San Francisco Giants and Halo Neuroscience Announce New Partnership – Yahoo Finance

SAN FRANCISCO, March, 29, 2017 /PRNewswire/ --The San Francisco Giants have partnered with Halo Neuroscience, a San Francisco-based company that develops neurotechnology to unlock human potential for both performance and medical applications.

The strength and conditioning staff for the Giants completed a successful proof-of-concept test of Halo Neuroscience's first product, Halo Sport, and measured accelerated gains in player performance. As a result, the Giants began to incorporate Halo Sport into the team's core training protocol.

"We are extremely excited to integrate Halo's neurostimulation technology into our core training regimen to improve and refine on-field player performance and athleticism," said Dave Groeschner, Head Athletic Trainer for the San Francisco Giants. "After testing the product internally, we've determined that incorporating Halo Sport 'Neuropriming' into our training programs produces measurable and significant results. "

The Giants first started working with Halo Neuroscience one year ago during the team's 2016 January Conditioning Camp in Phoenix, AZ. At this time, the team's coaches split top minor league prospects into two groupsone Halo and one control groupand then compared each group's progress across nine standard performance measures.

Training and testing lasted two weeks, during which all athletes completed the same program: twenty-minute warm-ups followed by sixty minutes or more of focused training to improve skill, speed, and power. Athletes in one group wore Halo Sport headsets during the 20-minute warm-up, whereas athletes in the other did not.

At the conclusion of the two-week period, the Halo Group saw the greatest improvements in speed workthe area most heavily emphasized during Neuropriming sessions with Halo Sport. In the 20-yard dash, for example, almost all the athletes tested demonstrated significant improvement after two weeks, versus athletes in the control group who only demonstrated modest improvement.

"Our goal with Halo was to improve our team's speed and explosiveness," said Geoff Head, Sports Science Specialist at the San Francisco Giants. "Overall, all players at camp showed general improvements in the testing parameters, but there was an additional increase in testing results in the players who used Halo Sport as compared to the players in the control groupespecially in the 20-yard dash."

As a result of these findings, the Giants will continue to implement Halo Sport to improve movement-based training for the athletes in the organization.

"As a San Francisco-based company, we are thrilled to be working with our hometown team. With the Giants' league-leading, innovation-based approach to player development, we were able to earn our way into their winning formula," said Dr. Daniel Chao, CEO and Co-Founder of Halo Neuroscience.

For more information about the San Francisco Giants' partnership with Halo Neuroscience, and to learn more about Halo Sport, please visit blog.haloneuro.com.

About Halo Neuroscience

Halo Neuroscience develops neurotechnology to unlock human potential for both performance and medical applications. The company's first product, Halo Sport, utilizes Neuropriming technology to accelerate the neurologic gains of strength and skill learning that result from athletic training. Halo is now used by teams and athletes from the military, Olympics, MLB, NBA, NHL, and NFL, in addition to thousands of other athletes, musicians, and gamers around the world.

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10x Genomics Launches New Immunology Kit for VDJ Analysis as It Eyes Translational Medicine Market – GenomeWeb

SAN FRANCISCO (GenomeWeb) 10x Genomics has launched a single-cell analysis kit for immune repertoire profiling. The first kit will begin shipping in April and will enable the analysis of the VDJ regions from human T cells, while a second kit that will be launched later in the second quarter will enable VDJ analysis of human B cells.

Also, in the second half of the year, the firm plans to enable the analysis of single immune cells from mice.

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Baby steps to forgiveness – Ashland Daily Tidings

By Charles "Al" Huth

There are people who want to forgive and cant. Others lack the desire to forgive the object of their grievance. Within the deep and long-held grievance is overwhelming emotional pain that has significantly impacted ones life.

In effect, this grievance becomes ones personal antagonist. This negative energy creates an obstacle for one to focus on their full potential possibilities. The pain of a deeply held grievance can be extremely difficult to overcome; therefore, forgiveness may be the only solution. It is easy to turn the lights on just flip the switch. But one cannot flip a magic switch and all is forgiven. However, there is a process one can entertain to forgive oneself and others. It takes a period of time to learn and absorb these steps, but the benefits are many.

