS ANGELES, CA (Catholic Online) - Gutierrez struggled with several issues and was diagnosed with benign intracranial hypertension after losing sight in her right eye in 2012 and going completely blind in both eyes in November 2015.

A doctor diagnosed her with benign intracranial hypertension, a condition in which the brain and spinal cord suffer high pressure, leading to blindness, double-vision, pain in the neck and shoulders and ringing in the ears.

Gutierrez, only 31-years-old and mother of four, was shocked then devastated at the news.

According to WNCT, she said: "For me, I was like, 'Please God, let me see those faces again. Let me be their mother again.' Because I feel like [my kids] were watching me, taking care of me 24-7."

In January 2016, Gutierrez remained hopeful and full of faith. Her sister told her St. Charbel's relics would be at St. Joseph Maronite Catholic Church in Phoenix, AZ.

St. Charbel is a Lebanese monk who lived a Christian life and was surrounded by miraculous healings. When he died, his tomb was surrounded by a bright light for months and when it was opened, his body was discovered intact, sweating and bleeding.

He was sainted by the Roman Catholic Church and many near his grave were healed. Today, St. Charbel's relics continue to bring about a great number of miraculous healings.

Gutierrez's sister told her of St. Charbel's relics healing a blind boy in Mexico, which gave her hope. She went to the church for Sunday Mass and confessed to Father Wissam Akiki then prayed over the relics.

"I felt my body different," she recalled. Wanting more, she went to pray at the Saint's relic again the following Sunday, after Mass.

The Monday after her second visit, January 18, Gutierrez woke in pain.

"I was just wiping my eyes, and I'm like, 'They burn! They burn!"

Dr. Borik explained: "We took her to actually two other specialists to look at the eyes and see how we can explain this medically, and in fact there was really no medical explanation."

According to Daily Mail, Borik added Gutierrez's vision was 20/20 and there was no evidence of damage to her optic nerve.

"After this happened, the optic nerve looked completely normal, with no signs of damage or atrophy. there's nothing in the medical literature that anything like this has ever happened."

"God gave me my vision back for a reason," Gutierrez stated. "I want to be able to help others. I give testimony wherever I can because it's important for people to know that God does exist and he does hear us."

After news of Gutierrez's healing spread, Maronite Bishop A. Elias Zaidan wrote a newsletter, garnering even more attention:

"May this healing of the sight of Dafne be an inspiration for all of us to seek the spiritual sight, in order to recognize the will of God in our lives and to act accordingly."

To commemorate the miraculous healing, St. Joseph Maronite Church holds a special ceremony on the 18th of each month to honor St. Charbel.

Father Akiki reported hundreds have been flocking to the church from around the world.

St. Joseph Maronite Catholic Church is now constructing a shrine to St. Charbel across from its sanctuary. It will include a 3-ton stone statue from Lebanon and the entire structure should be done by March.

---

Pope Francis Prayer Intentions for FEBRUARY 2017 Comfort for the Afflicted. That all those who are afflicted, especially the poor, refugees, and marginalized, may find welcome and comfort in our communities.

By Kenya Sinclair (CALIFORNIA NETWORK)

Time and time again Pope Francis calls for Christian unity. Well, it was certainly unity that saved a 3-year-old girl from being crushed by a train in Qinghai, China. LOS ANGELES, CA (Catholic Online) - Different people have different interpretations of Pope Francis' ... continue reading

By Kenya Sinclair (CALIFORNIA NETWORK)

Dafne Gutierrez was legally blind and doctors told her she would never see again. With help from St. Charbel, Gutierrez proved those doctors wrong. LOS ANGELES, CA (Catholic Online) - Gutierrez struggled with several issues and was diagnosed with benign intracranial ... continue reading

By Kenya Sinclair (CALIFORNIA NETWORK)

The National Center on Sexual Exploitation (NCOSE) joined 25 other anti-sex trafficking organizations to create a Super Bowl-themed awareness campaign called #TackleDemand. LOS ANGELES, CA (Catholic Online) - The campaign is based on the idea sex trafficking wouldn't ... continue reading

By (CNA/EWTN News)

