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Shoreline Biome to Launch New DNA Isolation Kit at Miami Winter Symposium 2020


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Shoreline Biome, a microbiome research company that develops tools for characterizing microbiome populations down to the strain level, today announced that the company will debut a novel new DNA isolation kit at the Miami Winter Symposium 2020, taking place January 26-29.

The new product, Shoreline Biome’s Rapid Prep kit, is a fast and easy-to-use kit designed for the efficient and unbiased isolation of high molecular weight (HMW) single-stranded DNA (ssDNA) in excess of 40KB from Gram-negative and Gram-positive bacterial and fungal cultures. The ssDNA output is ideal for downstream PCR applications targeting specific microbial, fungal, or mammalian genes of interest.

Additionally, the company will present a poster at the Symposium in collaboration with researchers from West Virginia University School of Medicine.

Shoreline Biome’s poster presentation, “Sustained Gut Dysbiosis Following Experimental Sepsis in Alzheimer’s Disease Transgenic Mice,” is scheduled for Monday, January 27, from 1:30–2:30 p.m. The poster presents research conducted by Allison L. Brichacek, Divine C. Nwafor, Dawn Gratalo, Mark D. Driscoll, and Candice M. Brown. The session will be presented by Brichacek, a student in Brown’s lab at West Virginia University School of Medicine.

Shoreline Biome will also be an exhibitor at the Symposium.

The Miami Winter Symposium 2020 will be held January 26–29, 2020, at the Hyatt Regency Miami in Miami, Fla. The symposium is dedicated to molecular mechanisms linking the microbiome and human health. It includes an international line-up of renowned speakers; award lectures by the “stars” of microbiome research; focused sessions on hot topics in microbiome research; the latest international research; and networking opportunities with key research teams from around the world. For more information about the Miami Winter Symposium 2020, visit miamiwintersymposium.com.

About Shoreline Biome:

Characterizing the human microbiome and analyzing its role in human health and disease are priority goals for researchers around the world. Shoreline Biome accelerates breakthroughs in microbiome research by developing transformative discovery tools that characterize microbiome populations down to the strain level. With Shoreline Biome products, all it takes is three easy steps: lyse, purify, and amplify. Shoreline Biome’s easy-to-use companion analysis software and comprehensive reference database enables straightforward strain-level identification and quantitation of all bacteria in the sample. To learn more, visit shorelinebiome.com.

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A Special Event on February 6th


We are delighted to bring together this talented panel to share their perspectives on the challenges of bringing genome editing from the laboratory to the bedside to educate and support the diverse population of gene and cell therapy companies in the greater Philadelphia region.

DelawareBio, a nonprofit trade organization with the mission of catalyzing growth in the state’s life-science industry, presents a panel discussion on gene editing that goes beyond CRISPR technology. To be held Thursday, February 6th from 1:30-5pm at the ChristianaCare John H. Ammon Medical Education Center, the event will provide an overview of the opportunities and challenges expected in bringing genome editing from the laboratory to the patient bedside.

As a leading biotech developer and center for pharma/life sciences research under the Greater Philadelphia ‘Cellicon Valley’ innovation hub, Delaware continues to play a leading role in the advancement of CRISPR technology.

The First State has the only gene-editing institute in the country embedded in a community cancer center, currently using CRISPR tech in lung cancer research. Delaware also can boast that the patent-pending computer code used to ‘translate’ the groundbreaking gene-editing technology was developed by a Newark Charter high school junior.

“Delaware is the health laboratory of the country,” said Eric Kmiec, PH.D., Director, Gene Editing Institute of the Helen F. Graham Cancer Center & Research Institute at ChristianaCare. “The state is a perfect testing ground because the population is representative of the general patient population across the county, a critical component of the development process. And the collaborative nature of our biotech industry allows for cross-pollination that would be more difficult elsewhere.”

Gene-Editing Technology Panel Discussion

DelawareBio, a nonprofit trade organization with the mission of catalyzing growth in the state’s life-science industry, is presenting a panel discussion on gene editing that goes beyond CRISPR technology. To be held Thursday, February 6th from 1:30-5pm at the ChristianaCare John H. Ammon Medical Education Center, the event will provide an overview of the opportunities and challenges expected in bringing genome editing from the laboratory to the patient bedside.

Registration is required. To sign up, visit delawarebio.org. Last day to register is Thursday, January 30th.

”We are delighted to bring together this talented panel to share their perspectives on the challenges of bringing genome editing from the laboratory to the bedside to educate and support the diverse population of gene and cell therapy companies in the greater Philadelphia region,” said DelawareBio President Helen Stimson.

Formed in early 2006 as Delaware BioScience Association, DelawareBio has brought together pharmaceutical and biotechnology firms, medical device manufacturers, agricultural biotech and chemical companies, research and testing companies, hospitals and medical institutions, and other organizations and related service companies, with the shared goal of expanding the state’s vibrant science economy.

