Genetic Approaches to Analyzing Membrane Proteins - Jonathan Beckwith

Abstract

Funding Agency

Agency: National Institute of Health (NIH)
Institute: National Institute of General Medical Sciences (NIGMS)
Type: Method to Extend Research in Time (MERIT) Award (R37)
Project #: 3R37GM038922-02S1
Application #: 3484879
Study Section: Microbial Physiology and Genetics Subcommittee 2 (MBC)

Project Start: 1987-09-01
Project End: 1992-03-31
Budget Start: 1989-04-01
Budget End: 1989-08-31
Support Year: 2
Fiscal Year: 1989
Total Cost
Indirect Cost

Institution

Name: Harvard University
Department
Type: Schools of Medicine
DUNS #: 082359691

City: Boston
State: MA
Country: United States
Zip Code: 02115

Related projects

Publications

Gonzalez, Mark D; Akbay, Esra A; Boyd, Dana et al. (2010) Multiple interaction domains in FtsL, a protein component of the widely conserved bacterial FtsLBQ cell division complex. J Bacteriol 192:2757-68

Gonzalez, Mark D; Beckwith, Jon (2009) Divisome under construction: distinct domains of the small membrane protein FtsB are necessary for interaction with multiple cell division proteins. J Bacteriol 191:2815-25

Bardwell, J C; Lee, J O; Jander, G et al. (1993) A pathway for disulfide bond formation in vivo. Proc Natl Acad Sci U S A 90:1038-42

Martin, J L; Waksman, G; Bardwell, J C et al. (1993) Crystallization of DsbA, an Escherichia coli protein required for disulphide bond formation in vivo. J Mol Biol 230:1097-100

Bardwell, J C; McGovern, K; Beckwith, J (1991) Identification of a protein required for disulfide bond formation in vivo. Cell 67:581-9

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