The baby steps towards forgiveness include an understanding of the development of human interactions. If you can see that the general developmental pattern of human behavior applies to you as well as to others, then the door to forgiveness opens a little wider.

As a practical matter, hanging onto your grievance may be more harmful to you then to the object of your grievance. The person related to your grievance may not even be aware of your stress in this regard.

A proponent of humanistic psychology, Abraham Maslow, believed that everyone was born inherently good. However, when the path to their full potential was frustrated or blocked, they can become angry, fearful and/or destructive.

It is well known that we cannot walk in someone elses shoes. If one is dealing with someone who is demonstrating harmful behavior, empathy may be required. This is not to say that one should accept physical abuse. In general, most of our human behavior patterns were formed in childhood. Often these patterns of behavior and unique perspectives remain operative in adulthood.

In addition, acceptable behavior patterns in children may not be acceptable as a course of action in adults. As an extreme example: If one was told how much they were loved while somebody was beating on them, one would tend to have a strong, adverse reaction to the word love. Without knowing this persons background information, this extreme reaction would make little sense to others. Sometimes empathy is required when dealing with others that we do not know well. Making assumptions about others is a risky business. The chances of making a correct assumption may be less than 50 percent.

Most of us have regrets about our own past behavior. We relive past events and contemplate over and over again about what we could have done better. There are those who are less forgiving of themselves than of their family, friends and/or acquaintances. I believe that everyone strives to do the best that they can at their level of awareness. As humans, we strive to do better.

With lessons learned, our level of awareness increases our understanding of self and others. When we hang on to our past indiscretions and do not acknowledge our limited awareness at that time, we tend not to be forgiving of ourselves. Ultimately, this can be a heavy, unnecessary burden for us to carry around.

The act of forgiveness does not include condoning the actions of others. It is simply an acknowledgement that each of us has an awareness of our own reality.

Baby steps to forgiveness:

1) Recognize the impact of difficult situations on children raised in situations that are not conducive to becoming a well-adjusted adult.

2) Everyone is trying to do the best they can at their level of awareness. Everyone is not on identical levels of awareness.

3) Learn to forgive yourself. From birth to maturity, we are in a learning environment called the School of Life.

4) When situations are not completely understood, have empathy for others as well as yourself.

5) Accepting the concept of Oneness supports the idea that everyone is interconnected. Therefore, any thought or activity that separates us from others is conflicted with our natural way to be.

If you cant forgive yourself, it is very difficult (if not impossible) to forgive others!

Charles Al Huth, M.Ed., is the author of three books and numerous articles. He currently is teaching a class on human potential at OLLI/SOU. He lives in the Rogue Valley and is an inspirational speaker, teacher and magician. His website is http://JoyAl.org.

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Robo Madness 2017: The Photos and Takeaways – Xconomy

Third times a charm and our third annual Robo Madness conference in Boston had plenty of that. (So did the first two.) From live robot demos to provocative discussions on the opportunities and challenges in artificial intelligence, our speakers really delivered on this years theme: A.I. Gets Real.

Huge thanks to our host, Google, whose venue and support seem to get stronger every year. Special thanks to our event sponsors, who made it all possible: GE, Harmonic Drive, iRobot, Mitsubishi Electric Research Laboratories, Cirtronics, and TriNet. And, of course, thanks to our speakers, attendees, and demo organizers, who are what the event is really about.

Also, a big shout-out to Keith Spiro Photography for the pictures above.

Now, on to a few takeaways from the day:

1. Self-driving vehicles are at peak hype. There are huge opportunities at stake, but some of the biggest problems have yet to be solved: data sharing, liability, urban infrastructure, accounting for human behavior. Not to mention the technology needs to improve. On the plus side, the money flowing into the sector will benefit robotics as a whole. And incremental advances will continue to boost vehicle safety.

2. Data ownership is the key issue in machine learning. Weve heard this before, but big companies access to datasee Google, Amazon, Facebook, Uber, Teslagives them a huge leg up in A.I. applications. Theres not much new under the sun in terms of algorithms, so startups opportunities are largely determined by their datasets and team expertise.