Event Information

Attendees of the February 6th event will…

  • Hear from leading experts on the science behind genome editing and challenges in IP landscapes
  • Get an update on the latest genome editing discoveries and ChristianaCare’s CRISPR lung cancer research initiative
  • Learn what is happening at NIST to set industry standards, and about anticipated challenges from a public policy perspective
  • Gain a high-level overview on product development strategies to ensure plans are scientifically sound and meet regulatory expectations and clinical objectives.

Moderated by Maiken Scott, host of WHYY’s The Pulse, a national health and science radio show and podcast, panel members include Eric Kmiec, PH.D, Director, Gene Editing Institute of the Helen F. Graham Cancer Center & Research Institute at ChristianaCare; Samantha Maragh, PH.D., Leader, Genome Editing Program, NIST (National Institute of Standards and Technology); Maritza McIntyre, PH.D., President, Advanced Therapies Partners, LLC; Robert Oakes, Esquire, Principal, Fish & Richardson, and Cartier Esham, Executive Vice President, Emerging Companies, of Biotechnology Innovation Organization (BIO).

For further information, contact Jamie Pedrick, Marketing Manager, Delaware BioScience Association at jamie.pedrick@delawarebio.org or 302.635.0445.

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Rigaku to present latest Single Crystal and Powder X-ray Diffraction methods at FSU symposium


Rigaku XtaLAB mini II

Rigaku XtaLAB mini II Benchtop Single Crystal X-ray Diffractometer

Informative talks and poster sessions will take place on Friday; hands-on workshops will be held on Saturday, led by Rigaku Application Scientists.

Rigaku Corporation will present a workshop on X-ray analysis techniques at the 1st Annual Florida State University Rigaku Symposium and Workshop on X-ray Crystallography and Diffraction. The event, to be held in conjunction with the Florida State University Department of Chemistry and Biochemistry, will take place Friday and Saturday, January 24th and 25th, at the Chemical Sciences Laboratory at Florida State University in Tallahassee.

It will cover both single crystal and powder X-ray diffraction methods. Single crystal X-ray diffraction is used to determine the three dimensional structure of molecules. For materials that cannot be prepared as single crystals of appropriate size and quality for conventional single crystal diffraction studies, structure determination from powder diffraction data represents a viable approach for understanding the structural properties of the material of interest.

Informative talks and poster sessions will take place on Friday; hands-on workshops will be held on Saturday, led by Rigaku Application Scientists. Systems will include the Rigaku XtaLAB mini benchtop chemical crystallography system, with the latest version of CrysAlisPro single crystal X-ray diffraction data collection and processing software, and the new sixth generation Rigaku MiniFlex benchtop X-ray diffractometer. Also featured will be the Rigaku XtaLAB Synergy-S single or dual microfocus X-ray diffractometer for small molecule 3D structure analysis.

Registration information, along with a program itinerary and list of invited speakers is available from the Rigaku global website at http://www.rigaku.com/mailers/2020/fsu.

About Rigaku

Since its inception in Japan in 1951, Rigaku has been at the forefront of analytical and industrial instrumentation technology. Rigaku and its subsidiaries form a global group focused on general-purpose analytical instrumentation and the life sciences. With hundreds of major innovations to their credit, Rigaku companies are world leaders in X-ray spectrometry, diffraction, and optics, as well as small molecule and protein crystallography and semiconductor metrology. Today, Rigaku employs over 1,400 people in the manufacturing and support of its analytical equipment, which is used in more than 90 countries around the world supporting research, development, and quality assurance activities. Throughout the world, Rigaku continuously promotes partnerships, dialog, and innovation within the global scientific and industrial communities.

For further information, contact:

Michael Nelson

Rigaku Global Marketing Group

tel: +1 512-225-1796

michael.nelson@rigaku.com

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Genomenon’s Mastermind Continues to Outpace Qiagen’s HGMD Genetic Database


Mastermind vs HGMD. How they compare.

“We are world-renowned for the speed of our WGS (whole genome sequencing) interpretations, and using Mastermind has been a crucial step in accelerating our progress.” Shareef Nahas, Senior Director, Clinical Operations, Rady Children’s Institute for Genomic Medicine.

Genomenon® announced that over 175,000 recently documented genetic variants (DNA mutations) have been added to the Mastermind® Genomic Search Engine in the 4th quarter of 2019, for a cumulative total of more than 5.9 million genetic variants. This number reflects the rapidly accelerating pace of genomic discovery, and stands in stark contrast to the number manually curated by HGMD, the previous “gold standard” tool for variant interpretation: Qiagen added just under 11,700 variants in the HGMD Q4 2019 release, for a total of less than 276,000 genetic variants.

For many children and adults with rare diseases, definitive diagnosis is challenging due to the difficulty doctors face in connecting patient DNA with the scientific evidence found in the medical research describing the causative genetic variants. This limits the ability of doctors to diagnose and treat rare disease patients. The team at Genomenon created the Mastermind Genomic Search Engine to overcome this challenge.

Since Mastermind’s launch in 2017, the world’s top clinical laboratories and pharmaceutical companies have come to rely on Genomenon’s patented Artificial Intelligence processes to keep pace with the explosive growth of genomic research. Manual curation used for databases such as HGMD simply cannot scale, as demonstrated by the numbers above.

