After a decade-long $3 billion international effort, scientists heralded the 2001 completion of the human genome as a moon landing achievement for biology and the key to finally solving intractable diseases like cancer.
But it turns out this was only the end of the beginning, with a much greater complexity to life revealed by the roughly 20,000 genes found within the human genome. For one, most diseases are incredibly complex, with very few caused by a single gene mutation. Rather, the more accurate picture is many acting genes acting in concert, with the routes to disease looking like public transit or subway maps.
Since then, efforts such as the modENCODE project – a $57 million multi-center initiative funded by the National Human Genome Research Institute (NHGRI) – have been aimed at identifying all the genome elements that can turn on and off genes.
Now, an international scientific team, led by Arizona State University professor and Biodesign Institute researcher Marco Mangone, has added a new worldwide resource with the first library built for researchers to explore genes’ deep and hidden messages. The paper was published in BMC Genomics (http://www.biomedcentral.com/1471-2164/16/1036, DOI 10.1186/s12864-015-2238-1).
The end of the message
“If the genome is considered the blueprint of the cell, proteins are the really bricks and mortars,” said Josh LaBaer, director of the Virginia Piper Center for Personalized Diagnostics, which aims to undercover the telltale early warning signs of disease from a systematic study of all of the proteins in the human body, a field called proteomics.
But to make proteins, first the DNA genomic information must be transcribed with complete fidelity, chemical letter by letter into an intermediary molecule, called messenger RNA, or mRNA. In what is known as the central dogma of biology, DNA makes RNA, which makes protein.
Marco Mangone, a core faculty member in LaBaer’s center, has devoted his career to looking at a peculiar region found at the ends of the mRNA sequence information, called untranslated elements, or UTRs. As the name suggests, these regions do not go on to make protein, but stresses Mangone: “They have to be there for a reason.”
Mangone’s raison d’etre is to understand the function of every UTR in the human body, called the 3’UTRome (3′ indicates a location at the end of the mRNA).
And so he and his team have painstakingly put together the first and largest human 3?UTRome library in the world. It is made up of 1,461 human 3?UTRs to date (representing about 10 percent of genome), and freely available to the worldwide scientific community to explore all aspects of biology, gene regulation and disease.
Shooting the messenger
Sophocles first wrote in his Greek civil war play “Antigone“: “no one loves the messenger who brings bad news.” And when all roads led to ancient Rome, and messengers were sent about delivering the news, a revolutionary change occurred in communications tactics: killing the messenger to prevent the communication from taking place.
Mangone, a native Italian who did his doctoral studies in Rome, has harkened back to this strategy when examining the role of the 3’UTRome. His lab uses standard molecular biology and bioinformatics tools to study the production, function and disease contributions of UTRs and their role in governing gene expression. He pioneered this work in a simple animal, the worm C. elegans, and now, in the new BMC paper, toward human genomics.
Why would this elaborate system be in place? Based on numerous studies, the role of the 3’UTRome is complicated, but one major theme that has emerged is to prevent the mRNA message from ever being delivered, or in biology terms, ever translated into protein.
Small RNAs, called micro RNAs (miRNAs), work to pair with a UTR to block translation, killing the message, and thus, silencing a gene. Uncovering the interplay between miRNA and their specific UTRs have become a hot area in biology, and big business.
Big pharma, big future
These gene silencers have become all the rage in the pharmaceutical industry. So much so, that the global miRNA research market was valued at nearly $295.1 million in 2011 and is expected to reach $763 million by 2017.
It’s become big business because of their potential as therapeutics for the treatment of some severe diseases, including cancer and genetic disorders, by introducing specific miRNAs into diseased cells to silence the defective gene.
A broad portfolio of miRNA pathway drug candidates have been developed, some already in Phase II clinical trials, showing promising clinical data in different areas of medicine, such as cancer, HCV infection, and cardiovascular diseases.
Read more: New ASU worldwide resource for exploring genes’ hidden messages
The Latest on: Proteomics
[google_news title=”” keyword=”proteomics” num_posts=”10″ blurb_length=”0″ show_thumb=”left”]
via Google News
The Latest on: Proteomics
- New multi-task deep learning framework integrates large-scale single-cell proteomics and transcriptomics dataon April 26, 2024 at 7:35 am
The exponential progress in single-cell multi-omics technologies has led to the accumulation of large and diverse multi-omics datasets. However, the integration of single-cell proteomics and ...
- Acrivon Therapeutics’ shares climb 14% on plans to present cancer-test dataon April 24, 2024 at 4:16 pm
Shares of Acrivon Therapeutics advanced in post-market trading after the biopharmaceutical company said it would present clinical trial data in ...
- Acrivon Therapeutics Reports Initial Positive Clinical Data for ACR-368 and Pipeline Program Progress Today at Corporate R&D Eventon April 24, 2024 at 1:25 pm
Initial ACR-368 Phase 2b clinical data in patients with ovarian or endometrial cancers (n=26; 10 OncoSignature-positive and 16 ...
- Identifying proteins causally related to COVID-19, healthspan and lifespanon April 24, 2024 at 1:05 pm
A new research paper titled "Using genetics and proteomics data to identify proteins causally related to COVID-19, healthspan and lifespan: a Mendelian randomization study" has been published in Aging ...
- Testing how well biomarkers work: New fluorescence microscopy method can improve resolution down to the Ångström scaleon April 24, 2024 at 9:49 am
LMU researchers have developed a method to determine how reliably target proteins can be labeled using super-resolution fluorescence microscopy.
- Proteomics Moves From Expression to Turnoveron April 22, 2024 at 4:59 pm
Measuring protein turnover is complex. Even in simple unicellular organisms such as bacteria and yeast, there are many up- and down-stream processes that must be considered. The major premise of ...
- Proteomics News and Researchon April 22, 2024 at 4:59 pm
A new case report published in the peer-reviewed OMICS: A Journal of Integrative Biology describes how longitudinal multi-omics monitoring (LMOM) helped to detect a precancerous pancreatic tumor ...
- Proteomics Market Expanding Rapidly, Predicted Value of USD 103.8 Billion by 2032on April 14, 2024 at 5:00 pm
According to a recent report by Market.us, the Global Proteomics Market size is expected to be worth around USD 103.8 Billion by 2032 from USD 30.8 Billion in 2023, growing at a CAGR of 14.9% during ...
- Biognosys and Alamar Biosciences Forge Strategic Partnership in Proteomics to Advance Biopharma and Precision Medicine Researchon April 4, 2024 at 1:11 am
Strategic partnership expands Biognosys’ services to include Alamar’s NULISA assays as well as joint scientific research in biofluid-based proteomics Complementary value of Biognosys’ DIA-MS ...
- Bruker Advances CCS-Enabled 4D-Proteomics timsTOF Solutions for Immunopeptidomes and Glycoproteomics at US HUPOon March 10, 2024 at 5:01 pm
The rapid advances in deep, at-scale proteomics, glycomics and peptidomics research solutions complement other performance-leading life-science tools for the post-genomic era by Bruker.
via Bing News