3. Humans will need to communicate their goals to A.I. systems. In a world where machines can do more and more, people need to lay out guidelines for their behavior. This is especially important given that deep learning systems are getting harder for humans to understand and predict. Which leads to

4. Wed better think about jobs and ethics now. Robotics companies would rather address inefficiencies and labor shortages in fields like logistics, manufacturing, and delivery. But it seems likely that some (and perhaps many) human jobs will eventually become automated. How will business and policy leaders empower the human side of this evolving relationship? Stay tuned.

Xconomys Jeff Engel contributed to this report.

Gregory T. Huang is Xconomy's Deputy Editor, National IT Editor, and Editor of Xconomy Boston. E-mail him at gthuang [at] xconomy.com.

Gregory T. Huang is Xconomy's Deputy Editor, National IT Editor, and Editor of Xconomy Boston. E-mail him at gthuang [at] xconomy.com.

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Robo Madness 2017: The Photos and Takeaways - Xconomy

How You Remember This Weekend’s Hangover Will Depend Genetics – SheKnows.com

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Studies have shown many times over that people with a family history of alcoholism may be predisposed to be at a greater risk of developing drinking problems. But what if genetics also impacts how you remember hangovers? At Keele University, psychologist Dr. Richard Stephens looked into exactly that.

The National Institute on Alcohol Abuse and Alcoholism has reported that people with a family history are four times more likely to develop a drinking problem. Stephens based his research on that statistic, but focusing more on whether hangovers have some sort of impact on this.

More:Dispatches From High School: Teens on Drinking Alcohol

Stephens and his team conducted two studies to test this theory. His first study included 142 people, with a small portion of them having a family history of problem drinking, where he had them complete a survey about their hangovers in the past year. This study found that those with alcoholism in their family background recalled more frequent hangover symptoms than those who didnt have any family history of problem drinking.

His second study was designed in the same way, except the participants were asked about hangover symptoms the morning directly after a night of drinking. The results showed that there were no greater signs of hangover symptoms in the participants with a family history of alcoholism than in those who did not.

More:Alcohol Is Never an Excuse For Sexual Assault Period

While the findings may seem cloudy, Stephens is relatively positive toward his research. To him, it seemed that people who [were] predisposed to develop problem drinking are no more susceptible to developing a hangover however, we found that such people appear to remember their hangovers more lucidly.

So, while the amount of hangovers experienced did not change, the results showed that individuals who have a family history of problem drinking or alcoholism are more clearly able to remember their hangovers or what those hangovers felt like than those who do not have that kind of background. Stephens hopes that this information can be used to help curb excessive drinking and facilitate the means to create programs or plans for managing alcohol consumption.

More:My Spouse and I Quit Drinking and It Changed Our Relationship

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Embryology program training for teachers is April 18 – By Haywood … – The Mountaineer

By Haywood County Cooperative Extension | Mar 31, 2017

Haywood County 4-H will host the 4-H School Enrichment Embryology program training at 4 p.m. Tuesday, April 18, at the Haywood County Cooperative Extension Center, 589 Raccoon Road, Waynesville.

In the program, students incubate chicken eggs for 21 days and then watch baby chicks hatch. Students care for the chicks several days before the chicks are returned to a local farmer.

The curriculum training is a free opportunity open to teachers from public, private and homeschool groups. The teacher training will walk teachers through using the kits and curriculum developed by North Carolina State University.

The curriculum was developed to match the second grade Common Core and essential standards, learning about the life cycle of animals. The Embryology School Enrichment and teacher training can be used as continuing education units.

The 4-H school enrichment programs are offered at no-cost to teachers. 4-H school enrichment programs add a learn by doing experimental learning element to classrooms in Haywood County.

Call the Extension Center at 456-3575 to sign-up in advance.

The 4-H program is the youth education program of North Carolina Cooperative Extension, based at North Carolina State and North Carolina A&T State universities. More than 218,000 young people between the ages of 5 and 19 participate in North Carolina 4-H activities. 4-H is a community of young people across America who are developing leadership, citizenship, public speaking, decision-making, and life skills. 4-H is about having fun, learning, exploring and discovering. In 4-H, young people make new friends, develop new skills, become leaders and help shape their communities. Haywood County 4-H has numerous special interest programs, school enrichment programs, day camps, 4-H clubs, and opportunities for youth to learn while doing. For more information on the 4-H program in Haywood County please contact the Extension Center at 456-3575.

