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    • GenomeIndia Project Finds 44 Million Indian Genetic Variants the World Had Never Seen Before. India’s biggest genomics study has uncovered 44 million previously unknown genetic variants. Scientists say the GenomeIndia Project could change how diseases are diagnosed and how medicines are developed for Indian patients.
      Biotech News

      GenomeIndia Project Finds 44 Million Indian Genetic Variants the World Had…

      Astronauts Advancing Life-Saving Cancer Research Beyond Earth
      Biotech News

      ASTRONAUTS SAVING LIVES : Cancer Research Beyond Earth

      Hantavirus The Rare Virus That Can Turn a Simple Fever Dangerous. Dramatic medical awareness poster about hantavirus, featuring a close-up of a rodent on the right and a stylized red virus illustration on the left. In the background, semi-transparent human lungs are shown, emphasizing respiratory impact. Large bold title reads “HANTAVIRUS,” with a subtitle stating “The Rare Virus That Can Turn a Simple Fever Dangerous.” The design uses dark tones with red highlights to convey urgency and health risk, along with small icons and warning-style information at the bottom about rodent transmission and potential severe lung effects.
      Biotech News

      Hantavirus: The Rare Virus That Can Turn a Simple Fever Dangerous

      Quantum Computing Takes a Big Leap for Faster Drug Discovery
      Biotech News

      Quantum Computing: A Giant Leap For Drug Discovery

      Scientists Discover a Simple Method using Red Blood Cells to Improve CAR T Cell Therapy, Offering Effective Cancer Treatment Possibilities.
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      A Simple Approach Enhancing CAR T Cell Therapy with Natural RBCs…

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      DEBEL DRDO Internship 2026 for Biomedical Engineering & Science Students –…

      Apply for AIIMS Patna Recruitment - Govt. Paid Internship. Life Sciences Internship for Biotechnology and Microbiology students at APIIC.
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      Paid Govt Life Sciences Internship at AIIMS Patna | Apply Now

      Paid Life Science Internship at Presidency University Project Intern Opportunity for MSc Candidates! Featured banner for “Paid Life Science Internship at Presidency University” featuring the Biotecnika logo at the top, a life sciences researcher working in a modern laboratory, a university campus backdrop, biotechnology-themed graphics, and a bold “Apply Now” button at the bottom.
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      Paid Life Science Internship at Presidency University | Opportunity for MSc…

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    • BioTecNika Times - 13-05-2026: New Internship Opportunity at DRDO | Freshers Job at Novonesis | Biotech Jobs at Top Companies and Institutes
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      BioTecNika Times – 13-05-2026: New Internship Opportunity at DRDO | Freshers…

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MSc Admission Notification 2020
Biotech Admissions

MSc Plant Biotech Admission Notification 2020 at TERI School of Advanced...

Diluxi Arya - March 19, 2020 0
BioTecNika TV

ICMR JRF 2020 Exam Notification – Eligibility, Revised Application Details &...

Diluxi Arya - March 19, 2020 3
Bill Gates Warned Us About Coronavirus
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How We Ignored Bill Gate’s Warning On An Epidemic Five Years...

Namitha Thampi - March 19, 2020 0
Facts of Coronavirus
Biotech News

Coronavirus Fact Check – Can Face Masks Prevent COVID-19?

Prathibha HC - March 19, 2020 0
New Hand Sanitizer By IHBT scientists
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New Hand Sanitizers Developed By IHBT Scientists To Prevent Coronavirus Infection

Prathibha HC - March 19, 2020 0
CUCET 2020 Notification - Central Universities Common Entrance Test
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CUCET 2020 Notification – Central Universities Common Entrance Test

Diluxi Arya - March 19, 2020 1
BioTecNika Times

Biotecnika Times – Newsletter 19.03.2020 – Cancer Center CNCI Job, NCBS...

Diluxi Arya - March 19, 2020 0
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Is Coronavirus A Man Made Bioweapon?