Rady Children’s Institute for Genomic Medicine, the organization that holds the world record for the fastest genetic diagnosis, uses Mastermind to ensure the most comprehensive and up-to-date information is available to doctors diagnosing and making treatment decisions for babies born with rare diseases.

“We are world-renowned for the speed of our WGS (whole genome sequencing) interpretations, and using Mastermind has been a crucial step in accelerating our progress.” said Shareef Nahas, Senior Director, Clinical Operations, Rady Children’s Institute for Genomic Medicine.

The stakes are high with variant interpretation, when lost time can mean lost lives. Ready access to the most comprehensive and updated information is essential. Below are some statistics that illustrate the challenge of finding this data.


  • PubMed (the U.S. government database of medical literature), which is limited to article titles and abstracts, contains less than 6.5% of all variants found across the medical literature. Variants found in PubMed tend to be the more “popular” variants that researchers mention in the publication title and abstract.
  • 69.5% of all variants are found only in the full text of medical articles – not in the title, abstract or supplemental material.
  • 25.7% of all variants are found in the supplemental data (additional materials provided with genetic literature by the authors) a quarter of which are identified only in the supplemental data.

Mastermind Genomic Search Engine has been integrated into many of the top clinical decision support platforms including Congenica, Fabric Genomics, and GenomOncology in order to provide their users access to the most comprehensive coverage of the genomic evidence needed to interpret variants. With more partner integrations in progress, Mastermind is providing the data needed to more quickly diagnose, treat, and cure rare diseases and cancer.

Mastermind Genomic Landscapes deliver a comprehensive view of genomic drivers of any disease to pharma and biopharma companies. Five of the top 25 pharma companies are using this data to inform their precision medicine development, deliver genomic biomarkers for clinical trial target selection, and support CDx regulatory submissions with empirical evidence.

About Genomenon

Genomenon connects patient DNA with the billions of dollars spent on research to help doctors diagnose and cure cancer patients and babies with rare diseases.

Our flagship product, the Mastermind Genomic Search Engine is used by hundreds of genetic labs worldwide to accelerate diagnosis, increase diagnostic yield and assure repeatability in reporting genetic testing results.

We license Mastermind Curated Genomic Datasets to pharmaceutical and bio-pharma companies to inform precision medicine development, deliver genomic biomarkers for clinical trial target selection, and support CDx regulatory submissions with empirical evidence.

For more information, visit Genomenon.com

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Microbial Discovery Group Appoints New Southern Midwest Industrial and Institutional Account Manager


Darrell Taylor

Darrell Taylor, Southern Midwest I&I Account Representative for Microbial Discovery Group

Having an experienced account manager, like Darrell, dedicated to this market will allow us to bring our partners sought-after solutions and support.

Microbial Discovery Group LLC (MDG) is pleased to announce the hiring of Darrell Taylor as Southern Midwest Region Industrial and Institutional (I&I) Account Manager. Darrell will focus on servicing MDG’s partners with strategic attention to the SporActiv™ product line.

Darrell brings over 30 years of sales experience working across multiple different market sectors such as; transportation, office products, and consumer electronics.

“From my first interactions with everyone, I knew there was something special happening here. Everyone I met made me feel at home. MDG is clearly driven by the desire to get the job done but the company also recognizes people are their greatest resource. To be a part of this environment is exciting!” stated Darrell.

“We are thrilled to have Darrell join our growing team. Over the past year, the I&I market has been a focus of MDG; having an experienced account manager, like Darrell, dedicated to this market will allow us to bring our partners sought-after solutions and support. We’re looking forward to the trusted relationships Darrell will build within this market,” added Jenna Trusso, Product Manager.

About Microbial Discovery Group

Microbial Discovery Group (MDG) is an R&D driven product development and Bacillus fermentation company. MDG has the capabilities to ensure success. When partnering with MDG, you can expect high quality, consistent Bacillus strain manufacturing delivered with efficiency and integrity. MDG is passionate about applying scientific principles to create indispensable solutions for our partners while working to Feed, Clean, and Save the World. For more information on Microbial Discovery Group, visit http://www2.mdgbio.com/DT2020.

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Global Team Enables Child With a Fatal Genetic Disease to Recover


A young boy with a rare genetic disease that typically kills within weeks of birth is now 3 years old and in remission thanks to a collaborative effort that included physicians at King Saud University Department of Pediatrics in Riyadh, Saudi Arabia, and immunologists at the Icahn School of Medicine at Mount Sinai in New York.

A report published in The New England Journal of Medicine today describes how the global team combined exceptional supportive clinical therapy, genetic diagnosis and a novel immunotherapeutic drug known as a protein kinase inhibitor to bring the Saudi Arabian boy into full remission from his deadly disease, known as “USP18 deficiency” because it is caused by a mutation of the USP18 gene.