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Annual Ag Fair was a success – Bureau County Republican

In an effort to demonstrate to all the fourth-graders in Bureau County the importance of agriculture in their lives, the Bureau County Farm Bureau Womens Committee held its 23rd annual Ag Fair on March 23.

The Ag Fair is a day-long event at the Bureau County Fairgrounds in which students make timed stops (9 minutes at each station) to 14 different stations.

These stations range from dairy, embryology, safety, pork, corn, seed science, conservation, beef, soybeans, wheat, technology, equipment, large animals and small animals.

The Farm Bureau Womens Committee and the Bureau County Ag Coalition Committee originally started Ag Fair.

The Ag Coalition Committee consists of a member from each participating Ag Fair station.

This committee was originally formed to develop and oversee the goals set for the Ag Fair.

Over time, the Ag Coalition Committee has handed the organizing process over to the Womens Committee, where the chair and co-chair persons take the lead on final decision-making.

The Ag Coalition members then handle the planning of their individual presentations.

Each year the Ag Fair is evaluated.

Any considerations for changes come through observation of the event, teachers input from evaluation sheets and suggestions made by volunteers.

The committee begins the planning process about five months in advance of the Ag Fair each year.

The committee works with local businesses, farmers, county commodity groups, U of I Extension, the local FS and SWCD, as well as state commodity groups to make presentations at each station.

Volunteers are recruited, a total of 75, to serve as presenters, leaders of the classes, time keepers, bus directors, goodie bag distributors and several other jobs including set-up and clean-up workers.

The day prior to the fair, the presenters take time to set up their displays, and the set-up crew puts up tables, chairs and partitions at each station.

The day of the fair coffee, juice, doughnuts and lunch are served to all the presenters and volunteers.

Following the Ag Fair, each student was given a bag of goodies the committee put together which contains items donated by each of the presenters from coloring books to balloons and pencils.

The teachers were given an evaluation that will assist not only the committee, but also the presenters next year.

As a follow up, the committee is sponsoring a thank you card drive for all the volunteers for the event.

Students are encouraged to draw about their favorite part of the educational event.

A teacher attending past Ag Fair best sums up the event, Ag Fair is the best-kept secret in Bureau County.

This year more than 375 students from 20 classrooms attended the Ag Fair.

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Annual Ag Fair was a success - Bureau County Republican

Surge in sperm donors after P&J highlights issue – Press and Journal

A surge in sperm donor applicants has been reported by north-east health chiefs thanks, in part, to the Press and Journal.

At the beginning of last month, we reported that NHS Grampian had launched a fresh drive to recruit male donors, because stocks in the regions only centre were being rapidly depleted.

It was understood there had been little or no improvement since it emerged in a 2013 freedom of information request that only two men regularly attended the Aberdeen Fertility Centre, based at Aberdeen Maternity Hospital.

However, since the article appeared, more than 40 men have joined the initiative.

Hazel McBain, donor programme co-ordinator at Aberdeen Fertility Centre, said: Weve had a good level of extra interest and we are really grateful to the Press and Journal for helping raise awareness and to the readers who have come forward so far.

Every year, we see a decline in the number of donors, so we really hope campaigns like this will help stop that trend.

Weve had around 40 potential donors contact us recently which is simply fantastic and will be welcome news for couple hoping to conceive.

NHS chiefs are offering healthy men between 18 and 41 up to 350 for donations.

In November 2013, the Press and Journal reported that couples were facing delays of up to two years to start fertility treatment because of the ongoing lack of sperm and egg donors in the Aberdeen area.

It is thought much of the downturn in numbers was due to a controversial change in the law in 2005 which stripped men of their anonymity after a child turns 18.

The law means children conceived using donor eggs or sperm will be able to trace their biological parent if they choose to.

Ms McBain added that not everyone would be a successful applicant.

She said: We are bound by the Human Fertilisation and Embryology Authority regulations, so not everyone will meet the criteria.

That means we still really need men who are considering donating to come forward.