The Holy See and the Democratic Republic of the Congo on Friday signed a framework agreement to govern relations between the Catholic Church and the state. Kinshasa, Democratic Republic of Congo (CNA/EWTN News) - Cardinal Pietro Parolin, the Holy See's Secretary of ... continue reading

By (CNA/EWTN News)

On Sunday Pope Francis stressed the sanctity of life and encouraged Christians to fulfill Jesus Christ's command to be salt of the earth and light of the world. Vatican City, Italy (CNA/EWTN News) - "May no one be left alone and may love defend the sense of life," Pope ... continue reading

By Kenya Sinclair (CALIFORNIA NETWORK)

Pope Francis' February prayer intention video has been posted to YouTube. LOS ANGELES, CA (Catholic Online) - The 60-second video features Pope Francis' narration as scenes of society ignoring people in need are displayed. A young man shivers in the cold as people are ... continue reading

By Tony Magliano

What a sight! Over 25 times from the top of Capitol Hill in Washington, D.C., I have seen a sea of people marching to proclaim the dignity of unborn human life, and how death-dealing abortion sends the unholy message that some human beings are ... continue reading

By Kenya Sinclair (CALIFORNIA NETWORK)

Youth Pastor Eric Dill was at a Central High football game in Tennessee when a player was severely injured by a neck injury, leaving the teen in critical condition on the field for over half-an-hour. LOS ANGELES, CA (Catholic Online) - According to WRCBTV, Dill took a ... continue reading

By Elise Harris (CNA/EWTN News)

As the Patriots and the Falcons gear up for Super Bowl LI, Pope Francis sent a message to both players and viewers, saying the game is an opportunity to show solidarity and build virtue. Houston, TX (CNA/EWTN News) - "Great sporting events like today's Super Bowl are ... continue reading

By (CNA/EWTN News)

Pope Francis warned of the "hidden victims" of capitalism, the idolatry of money and false philanthropy, telling a Saturday gathering of entrepreneurs they must act to change a system that creates victims, not simply help people after the fact. Vatican City, Italy ... continue reading

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Love at first sight – win Free Laser Eye Surgery for you or your partner – Belfast Live

February 7th, 2017 2:54 am

See your loved one with 20:20 vision or give that special someone in your life the gift of perfect vision this Valentine's Day by entering to WIN FREE Laser Eye Surgery at Optilase Clinic.

Optilase Clinic are Europes Number One Eye Clinic, with Clinics situated throughout Northern Ireland in Belfast, Newry, L/Derry and Enniskillen.

Optilase Clinic are dedicated to providing the most innovative treatments, using only the latest technology to deliver exceptional results for our patients to ensure they can have freedom from glasses and contact lenses for the rest of their life.

Watch the short video below to hear from DJ Hix who recently had Laser Eye Surgery at Optilase.

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To be in with a chance of winning this fantastic prize, all you have to do is fill in your details and tell us how many hearts there are in the puzzle below, its that simple!

Also as an added bonus anyone who enters this competition and fills in all their details (*with the exception of the winner) will receive a voucher for 500 off laser eye surgery. Vouchers will be sent by email after the competition closes.

How many hearts are in the puzzle?

Terms and Conditions

Free draw open to UK and Republic of Ireland residents aged 18-65. Closing date for entries is 2pm on Monday, February 13 , 2017. Any entries after the closing date and time will not be counted. Strictly one entry per person. One winner will be selected from all correct answers to the competition question. The winners will be contacted by phone on Tuesday, February 14, 2017. Prize is as stated. No alternatives, cash or otherwise, will be offered. By entering this competition, you consent to being contacted by Trinity Mirror for marketing purposes. We will not share your details with any third party. The promoter of this competition is Optilase. This promotion is in no way sponsored, endorsed or administered by, or associated with, Facebook. Optilase T+C's apply.

Standard Belfast Live rules apply - see http://www.belfastlive.co.uk/rules/

Click here for Optilase full T+C's

For more information on treatments at Optilase Clinic or to book a Free Laser Eye Surgery Consultation visit http://www.optilase.co.uk

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Do you need help fighting diabetes? – whnt.com

February 7th, 2017 2:54 am

Please enable Javascript to watch this video

Some people, due to family history or other physical conditions, are dealt a bad hand and have to cope with diabetes.