Namitha Thampi - March 18, 2020 3
Summer Training Program 2020
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Summer Training Program 2020 at Dept of Bioengineering, NIT Agartala

Diluxi Arya - March 18, 2020 0
Editing Multiple Genome Fragments At A Time Scientists can now edit multiple sites in the genome at the same time to learn how different DNA stretches co-operate in health and disease. CRISPR-based DNA editing has revolutionized the study of the human genome by allowing precise deletion of any human gene to glean insights into its function. But one feature remained challenging—the ability to simultaneously remove multiple genes or gene fragments in the same cell. Yet this type of genome surgery is key for scientists to understand how different parts of the genome work together in the contexts of both normal physiology and disease. Now such a tool exists thanks to the teams of Benjamin Blencowe and Jason Moffat, both professors of molecular genetics at the Donnelly Centre for Cellular and Biomolecular Research. Dubbed 'CHyMErA', for Cas Hybrid for Multiplexed Editing and Screening Applications, the method can be applied to any type of mammalian cell to systematically target the DNA at multiple positions at the same time, as described in a study published in the journal Nature Biotechnology. Often described as genome scissors, CRISPR works by sending a DNA-cutting enzyme to desired sites in the genome via guide RNA molecules, engineered to adhere to the target site. The most widely used DNA-cutting enzyme is Cas9. - Editing Multiple Genome Fragments At A Time. Since Cas9 first came to light, other Cas enzymes with distinct properties have been identified by scientists seeking to improve and expand the applications of the technology. Unlike the CRISPR-Cas9 technology, CHyMErA combines two different DNA-cutting enzymes, Cas9 and Cas12a, to allow more versatile applications. Cas12a is an enzyme that can be used to generate multiple guide RNA molecules in the same cell, which is key for simultaneous DNA editing. Thomas Gonatopoulos-Pournatzis, a research associate in Blencowe's group, had spent several years trying to develop combinatorial gene editing by testing Cas9 and Cas12a enzymes on their own. He then had the idea to combine these enzymes to generate the CHyMErA system. "We had been trying a number of approaches to induce genetic fragment deletions and nothing worked as well as CHyMErA," he says. "I was thrilled when together with Shaghayegh Farhangmehr, a Ph.D. student in the Blencowe lab, we saw the first evidence that CHyMErA was successful in deleting gene segments. We obtained these results on Boxing Day and it was the best Christmas present I could have wished for." The next step was to harness CHyMErA in large-scale screens to systematically analyze how genes act together, as well as the functions of individual parts of genes. Blencowe's team, which studies the regulation and function of gene segments known as exons, approached Moffat, whose group had developed extensive experience with CRISPR technology. "With CHyMErA, you can use the best of the two enzymes," says Michael Aregger, a research associate in the Moffat lab, who played a key role in developing the screen-based applications of CHyMErA. "Cas9 has been improved by the community to have a very high editing efficiency, whereas Cas12a allows multiplexing of guide RNAs and therefore provides a lot more flexibility in finding sites in the genome that we can cut." In one application of CHyMErA, the researchers targeted pairs of genes known as paralogs, which have a similar DNA code but remain poorly studied because they were difficult to research. Because paralogs arose by duplication of an ancestral gene, it had been assumed they would largely have similar roles. But their function could not be revealed by the existing single-gene targeting methods typically employed in genetic screens, mostly because the other paralog would compensate for the one that's missing. "With CHyMErA, we can take out both paralogs in pairs to see if that ancestral function is important for the cell to survive," says Kevin Brown, a senior research associate in the Moffat lab and co-lead author on the study along with Aregger and Gonatopoulos-Pournatzis. "We are able to now interrogate a class of genes that were previously missed." After knocking out ~700 paralog pairs, almost all that exist in the human genome, the analysis confirmed that many of these gene pairs do indeed perform similar roles in cell survival, whereas others have distinct functions. Another feature of CHyMErA is that both Cas9 and Cas12a can be deployed to nearby genome sites to cut out gene fragments such as exons. This allowed the team to individually delete thousands of exons that have been linked to cancer and brain function but were not amenable to targeting with Cas9 alone. Exons are variably included in genes' transcripts and can modify the function of the encoded proteins, although how individual exons contribute to cellular processes remains largely unknown. Out of 2,000 exons analyzed by CHyMErA, over 100 were found to be critical for cell survival, enabling future research to now focus on shining light on their potential roles in disease. "Once we identify exons that have a critical role in disease, we can use this information to develop new therapies," says Gonatopoulos-Pournatzis. Editing Multiple Genome Fragments At A Time - Source
Biotech News

New System To Edit Multiple Genome Fragments Together

Prathibha HC - March 18, 2020 0
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