You can become a real hero by donating you are literally giving the gift of life. If you are unsure, have questions or want to have an informal chat about it, I would strongly encourage you to give us a ring at the Aberdeen Fertility Centre on 01224 553582.

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Ligand (biochemistry) – Wikipedia

In biochemistry and pharmacology, a ligand is a substance that forms a complex with a biomolecule to serve a biological purpose. In protein-ligand binding, the ligand is usually a molecule which produces a signal by binding to a site on a target protein. The binding typically results in a change of conformation of the target protein. In DNA-ligand binding studies, the ligand can be a small molecule, ion,[1] or protein[2] which binds to the DNA double helix. The relationship between ligand and binding partner is a function of charge, hydrophobicity, and molecular structure. The instance of binding occurs over an infinitesimal range of time and space, so the rate constant is usually a very small number.

Binding occurs by intermolecular forces, such as ionic bonds, hydrogen bonds and Van der Waals forces. The association of docking is actually reversible through dissociation. Measurably irreversible covalent bonding between a ligand and target molecule is atypical in biological systems. In contrast to the definition of ligand in metalorganic and inorganic chemistry, in biochemistry it is ambiguous whether the ligand generally binds at a metal site, as is the case in hemoglobin. In general, the interpretation of ligand is contextual with regards to what sort of binding has been observed. The etymology stems from ligare, which means 'to bind'.

Ligand binding to a receptor protein alters the chemical conformation by affecting the three-dimensional shape orientation. The conformation of a receptor protein composes the functional state. Ligands include substrates, inhibitors, activators, and neurotransmitters. The rate of binding is called affinity, and this measurement typifies a tendency or strength of the effect. Binding affinity is actualized not only by host-guest interactions, but also by solvent effects that can play a dominant, steric role which drives non-covalent binding in solution.[3] The solvent provides a chemical environment for the ligand and receptor to adapt, and thus accept or reject each other as partners.

Radioligands are radioisotope labeled compounds are used in vivo as tracers in PET studies and for in vitro binding studies.

The interaction of most ligands with their binding sites can be characterized in terms of a binding affinity. In general, high-affinity ligand binding results from greater intermolecular force between the ligand and its receptor while low-affinity ligand binding involves less intermolecular force between the ligand and its receptor. In general, high-affinity binding results in a higher degree of occupancy for the ligand at its receptor binding site than is the case for low-affinity binding; the residence time (lifetime of the receptor-ligand complex) does not correlate. High-affinity binding of ligands to receptors is often physiologically important when some of the binding energy can be used to cause a conformational change in the receptor, resulting in altered behavior of an associated ion channel or enzyme.

A ligand that can bind to a receptor, alter the function of the receptor, and trigger a physiological response is called an agonist for that receptor. Agonist binding to a receptor can be characterized both in terms of how much physiological response can be triggered and in terms of the concentration of the agonist that is required to produce the physiological response. High-affinity ligand binding implies that a relatively low concentration of a ligand is adequate to maximally occupy a ligand-binding site and trigger a physiological response. The lower the Ki concentration is, the more likely there will be a chemical reaction between the pending ion and the receptive antigen. Low-affinity binding (high Ki level) implies that a relatively high concentration of a ligand is required before the binding site is maximally occupied and the maximum physiological response to the ligand is achieved. In the example shown to the right, two different ligands bind to the same receptor binding site. Only one of the agonists shown can maximally stimulate the receptor and, thus, can be defined as a full agonist. An agonist that can only partially activate the physiological response is called a partial agonist. In this example, the concentration at which the full agonist (red curve) can half-maximally activate the receptor is about 5 x 109Molar (nM = nanomolar). Ligands that bind to a receptor but fail to activate the physiological response are receptor antagonists.

In the example shown to the left, ligand-binding curves are shown for two ligands with different binding affinities. Ligand binding is often characterized in terms of the concentration of ligand at which half of the receptor binding sites are occupied, known as the IC50, which is related to but different from the dissociation constant. The ligand illustrated by the red curve has a higher binding affinity and smaller Kd than the ligand illustrated by the green curve. If these two ligands were present at the same time, more of the higher-affinity ligand would be bound to the available receptor binding sites. This is how carbon monoxide can compete with oxygen in binding to hemoglobin, resulting in carbon monoxide poisoning.