“The teamwork between our two institutions and others around the world is a textbook case of science without borders,” says Dusan Bogunovic, PhD, Associate Professor of Microbiology, and Pediatrics, at the Icahn School of Medicine at Mount Sinai and co-corresponding author of the study. “We showed that even with a disease like USP18 deficiency, sound clinical care and timely drug administration can rescue patients from what was previously considered a death sentence.”

USP18 (ubiquitin-specific peptidase 18) is a protein coding gene involved in immune system. It is important to regulate inflammation driven by a substance that our body normally secretes to fight off viruses, type 1 interferons. Mutations of USP18 result in an uncontrolled response to type 1 interferons, triggering IFN-I-mediated inflammation that’s lethal in utero or shortly after birth. JAK1 inhibitor drugs, like ruxolitinib, the protein kinase inhibitor given to the Saudi Arabian boy, take over the intended role of USP18, and thus have the potential for a prompt and sustained recovery by patients.

Dr. Bogunovic and his lab, widely known for their work in the field of rare inflammatory diseases in children, first described USP18 deficiency in 2016. The following year, physicians at King Saud University reached out to Mount Sinai via Paris Descartes University in France about a gravely ill young patient in their intensive care unit who appeared to have a variant of the USP18 gene. Thus began a clinical/research collaboration—which included Paris Descartes University as well as Rockefeller University in New York—in which scientists characterized in detail the molecular basis of the disease through a battery of whole exome sequencing, expression assays, protein analysis, and antibody detection. “After seeing a potential variation in the USP18 gene, we conducted a complete set of tests to determine what it meant in terms of protein function,” explains Marta Martin-Fernandez, PhD, a postdoctoral fellow at the Icahn School of Medicine and a first author of the published study, who performed many of its biochemical and genetic analyses. “Those findings confirmed for us that ruxolitinib was the appropriate treatment.”

The young patient, who had been kept alive for months through the extraordinary care of physicians led by Fahad Alsohime, MD, Assistant Professor at the College of Medicine, King Saud University, was promptly put on oral, twice-daily doses of ruxolitinib. The dosage was increased after insufficient changes were seen, and within two weeks his symptoms began to rapidly improve, allowing doctors to wean him from respiratory support. Subsequent CT and MRI imaging showed a resolution of hemorrhaging, ischemia, cellulitis of the right forearm, and hydrocephalus, a condition in which cerebrospinal fluid accumulates in the brain. After two years of follow-up in an outpatient clinic in Riyadh, and continued administration of the JAK1 inhibitor, the child remains free of clinical problems and has been given an encouraging prognosis by his physicians. He will likely have to take ruxolitinib for the rest of his life.

The success of this case has provided a further springboard for Mount Sinai scientists to investigate the genomics and molecular/cellular biology behind conditions less severe than the boy’s. This ongoing work links to other studies that have shown that JAK inhibitors—which were initially developed as anti-cancer drugs but proved to be largely ineffective—can improve symptoms and control disease activity in patients with other type 1 interferon abnormalities.

“We were able to demonstrate the benefits of rapid genetic diagnosis of an inherited disorder for which an immunosuppressant drug like ruxolitinib can provide effective and sustained treatment,” says Dr. Bogunovic of Mount Sinai, a senior author on the publication. “That kind of discovery and drug repurposing must continue to be pursued by the scientific community without interruption.”

About the Mount Sinai Health System

The Mount Sinai Health System is New York City’s largest integrated delivery system, encompassing eight hospitals, a leading medical school, and a vast network of ambulatory practices throughout the greater New York region. Mount Sinai’s vision is to produce the safest care, the highest quality, the highest satisfaction, the best access and the best value of any health system in the nation. The Health System includes approximately 7,480 primary and specialty care physicians; 11 joint-venture ambulatory surgery centers; more than 410 ambulatory practices throughout the five boroughs of New York City, Westchester, Long Island, and Florida; and 31 affiliated community health centers. The Icahn School of Medicine is one of three medical schools that have earned distinction by multiple indicators: ranked in the top 20 by U.S. News & World Report’s “Best Medical Schools”, aligned with a U.S. News & World Report’s “Honor Roll” Hospital, No. 12 in the nation for National Institutes of Health funding, and among the top 10 most innovative research institutions as ranked by the journal Nature in its Nature Innovation Index. This reflects a special level of excellence in education, clinical practice, and research. The Mount Sinai Hospital is ranked No. 14 on U.S. News & World Report’s “Honor Roll” of top U.S. hospitals; it is one of the nation’s top 20 hospitals in Cardiology/Heart Surgery, Diabetes/Endocrinology, Gastroenterology/GI Surgery, Geriatrics, Gynecology, Nephrology, Neurology/Neurosurgery, and Orthopedics in the 2019-2020 “Best Hospitals” issue. Mount Sinai’s Kravis Children’s Hospital also is ranked nationally in five out of ten pediatric specialties by U.S. News & World Report. The New York Eye and Ear Infirmary of Mount Sinai is ranked 12th nationally for Ophthalmology, Mount Sinai St. Luke’s and Mount Sinai West are ranked 23rd nationally for Nephrology and 25th for Diabetes/Endocrinology, and Mount Sinai South Nassau is ranked 35th nationally for Urology. Mount Sinai Beth Israel, Mount Sinai St. Luke’s, Mount Sinai West, and Mount Sinai South Nassau are ranked regionally.