But for many, diabetes is self-inflicted. We dont exercise or eat smart. After a few years of that, the grim reality is people go to a doctors appointment and find out they have blood sugar issues.

Huntsville Hospitals Diabetes University is program dedicated to helping patients not only navigate, but beat, diabetes.

Untreated, diabetes can lead to blindness, kidney disease, heart attack, and stroke. A serious issue with patients who have diabetes is infections with extremities that lead to amputations.

The focus of Diabetes University is help patients identify blood glucose levels, develop problem solving skills for diabetes, and how to prevent further damage from diabetes.

Also, the all-important portion control and exercise components are critical.

Fighting diabetes is a daily battle. It requires discipline and resolve. And you dont have to fight alone.

Huntsville Hospital Diabetes University is at 420 Lowell Drive, Suite 500 in Huntsville. The number is 256-265-3069.

34.721457 -86.575366

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Just One Weight-Lifting Session Can Do THIS for Diabetes – Reader’s Digest

February 7th, 2017 2:54 am

iStock/gilaxia

If you have diabetes, which affects over 29 million Americans and can lead to serious complications including stroke, cardiovascular disease, nerve damage, eye problems, and kidney disease, exercise is a powerful means of prevention. Obviously working out regularly is ideal, but if thats not feasible, not all is lost. A new study out of British Columbia shows that just one strength-training session delivers measurable benefits for people with Type 2 diabetes. In our study, a single set of lightweight leg exercises was able to improve blood vessel function, says Jonathan Little, senior author of the study and Assistant Professor at the University of British Columbia. The arteries were better able to dilate after exercise.

The study examined three groups: people with Type 2 diabetes, healthy non-exercisers, and healthy regular exercisers. All were asked to perform a 20-minute exercise routine, which included a warm-up and seven one-minute, high-intensity moves with a one-minute rest between each interval. The positive effects persisted for two hours, showing that there were immediate benefits to the cardiovascular system from doing a single weight workout, Little says.

Experts believe that fast-paced high-interval training workouts (HIIT), which have been getting super popular, can improve our blood pressure, cardiovascular health, and cholesterol levels, all while burning fat and toning muscle. Kettlebells and your own body weight are amazing tools, says Max Zeumer, New York Health & Racquet Club Personal Training Manager. Theyre easy to use and provide an array of exercise options.

Here is a quick lower body workout that you can adapt to your training level by upgrading weights as you progress. As with any exercise program, check with your doc first to make sure this workout is right for you.

As you begin to adapt to these exercises without any issues, you can add a set to the exercise, maxing out at three sets, and gradually increasing weight to progress.

If youre really focusing on improving blood flow, add in kettlebell swings as you advance. Add one minute to each exercise. Dont forget to take your time watch your form.

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‘Skinny Fat’ People Run a High Risk of Developing Diabetes – Paste Magazine

February 7th, 2017 2:54 am

Skinny fat people are those who look skinny based on outward appearance, but, because of their diet, have the same health concerns as someone who is overweight or obese. Put simply: thin on the outside, fat on the inside.

This phenomenon is incredibly dangerous, because the skinny fat person is deceived. He or she can easily think that his or her body is completely healthy because of its shape, when in reality its suffering just as harshly as if it were obese.

A study was conducted at the University of Florida in order to explore an explanation as to why nearly one third of slim Americans have prediabetes. Prediabetes is defined as the grey area between health and illness: it is the precursor stage during which blood sugar is abnormally highlevels above 5.7, according to the American Diabetes Associationbut not all of symptoms associated with full-blown diabetes are apparent.

Arch Mainous III, the studys lead investigator and the chair of health services research, management and policy in UFs College of Public Health and Health Professions, commented said that the researchers have found that a lot of people who we would consider to be at healthy weighttheyre notoverweightorobeseare not metabolically healthy.

The culprit? Researches hypothesize that it could be inactivity, alongside a poor diet.

Though there is no direct cause-and-effect relationship established as a result of the study, about a quarter of people tested who lived sedentary lifestyles met the criteria for prediabetes.

