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Prof. Phillip A Sharp
Institute Professor
Professor of Biology
Primary DLC
Department of Biology
MIT Room:
76-461
(617) 253-6421
sharppa@mit.edu
https://ki-mit-edu.ezproxy.canberra.edu.au/people/faculty/phillip-sharp
Assistant
Geoffrey Shamu
(617) 253-6425
shamu@mit.edu
Areas of Interest and Expertise
Gene Regulation
Virology
Molecular Biology: Regulation of Transcription/RNA Splicing
Biochemistry and Regulation of Messenger RNA Synthesis in Mammalian Cells
Identification of Factors Responsible for Controlling Initiation or Elongation of Transcription
Studies of the Mechanisms for RNA Splicing and Polyadenylation
Development of Methods for Genetic Analysis of Mammalian Cells
Biochemistry and Biophysics
Therapeutic Gene Biotechnology
Splicing of Introns from Nuclear Perecursor RNA
Dupont/MIT Alliance (DMA)
Cancer Biology
Cell Biology
Cellular and Genetic Neuroscience
Bioengineering
Nano-Based Drugs
Metastasis, 
Personalized Medicine
Research Summary
MicroRNAs (miRNAs) are encoded by endogenous genes and regulate over half of all genes in mammalian cells. They regulate gene expression at the stages of translation and mRNA stability. Developing methods to physically identify the target mRNAs for particular miRNAs is on going. The surprising recent finding that expression of certain microRNAs can induce a pluripotent stem cell indicates that this mechanism of cytoplasmic regulation rivals that of transcription factors in the nucleus. RNA interference (RNAi) has dramatically expanded the possibilities for genotype/phenotype analyses in cell biology. Investigations into the mechanisms responsible for the activities of short interfering RNAs (siRNAs) are underway with the objective of increasing their effectiveness in gene silencing. Delivery of siRNAs by nanoparticles to silence genes in tumors is being tested in ovarian tumor models. High throughput sequencing of RNA populations revealed the generation of small RNAs in divergent transcription in mammalian cells. The role of this pervasive transcription from the anti-sense strand is under investigation. It is likely that these anti-sense transcripts are unstable because, in contrast to the sense transcript, they are not recognized by the certain RNA splicing factors. The same high throughput technology allows definition of alternatively spliced isoforms. Shifts in isoforms are common in cancer versus normal cells. Also, recent results from other labs have suggested that chromatin structure is related to control of alternative splicing. We are investigating these processes and, in particular, the relationship between elongation of transcription, RNA splicing and chromatin modifications.
Recent Work
Projects
October 31, 2024
MIT Life Sciences and Health Collaborative
Principal Investigators
Nergis Mavalvala
,
Phillip Sharp
November 7, 2016
Department of Biology
Non-Coding RNAs
Principal Investigator
Phillip Sharp
October 19, 2016
Department of Biology
Convergence: The Future of Health
Principal Investigator
Phillip Sharp
December 5, 2011
Department of Biology
Sharp Laboratory
Principal Investigator
Phillip Sharp
September 10, 2009
Department of Biology
Characterization of Pathways Controlling Cancer at the Level of Gene Regulation
Principal Investigator
Phillip Sharp
September 10, 2009
Department of Biology
Regulation of mRNA Processing
Principal Investigator
Phillip Sharp
September 10, 2009
Department of Biology
Stress and Proliferation States Impact microRNA-Mediated Regulation in Cancer
Principal Investigator
Phillip Sharp
December 21, 2006
Department of Biology
Molecular Genetics and Immunology Program
Principal Investigator
Phillip Sharp
July 13, 1999
Department of Biology
RNA Splicing
Principal Investigator
Phillip Sharp
Video
2021-RD-Philip-Sharp
November 18, 2021
Conference Video
Duration: 26:13
Show more
Phillip A. Sharp
Institute Professor and Professor of Biology
Related Faculty
Prof. Nancy H Hopkins
Professor of Biology, Emerita
Dr. Jens K Plassmeier
Research Affiliate
Prof. Robert T Sauer
Salvador E Luria Professor of Biology