Binding affinity is most commonly determined using a radiolabeled ligand, known as a tagged ligand. Homologous competitive binding experiments involve binding competition between a tagged ligand and an untagged ligand.[4] Non-labelled methods such as surface plasmon resonance, dual polarization interferometry and Multi-Parametric Surface Plasmon Resonance (MP-SPR) can not only quantify the affinity from concentration based assays; but also from the kinetics of association and dissociation, and in the later cases, the conformational change induced upon binding. MP-SPR also enables measurements in high saline dissociation buffers thanks to a unique optical setup. Microscale Thermophoresis (MST), an immobilization-free method[5] was developed. This method allows the determination of the binding affinity without any limitation to the ligand's molecular weight.[6]

For the use of statistical mechanics in a quantitative study of the ligand-receptor binding affinity, see the comprehensive article[7] on the configurational partition function.

Binding affinity data alone does not determine the overall potency of a drug. Potency is a result of the complex interplay of both the binding affinity and the ligand efficacy. Ligand efficacy refers to the ability of the ligand to produce a biological response upon binding to the target receptor and the quantitative magnitude of this response. This response may be as an agonist, antagonist, or inverse agonist, depending on the physiological response produced.[8]

Selective ligands have a tendency to bind to very limited kinds of receptor, whereas non-selective ligands bind to several types of receptors. This plays an important role in pharmacology, where drugs that are non-selective tend to have more adverse effects, because they bind to several other receptors in addition to the one generating the desired effect.

Bivalent ligands consist of two drug-like molecules (pharmacophores or ligands) connected by an inert linker. There are various kinds of bivalent ligands and are often classified based on what the pharmacophores target. Homobivalent ligands target two of the same receptor types. Heterobivalent ligands target two different receptor types. Bitopic ligands target an orthosteric binding sites and allosteric binding sites on the same receptor.

In scientific research, bivalent ligands have been used to study receptor dimers and to investigate their properties. This class of ligands was pioneered by Philip S. Portoghese and coworkers while studying the opioid receptor system.[9][10][11] Bivalent ligands were also reported early on by Micheal Conn and coworkers for the gonadotropin-releasing hormone receptor.[12][13] Since these early reports, there have been many bivalent ligands reported for various GPCR systems including cannabinoid,[14] serotonin,[15][16] oxytocin,[17] and melanocortin receptor systems.[18][19][20]

Bivalent ligands usually tend to be larger than their monovalent counterparts, and therefore, not drug-like. (See Lipinskis rule of five.) Many believe this limits their applicability in clinical settings.[21][22] In spite of these beliefs, their have been many ligands that have reported successful per-clinical animal studies.[19][23][24][25][26][27] Given that some bivalent ligands can have many advantages compared to their monovalent counterparts (such as tissue selectivity, increased binding affinity, and increased potency or efficacy), bivalents may offer some clinical advantages as well.

A privileged scaffold[28] is a molecular framework or chemical moiety that is statistically recurrent among known drugs or among a specific array of biologically active compounds. These privileged elements[29] can be used as a basis for designing new active biological compounds or compound libraries.

Main methods to study proteinligand interactions are principal hydrodynamic and calorimetric techniques, and principal spectroscopic and structural methods such as

Other techniques include: fluorescence intensity, bimolecular fluorescence complementation, FRET (fluorescent resonance energy transfer) / FRET quenching surface plasmon resonance, bio-layer interferometry, Coimmunopreciptation indirect ELIS, equilibrium dialysis, gel electrophoresis, far western blot, fluorescence polarization anisotropy, electron paramagnetic resonance, microscale thermophoresis

The dramatically increased computing power of supercomputers and personal computers has made it possible to study proteinligand interactions also by means of computational chemistry. For example, a worldwide grid of well over a million ordinary PCs was harnessed for cancer research in the project grid.org, which ended in April 2007. Grid.org has been succeeded by similar projects such as World Community Grid, Human Proteome Folding Project, Compute Against Cancer and Folding@Home.