The grand takeaway from this is that we should not see our scales as the determinant of our health. High blood sugar is not something that a scale can detect. It is incredibly important to remain active, eat well and attend regular checkups during which you monitor your blood sugar to be sure your levels are healthy.

Photo: Alden Chadwick, CC-BY

Elizabeth Chambers is a health intern with Paste and a freelance writer based out of Athens, Georgia.

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LIFE AFTER DEATH? Scientists claim dying is ‘NOT like turning off a lightbulb’ – Express.co.uk

February 7th, 2017 2:52 am

GETTY

A new study claims life remains in the human body - even 48 hours after the person has been scientifically declared dead.

The Open Biology report said genetic activity actually increases after death - a bizarre discovery.

Senior author Peter Noble said: Not all cells are 'dead' when an organism dies. Different cell types have different life spans, generation times and resilience to extreme stress.

It is likely that some cells remain alive and are attempting to repair themselves, specifically stem cells.

Life is not simply extinguished after death, like a flame or lightbulb, but instead lives on in stages, like a computer slowly shutting down, the scientists said.

GETTY

Death is probably more like turning a computer off and much less like turning a light bulb of

Arne Traulsen

Arne Traulsen of the Max Planck Institute for Evolutionary Biology said: In spirit, death is probably more like turning a computer off and much less like turning a light bulb off.

Mr Nobles, of the University of Washington and Alabama State University, agreed with this interpretation.

He likened it to the Twin Towers collapsing floor by floor during the September 11 terror attacks in New York.

GETTY

He said: Like the Twin Towers on 9-11, we can get a lot of information on how a system collapses by studying the sequence of events as they unfold through time.

"In the case of the twin towers, we saw a systematic collapse of one floor at a time that affected the floors underneath it. This gives us an idea of the structural foundations supporting the building and we see a similar pattern in the shutdown of animals."

Death is a time-dependent process. We have framed our discussion of death in reference to 'postmortem time' because on the one hand, there is no reason to suspect that minutes after an animal dies, gene transcription will abruptly stop.

GETTY

On the other hand we know that within hours to days, the animal's body will eventually decompose by natural processes and gene transcription will end."

This was described by the reports authors as the twilight of death - when gene expression occurs but not all the cells are dead yet.

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Allergan pledges to battle blindness with ‘See America’ initiative – New York Business Journal

February 7th, 2017 2:51 am

New York Business Journal
Allergan pledges to battle blindness with 'See America' initiative
New York Business Journal
... blindness in the U.S.. The Dublin, Ireland-based company which has a U.S. headquarters in Parsippany, New Jersey is partnering with volunteer eye health and safety organization Prevent Blindness to champion better access to vision care.
Why You Should Get Your Eyes Checked NowOZY

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Bowling and blindness: White Cane Week kicks off in Regina – Globalnews.ca

February 7th, 2017 2:51 am

Visual impairment didnt stop the clatter of falling pins at Reginas Golden Mile Bowling Lanes Monday morning.

Members of the Canadian Council of the Blind (CCB) Regina chapter took on the citys media in five-pin bowling in a friendly competition to focus attention on blindness and visual impairment.

CCB spokesperson Russell Coubrough put together the 46th Annual Media Bowling Challenge to kick-off White Cane Week 2017, the national initiative that puts visual impairment into the spotlight.

This is our main event that we have, the Media Bowling Challenge to promote awareness, Coubrough said.

According to the Canadian National Institute for the Blind (CNIB), approximately half a million Canadians live with significant vision loss around 15,000 of them are in Saskatchewan. Those numbers are expected to increase as much as 30 per cent in the next decade due to an aging population.

Terry Parsons, partially blind and an avid bowler since 1972, participated in the challenge and said the public needs to be aware that while the visually impaired may do some things slower, they should be treated equally.

We do things a little differently than what you guys might do, but were still doing it and were getting the job done, he said.

Visually impaired bowler Darlene Smith also had a message. She often has to remind the public that her guide dog, Deidra, is for her use only and cant be pet on the street like most other dogs.

People get mad at you when you tell them to leave her alone, because they dont understand that shes working, Smith said.