For more information, visit https://www.mountsinai.org or find Mount Sinai on Facebook, Twitter and YouTube.

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Worcester Polytechnic Institute Professor Bruce Bursten Honored for Distinguished Service in Field of Inorganic Chemistry


Bruce Bursten, chemistry and biochemistry professor at WPI.

Bruce Bursten, chemistry and biochemistry professor at WPI.

“We are very proud when our faculty are nationally recognized for their contributions, and grateful that the American Chemical Society saw fit to recognize our distinguished colleague.”-Jean King, Peterson Family Dean of Arts and Sciences at WPI

Bruce Bursten, a chemistry and biochemistry professor at Worcester Polytechnic Institute (WPI), has been named by the American Chemical Society (ACS) to receive the 2020 ACS Award for Distinguished Service in the Advancement of Inorganic Chemistry.

The annual award recognizes individuals who have advanced inorganic chemistry by significant service and outstanding research. The award cites Bursten “for distinguished contributions to inorganic chemistry as an outstanding researcher in inorganic electronic structure and bonding, inspirational teacher and author, and forward-thinking leader.”

Bursten will receive the award in March at the ACS National Meeting in Philadelphia. The event will include a symposium in his honor.

“I am deeply humbled to receive this award from the American Chemical Society,” Bursten said. “To be selected to receive this award by peers within my discipline is a very special honor to me. I am grateful to my students and colleagues who have given me such a rich and satisfying career in chemistry.”

Bursten’s research centers on the correlation of theoretical and experimental electronic structural data with the bonding and reactivity patterns of metal-containing molecules. He is the author or co-author of more than 160 research papers, and he has presented more than 200 research seminars at universities other than WPI, national laboratories, and companies. He is also a co-author of one of the leading textbooks in college general chemistry, currently in its 14th edition.

Bursten is a former provost of WPI. He has served as chairman of the ACS Division of Inorganic Chemistry, as president of ACS, and as chairman of the chemistry division of the American Association for the Advancement of Science (AAAS). His honors include a Camille and Henry Dreyfus Foundation Teacher-Scholar Award, an Alfred P. Sloan Foundation Fellowship, the Spiers Medal and Prize from the Royal Society of Chemistry in the United Kingdom, and the Morley Medal of the Cleveland Section of the ACS. He has also received the Catalyst Award, a teaching honor, from the American Chemistry Council. He is a fellow of AAAS and ACS.

Bursten received a bachelor of science in chemistry, with honors, from the University of Chicago in 1974, and a PhD in chemistry from the University of Wisconsin-Madison in 1978.

“We congratulate Dr. Bursten for his tremendous contribution to the field of inorganic chemistry,” said Jean King, Peterson Family Dean of Arts and Sciences at WPI. “We are very proud when our faculty are nationally recognized for their contributions, and grateful that the American Chemical Society saw fit to recognize our distinguished colleague.”

About Worcester Polytechnic Institute

WPI, the global leader in project-based learning, is a distinctive, top-tier technological university founded in 1865 on the principle that students learn most effectively by applying the theory learned in the classroom to the practice of solving real-world problems. Recognized by the National Academy of Engineering with the 2016 Bernard M. Gordon Prize for Innovation in Engineering and Technology Education, WPI’s pioneering project-based curriculum engages undergraduates in solving important scientific, technological, and societal problems throughout their education and at more than 50 project centers around the world. WPI offers more than 50 bachelor’s, master’s, and doctoral degree programs across 14 academic departments in science, engineering, technology, business, the social sciences, and the humanities and arts. Its faculty and students pursue groundbreaking research to meet ongoing challenges in health and biotechnology; robotics and the internet of things; advanced materials and manufacturing; cyber, data, and security systems; learning science; and more. http://www.wpi.edu

Contact:

Alison Duffy

Director of Strategic Communications

Worcester Polytechnic Institute

Worcester, Massachusetts

508-831-6656; 508-340-5040 (cell)

amduffy@wpi.edu

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Life Molecular Imaging announces presentation of new scientific data at the Human Amyloid Imaging Meeting


Life Molecular Imaging at the 14th Human Amyloid Imaging meeting in Miami

Exciting new research presented using Life Molecular Imaging compounds at the 14th Human Amyloid Imaging meeting in Miami, Florida

Life Molecular Imaging (LMI) announces today that new research results on its approved and investigational positron emission tomography (PET) neuroimaging tracers will be presented at the 14th Human Amyloid Imaging (HAI) meeting in Miami (January 15-17, 2020). The contributions cover nine (9) presentations demonstrating the value of its approved compound Neuraceq™ (florbetaben F18 injection), and fifteen (15) presentations supporting the potential of its investigational Tau-PET tracer PI-2620.