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Ligand (biochemistry) - Wikipedia

RNA Biologist Kristen Lynch Appointed Chair of Department of Biochemistry and Biophysics at Penn – Newswise (press release)

Newswise PHILADELPHIA Kristen W. Lynch, PhD, has been appointed chair of the Department of Biochemistry and Biophysics, in the Perelman School of Medicine at the University of Pennsylvania, following eight years as a tenured faculty member in the department.

Dr. Lynch has a broad vision of the future of biochemistry and biophysics at Penn, said J. Larry Jameson, MD, PhD, executive vice president of the University of Pennsylvania for the Health System and dean of the Perelman School of Medicine. Her experience, talent, and collaborative spirit will foster strong ties among investigators within the department, as well as across Penn Medicine and the University. I am confident that under Dr. Lynchs leadership Penn will secure its place among the nations top biochemistry and biophysics departments.

Lynch, who is a professor of Biochemistry and Biophysics, also holds a secondary appointment in the department of Genetics and has expertise in RNA biology and immunology. Her laboratory focuses on understanding the biochemical mechanisms and regulatory networks that control alternative gene splicing in response to antigens. (Antigens are toxins and foreign substances, such as bacteria, viruses, and cells of transplanted organs, that stimulate the production of antibodies to protect an organism.)

Alternative splicing is a process in which a single gene codes for differentbut related forms of a given protein (called isoforms), each of which has similar functions. It eliminates the need for an organism to have large numbers of genes make distinctive proteins for carrying out similar functions throughout the body. Additionally, alternative splicing helps explain why humans have substantial genetic similarity with animals and insects, for example, yet such obvious physical and behavioral differences.

The Lynch laboratory specializes in understanding how alternative splicing is regulated in T cells when the cells are stimulated by an antigen during an immune response. Lynch and her team have identified more than 500 genes that undergo alternative splicing in response to T cell stimulation and have discovered some of the molecular mechanisms and signaling pathways that lead to this regulation.

She received her doctorate from Harvard University in 1996 and completed her postdoctoral training at the University of California, San Francisco. Lynch joined the Penn faculty as an associate professor in the department of Biochemistry and Biophysics in 2009, having been recruited from University of Texas Southwestern Medical Center, where she chaired the biological chemistry graduate program.

She is the author of more than 50 scientific papers in the leading journals in her field and the recipient of numerous awards and honors in recognition of her scientific achievements, including a National Science Foundation Career Award. Lynch founded and directs the campus-wide RNA Group, a central forum for investigators in and around Penn interested in RNA-related topics. Lynch has served as a director of the RNA Society, an international scientific organization; is an editor for Molecular and Cellular Biology; and has co-chaired several international meetings in the field of RNA processing.

Penn Medicine is one of the world's leading academic medical centers, dedicated to the related missions of medical education, biomedical research, and excellence in patient care. Penn Medicine consists of the Raymond and Ruth Perelman School of Medicine at the University of Pennsylvania (founded in 1765 as the nation's first medical school) and the University of Pennsylvania Health System, which together form a $5.3 billion enterprise.

The Perelman School of Medicine has been ranked among the top five medical schools in the United States for the past 18 years, according to U.S. News & World Report's survey of research-oriented medical schools. The School is consistently among the nation's top recipients of funding from the National Institutes of Health, with $373 million awarded in the 2015 fiscal year.

The University of Pennsylvania Health System's patient care facilities include: The Hospital of the University of Pennsylvania and Penn Presbyterian Medical Center -- which are recognized as one of the nation's top "Honor Roll" hospitals by U.S. News & World Report -- Chester County Hospital; Lancaster General Health; Penn Wissahickon Hospice; and Pennsylvania Hospital -- the nation's first hospital, founded in 1751. Additional affiliated inpatient care facilities and services throughout the Philadelphia region include Chestnut Hill Hospital and Good Shepherd Penn Partners, a partnership between Good Shepherd Rehabilitation Network and Penn Medicine.

Penn Medicine is committed to improving lives and health through a variety of community-based programs and activities. In fiscal year 2015, Penn Medicine provided $253.3 million to benefit our community.

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RNA Biologist Kristen Lynch Appointed Chair of Department of Biochemistry and Biophysics at Penn - Newswise (press release)