In the friendly five-pin competition, the media managed to squeak by with a 135-115 victory.

White Cane Week runs from Feb 5 to Feb 11. Saskatchewan also has a team competing at the Canadian Vision Impaired Curling Championship in Ottawa.

2017Global News, a division of Corus Entertainment Inc.

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Bowling and blindness: White Cane Week kicks off in Regina - Globalnews.ca

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Beyond Bricks And Mortar: Reimagining Infrastructure Investment To Spur Biotechnology Innovation – Forbes

February 7th, 2017 2:51 am

Forbes
Beyond Bricks And Mortar: Reimagining Infrastructure Investment To Spur Biotechnology Innovation
Forbes
Biotechnology (including not only biopharmaceuticals, but also bioengineered food products, biofuels and biodefense mechanisms) is primed for an infusion of infrastructure investment. By supplementing existing tools with robotics, advanced computing ...

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Beyond Bricks And Mortar: Reimagining Infrastructure Investment To Spur Biotechnology Innovation - Forbes

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Animal Biotechnology Technologies, Markets and Companies 2017 – Research and Markets – Yahoo Finance

February 7th, 2017 2:51 am

DUBLIN--(BUSINESS WIRE)--

Research and Markets has announced the addition of Jain PharmaBiotech's new report "Animal Biotechnology - Technologies, Markets and Companies" to their offering.

This report describes and evaluates animal biotechnology and its application in veterinary medicine and pharmaceuticals as well as improvement in food production. Knowledge of animal genetics is important in the application of biotechnology to manage genetic disorders and improve animal breeding. Genomics, proteomics and bioinformatics are also being applied to animal biotechnology.

Transgenic technologies are used for improving milk production and the meat in farm animals as well as for creating models of human diseases. Transgenic animals are used for the production of proteins for human medical use. Biotechnology is applied to facilitate xenotransplantation from animals to humans. Genetic engineering is done in farm animals and nuclear transfer technology has become an important and preferred method for cloning animals. There is discussion of in vitro meat production by culture.

Biotechnology has potential applications in the management of several animal diseases such as foot-and-mouth disease, classical swine fever, avian flu and bovine spongiform encephalopathy. The most important biotechnology-based products consist of vaccines, particularly genetically engineered or DNA vaccines. Gene therapy for diseases of pet animals is a fast developing area because many of the technologies used in clinical trials humans were developed in animals and many of the diseases of cats and dogs are similar to those in humans.RNA interference technology is now being applied for research in veterinary medicine.

Molecular diagnosis is assuming an important place in veterinary practice. Polymerase chain reaction and its modifications are considered to be important. Fluorescent in situ hybridization and enzyme-linked immunosorbent assays are also widely used. Newer biochip-based technologies and biosensors are also finding their way in veterinary diagnostics.

Biotechnology products are approved by the Center for Veterinary Medicine of the FDA. Regulatory issues relevant to animal biotechnology are described.

Approximately 124 companies have been identified to be involved in animal biotechnology and are profiled in the report. These are a mix of animal healthcare companies and biotechnology companies. Top companies in this area are identified and ranked. Information is given about the research activities of 11 veterinary and livestock research institutes. Important 108 collaborations in this area are shown.

Share of biotechnology-based products and services in 2015 is analyzed and the market is projected to 2025.

The text is supplemented with 35 tables and 5 figures.Selected 260 references from the literature are appended.

Key Topics Covered:

Executive Summary

1. Introduction to Animal Biotechnology

2. Application of Biotechnology in Animals

3. A Biotechnology Perspective of Animals Diseases

4. Molecular Diagnostics in Animals

5. Biotechnology-based Veterinary Medicine

6. Research in Animal Biotechnology

7. Animal Biotechnology Markets

8. Regulatory issues

9. Companies Involved in Animal Biotechnology

10. References

For more information about this report visit http://www.researchandmarkets.com/research/b9fmth/animal

View source version on businesswire.com: http://www.businesswire.com/news/home/20170203005322/en/

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Animal Biotechnology Technologies, Markets and Companies 2017 - Research and Markets - Yahoo Finance

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