A comprehensive clinical evaluation with imaging biomarkers, such as amyloid PET imaging, can improve the diagnostic accuracy. In addition, the combination of Neuraceq™ and the investigational PI-2620 tracer for the detection of tau pathology, provides a powerful PET imaging biomarker platform for the appropriate characterization of subjects enrolled in clinical trials supporting drug development in neurodegenerative diseases. The value of imaging biomarkers, particularly the combination of amyloid-beta and tau in the same subjects, is increasingly recognized. Highlights also include the presentation of the results from a multi-center evaluation of PI-2620 in subjects with progressive supranuclear palsy (PSP) as well as a poster describing the performance of PI-2620 in subjects with corticobasal syndrome (CBS).

“We are particullary impressed by the data that the research groups collected over the last year in PSP patients” said Dr. Andrew Stephens, MD, PhD, CMO of Life Molecular Imaging. “PI-2620’s ability to also detect 4R tauopathies, such as PSP and CBS allows us to pursue the development of PI-2620 not only for AD, but also for additional neurodegenerative diseases, where previous tau tracers showed limitations.”

Datasets involving LMI compounds presented at the HAI meeting include the following presentations:

Amyloid-PET Neuroimaging presentations involving Neuraceq (florbetaben F18 injection):

January 15, 2020

  • Bullich et al. (Poster #5 Session 1A): Early detection of amyloid load using 18F-Florbetaben PET
  • Klein et al. (Poster #21 Session 1A): Concordance of visual and quantitative assessments of baseline amyloid scans in the GRADUATE gantenerumab studies
  • Landau et al. (Poster #24 Session 1A): Validation of highly sensitive and specific florbetaben positivity thresholds using ADNI participants and young controls
  • Lao et al. (Poster #25 Session 1A): Additive contribution of white matter hyperintensity to amyloid and neurodegeneration on cognitive decline in a diverse, community-based cohort of older adults

January 16, 2020

  • Gispert et al. (Poster #84 Session 2A): Preliminary quantitative results of the AMYPAD prognostic and natural history study
  • Seo et al. (Poster #88 Session 2A): Head-to-head comparison of F-Florbetaben and F-Flutemetamol uptakes in the cortex, striatum and white matter
  • Ewers et al. (Poster #69 Session 2A): Higher microglia biomarker levels are associated with slower rates of amyloid-beta accumulation in humans and in a transgenic mouse model of amyloid-beta
  • Kim et al. (Poster #91 Session 2A): Prevalence of amyloid PET positivity in cognitively normal East Asian populations

January 17, 2020

  • Iaccarino et al. (Poster #137 Session 3A): In vivo amyloid-PET and tau-PET evidence in early-onset Alzheimer’s Disease: taking the LEADS

Tau-PET Neuroimaging presentations involving PI-2620:

January 15, 2020

  • Bischof et al. (Poster #4 Session 1A): A pons cluster detected by a data-driven approach may serve as a favorable reference region for 18F-PI-2620 Tau PET analysis
  • Stevenson et al. (Poster #48 Session 1A): Monitoring disease pathophysiology using multiparametric PET acquisitions: The McGill TRIAD Cohort

January 16, 2020

  • Aguero et al. (Session 3: Neuropathology I): Comparison of autoradiographic binding profiles of Flortaucipir, MK-6240 and PI-2620 in human postmortem tissue samples across the spectrum of neurodegenerative diseases
  • Malarte et al. (Session 4: Neuropathology II): In vitro characterization of second-generation tau pet tracers in human autopsy brain tissue
  • Brendel et al. (Session 5: Clinical I): 18F-PI-2620 tau-PET in Progressive Supranuclear Palsy – A multi-center evaluation
  • Stephens et al. (Poster #90 Session 2A): PI-2620 Tau PET is associated with amyloid-beta levels in scans from subjects of the elenbecestat MissionAD program
  • Villemagne et al. (Poster #76 Session 2A): Assessing Aβ, tau, and reactive astrocytosis in aging and AD

January 17, 2020

  • Brendel et al. (Poster #122 Session 3A): Perfusion-phase 18F-PI-2620 tau-PET imaging as a surrogate marker of neuronal injury
  • Brendel et al. (Poster #123 Session 3A): Binding characteristics of 18F-PI-2620 differentiate the clinically predicted tau isoform in suspected 3/4-repeat and 4-repeat tauopathies
  • Brendel et al. (Poster #124 Session 3A): 18F-PI-2620 tau-PET for assessment of heterogeneous neuropathology in corticobasal syndrome
  • Bullich et al. (Poster #125 Session 3A): Optimal reference region for the quantification of tau load in the brain using 18F-PI-2620 PET
  • Koran et al. (Poster #143 Session 3A): Validation of clinical protocols for clinicians analyzing 18F-PI-2620 tau PET/MRI images
  • Dore et al. (Session 7: Tau I): Towards a CenTauR cortical mask
  • Toueg et al. (Poster #169 Session 3A): Elevated medial temporal lobe Tau PET with 18F-PI2620 in normal controls with “borderline” neuropsychological testing profiles
  • Trelle et al. (Poster #170 Session 3A): Hippocampal tau accumulation predicts individual differences in episodic memory in cognitively normal older adults

About Neuraceq (florbetaben F18 injection)

Indication

Neuraceq™ (florbetaben F18 injection) is a radioactive diagnostic agent indicated for Positron Emission Tomography (PET) imaging of the brain to estimate β-amyloid neuritic plaque density in adult patients with cognitive impairment who are being evaluated for Alzheimer’s Disease (AD) and other causes of cognitive decline.

