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!--Ewebeditor: Page title"--August 6, 2020 //--- In a new study, the first experimental SARS-CoV-2 experimental mRNA vaccine to enter human trials in the United States has been shown to cause neutral antibody and beneficial T-cell reactions with the help of a carefully modified tyragen.
findings were published online August 5, 2020 in the journal Nature under the title "SARS-CoV-2 mRNA vaccine design enabled by prototypeogen preparedness".
vaccine, called mRNA-1273, was developed by the National Institutes of Health (NIH) in collaboration with biotech company Moderna.
The latest study of the Modena-NIH vaccine, which recently entered Phase III human clinical trials, describes preclinical studies in mice and important genetic modifications to the tingling protein by a team at the University of Texas at Austin.
lead authors of the study were Barney Graham and Kizzmekia Corbett of the National Institute of Allergy and Infectious Diseases (NIAID) Vaccine Research Center, part of the NIH, and Andrea Carfi of Modena.
photo Source: www.pixabay.com.
part of this paper describes keeping THES-CoV-2 stable with the stinging protein that fuses with the host cell and infects it.
early study of coronaviruses is critical to the fastest progress from genome sequencing to human vaccine testing, which takes only 66 days.
"There are several things that are key to rapid vaccine development, including understanding the precise atomic level structure of the hedgehog protein and how to keep it stable," said Jason McLellan, co-author of the paper and an associate professor of molecular biosciences at the University of Texas at Austin.
that although all this happened quickly, it was possible to develop the vaccine because of years of early research.
" NIAID team and members of the McLellan Laboratory at the University of Texas at Austin announced earlier this year that they had identified the molecular structure of the stabilized SARS-CoV-2 protrusion protein within weeks of receiving the gene sequence, and published the structure of the hedgehog protein in the journal Science. 2020, doi:10.1126/science.abb2507, see news reports: In-depth analysis of why new coronaviruses are more likely to spread from person to person Viral S protein and host cell receptacle ACE2 affinity is 10-20 times that of SARS! )。
NIAID and Moderna, based in Cambridge, Massachusetts, are working on a messenger RNA (mRNA) vaccine.
NIH, the vaccine can guide human cells to express the puncture protein under the pre-fusion structure to cause an immune response.
new paper describes how the vaccine blocks SARS-CoV-2 infection from spreading to the trachea of mice, producing mediated antibodies and prompting immune cells called memory T cells to respond.
the stable tyrogen, known as S-2P, and several other coronavirus vaccines currently undergoing clinical trials in humans have also used stabilized tyrogens.
SARS-CoV-2 puncture protein is a shape-changing protein that changes its structure before and after fusion with host cells.
when the hedgehog is in the pre-fusion shape, the immune system responds best, so McLellan's team redesigned the protein in two key places to lock it in.
Nianshuang Wang, a postdoctoral researcher at McLellan Labs, discovered genetic mutations necessary to keep THES-CoV's shape-changing protrusion protein stable as early as 2017 (PNAS, 2017, doi:1073/pnas.1707304114), and the team found that the same strategy worked on the new coronavirus.
the researchers used smaller genetic modifications to the gene sequences that encode the protein, essentially hardening the spring-loaded portion of the protein's molecules and preventing it from rearranging.
the researchers did not go through a painful trial and error process, but instead designed the necessary genetic mutations about a day after receiving the SARS-CoV-2 virus genome.
McLellan laboratory identified the atomic-level structure of the hedgehog protein, which graduate student Daniel Wrapp harvested and purified: S-2P.
, NIAID's Corbett and Graham verified that the S-2P protein produced powerful antibodies in mice.
(bioon.com) Reference: 1.Kizzmekia S. Corbett et al. SARS-CoV-2 mRNA vaccine design enabled by prototype pathogen preparedness. Nature, 2020, doi:10.1038/s41586-020-2622-0.2.Locking Down Shape-Shifting Protein Protein Aids Development of COVID-19 Vaccine Title."--!--/ewebeditor:page--.