A negative Neuraceq scan indicates sparse to no amyloid neuritic plaques and is inconsistent with a neuropathological diagnosis of AD at the time of image acquisition; a negative scan result reduces the likelihood that a patient’s cognitive impairment is due to AD. A positive Neuraceq scan indicates moderate to frequent amyloid neuritic plaques; neuropathological examination has shown this amount of amyloid neuritic plaque is present in patients with AD, but may also be present in patients with other types of neurologic conditions as well as older people with normal cognition.

Neuraceq™ is an adjunct to other diagnostic evaluations.

Limitations of Use

  • A positive Neuraceq™ scan does not establish the diagnosis of AD or any other cognitive disorder.
  • Safety and effectiveness of Neuraceq™ have not been established for (i) Predicting development of dementia or other neurologic conditions; (ii) Monitoring responses to therapies.

Important Safety Information

Risk for Image Interpretation and Other Errors

Neuraceq can be used to estimate the density of β-amyloid neuritic plaque deposition in the brain. Neuraceq is an adjunct to other diagnostic evaluations. Neuraceq images should be interpreted independent of a patient’s clinical information. Physicians should receive training prior to interpretation of Neuraceq images. Following training, image reading errors (especially false positives) may still occur. Additional interpretation errors may occur due to, but not limited to, motion artifacts or extensive brain atrophy.

Radiation Risk

Administration of Neuraceq, similar to other radiopharmaceuticals, contributes to a patient´s overall long-term cumulative radiation exposure. Long-term cumulative radiation exposure is associated with an increased risk of cancer. It is important to ensure safe handling to protect patients and health care workers from unintentional radiation exposure.

Most Common Adverse Reactions

In clinical trials, the most frequently observed adverse drug reactions in 872 subjects with 1090 Neuraceq™ administrations were injection/application site erythema (1.7%), injection site irritation (1.1%), and injection site pain (3.4%).

About PI-2620

Tau deposits, in conjunction with beta-amyloid plaques, represent the other pathological hallmark of Alzheimer’s disease, with tau deposits further playing an important role in other neurodegenerative diseases. PI-2620 is binding to 3R/4R and 4R tau deposits and is a next generation 18F-labeled investigational PET tracer with favourable properties and imaging characteristics. It was discovered in a research collaboration between Life Molecular Imaging and AC Immune, a Swiss-based clinical stage biopharmaceutical company. Life Molecular Imaging has the exclusive, world-wide license for research, development and commercialization of tau PET tracers generated within the discovery program.

About Life Molecular Imaging (LMI)

Life Molecular Imaging (LMI, formerly Piramal Imaging) was formed in 2012 with the acquisition of the molecular imaging research and development portfolio of Bayer Pharma AG. It is now part of the Alliance Medical Group (a member of the Life Healthcare Group) offering an integrated business including research and development laboratories, a network of cyclotrons, radiopharmacies and imaging facilities. By developing novel PET tracers for molecular imaging, LMI is focusing on a key field of modern medicine. The organization strives to be a leader in the Molecular Imaging field by developing innovative products that improve early detection and characterization of chronic and life-threatening diseases, leading to better therapeutic outcomes and improved quality of life.

Please visit https://life-mi.com.

About Life Healthcare Group

Life Healthcare Group is a market-leading, international, diversified healthcare organization. Life Healthcare has over 33 years’ experience in the South African private healthcare sector, and currently operates 66 healthcare facilities in southern Africa. Services include acute hospital care, acute physical rehabilitation, acute mental healthcare, renal dialysis, and employee health and wellness services. The Group owns Alliance Medical Group, the leading independent provider of medical imaging services within Europe, operating across 10 international countries. Life Healthcare also owns Scanmed S.A. (Poland) which provides healthcare and medical services in 20 Polish cities, with over 65 medical specialisations and diagnostic services available in 32 facilities. Visit lifehealthcare.co.za

Media Contact:

Nicole Fletcher | Marketing Communications | Life Molecular Imaging

+1 857-202-1122 | n.fletcher@life-mi.com

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Microbial Discovery Group Announces Updated Brand


MDG Full Color Logo

Microbial Discovery Group announces updated branding including this new logo.

It was time to bring cohesion to our brand and our company values of working to Feed, Clean, and Save the World.

Microbial Discovery Group LLC (MDG), a leading R&D driven product development and Bacillus fermentation company, announced that as of January 2020 the brand will be refreshed with a new logo and color scheme. MDG wanted to share the rationale behind the updates and what they represent for their brand and customers.

“Having experienced significant growth over the past few years and expansion into new markets, it was time to bring cohesion to our brand and our company values of working to Feed, Clean, and Save the World,” explained Jackie Worth, Head of Marketing.

“We needed the ability to clearly communicate MDG’s commitment to our values and unique identity.”

The new bolder logo and color scheme work to better represent the company’s drive towards creating cutting edge solutions backed by what they describe as Real Science, Trusted Process, and Proven Success in their corporate tagline.

“Our new logo really embodies the strength we have within our R&D team as we gain momentum towards safely meeting the growing market demands from Probiotic Usage, Plant Health, Antibiotic Alternatives, and Biological Solutions within Wastewater and Industrial and Institutional cleaning,” added Michael King, CEO/CSO.

With healthy growth projections for 2020, MDG remains extremely committed to providing value for their customers with meaningful, quality solutions.

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About Microbial Discovery Group

Microbial Discovery Group (MDG) is an R&D driven product development and Bacillus fermentation company. MDG has the capabilities to ensure success. When partnering with MDG, you can expect high quality, consistent Bacillus strain manufacturing delivered with efficiency and integrity. MDG is passionate about applying scientific principles to create indispensable solutions for our partners while working to Feed, Clean, and Save the World. For more information on Microbial Discovery Group, visit http://www2.mdgbio.com/2020.

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Worcester Polytechnic Institute Researchers Develop Tool to Identify Molecular Receptors for Pheromones in Worms


WPI researcher Jagan Srinivasan (left) and Douglas K. Reilly.

WPI researcher Jagan Srinivasan (left) and Douglas K. Reilly.

“Here we are saving months of work, we’re streamlining the process, and we’re getting a targeted approach.”- Jagan Srinivasan, Associate Professor of Biology and Biotechnology at WPI

Researchers at Worcester Polytechnic Institute (WPI) have developed a tool to identify molecular receptors in worms that are involved in sensing pheromones related to mating, an advance that could speed up neuroscience research into pheromones by eliminating months of work.

Associate professor of biology and biotechnology Jagan Srinivasan, doctoral candidate in biology Douglas K. Reilly, and researchers at Cornell University published their findings in Organic & Biomolecular Chemistry, a journal of the Royal Society of Chemistry in the United Kingdom.

Pheromones are chemicals produced by animals that send signals to other animals and trigger social responses, such as mating. Srinivasan and Reilly study pheromones in microscopic worms known as Caenorhabditis elegans, or C. elegans, to better understand how the sense of smell works. Their research could have implications for human research because C. elegans has a nervous system that mimics the basic mechanisms of smell in humans, and loss of the sense of smell is associated with neurodegenerative disorders such as Alzheimer’s disease.

Srinivasan and Reilly developed a process that more quickly isolates pheromone receptors in C. elegans. Receptors are specialized proteins that act as docking stations for molecules. When worms are exposed to pheromones, the pheromones latch onto the molecular receptors in the worms.

Isolating a specific molecular receptor traditionally has been a long, laborious process because the worms possess more than 1,000 molecular receptors. Srinivasan described the traditional process—which takes three or four months—as hunting for a needle in a haystack. The new method he and Reilly developed takes about a month.

“Here we are saving months of work, we’re streamlining the process, and we’re getting a targeted approach,” Srinivasan said.

In their study, Srinivasan and Reilly attached a chemical known as an alkyne to an ascaroside, a pheromone produced by C. elegans to attract male worms for mating.

“We wanted to find a way that we could take a pheromone and link it to a probe, yet it would still be biologically active so a male would sense it and respond to it with the right receptor,” Reilly said. “Then we wouldn’t have to screen 1,200 receptors that are in the genome.”

For this study, the researchers focused on the process rather than the resulting receptor, which they said could be a subject of further research. Their probe methods could also be applied to other pheromones and to other research organisms, such as flies, to better understand how receptors function, they said.

“We’re looking at this mate attractant pheromone, but there are people looking at pheromones involved in foraging for food and other actions,” Reilly said. “For those, we can start to ask what receptors are sensing the pheromone we’re using.”

In addition, Srinivasan said, “Applications of this new technology could help identify receptors in parasitic nematodes that cause damage to agricultural crops.”

About Worcester Polytechnic Institute

WPI, the global leader in project-based learning, is a distinctive, top-tier technological university founded in 1865 on the principle that students learn most effectively by applying the theory learned in the classroom to the practice of solving real-world problems. Recognized by the National Academy of Engineering with the 2016 Bernard M. Gordon Prize for Innovation in Engineering and Technology Education, WPI’s pioneering project-based curriculum engages undergraduates in solving important scientific, technological, and societal problems throughout their education and at more than 50 project centers around the world. WPI offers more than 50 bachelor’s, master’s, and doctoral degree programs across 14 academic departments in science, engineering, technology, business, the social sciences, and the humanities and arts. Its faculty and students pursue groundbreaking research to meet ongoing challenges in health and biotechnology; robotics and the internet of things; advanced materials and manufacturing; cyber, data, and security systems; learning science; and more. http://www.wpi.edu

Contact:

Alison Duffy

Director of Strategic Communications

Worcester Polytechnic Institute

Worcester, Massachusetts

508-831-6656; 508-340-5040 (cell)

amduffy@wpi.edu

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