Abstract

Structure/function analysis will continue on the interaction of proteins with the surface of membranes and with steroids. Both processes figure heavily in the control of intracellular metabolism; the former through the enzymatic release of second mssengers from the cytosolic leaflet of the plasma membrane; the later through steroid activation of genetic control elements. Our principal tool will be high resolution crystallography of the appropriate proteins and of their physiologically important complexes. Phosphlipase A2 (PLA2) offers an ideal model for studying the interaction of proteins with membrane surfaces since it prefers to attack phospholipid head groups if they are in membranes or membrane-like aggregates. Despite several high resolution crystal structures of PLA2 we do not yet understand its action. To resolve this issue we will continue to systematically build a stereochemical picture of the enzyme's functional interactions. The steps are: (1) To complete the 1.7 A refinement of the ligand free form of C. atrox PLA2; (2) To solve the high resolution crystal structure of the calcium complex of C. atrox of PLA2; (3) To solve the high resolution crystal structure of crotoxin, a phosphlipiasic neurotoxin whose action is targeted to the presynaptic membrane; (4) To prepare crystals of PLA2 in complexes with phosphlipid analogues that emulate the interaction between PLA2 and phosphlipids in membrane-like aggregates. This requires the synthesis of stable analogues in which the head groups are constrained to resemble those in an aggregate, but that are small enough to cocrystallize with the enzyme; (5) To explore the preparation of crystalline intracellular phospholipases that mediate internal cell responses. As a first model for protein steroid interaction, we will interpret the 2.5 A map of delta 5-KSI and contrast the structure with that of its isomorphous steroid inhibitor complex. Once refined, these structures should reveal the enzyme's mechanism of specific steroid binding and catalysis. We hope to prepare crystals of the rather plentiful human sex steroid binding globulin and ultimately to crystallize estrogen and progesterone receptors.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM022324-12
Application #
3271098
Study Section
Biophysics and Biophysical Chemistry B Study Section (BBCB)
Project Start
1978-09-01
Project End
1988-12-31
Budget Start
1988-01-01
Budget End
1988-12-31
Support Year
12
Fiscal Year
1988
Total Cost
Indirect Cost

  Institution

Name
University of Chicago
Department
Type
Schools of Medicine
DUNS #
225410919
City
Chicago
State
IL
Country
United States
Zip Code
60637

  Publications

Han, M; Gurevich, V V; Vishnivetskiy, S A et al. (2001) Crystal structure of beta-arrestin at 1.9 A: possible mechanism of receptor binding and membrane Translocation. Structure 9:869-80
Schubert, C; Hirsch, J A; Gurevich, V V et al. (1999) Visual arrestin activity may be regulated by self-association. J Biol Chem 274:21186-90
Hirsch, J A; Schubert, C; Gurevich, V V et al. (1999) The 2.8 A crystal structure of visual arrestin: a model for arrestin's regulation. Cell 97:257-69
Gaudet, R; Savage, J R; McLaughlin, J N et al. (1999) A molecular mechanism for the phosphorylation-dependent regulation of heterotrimeric G proteins by phosducin. Mol Cell 3:649-60
Vishnivetskiy, S A; Paz, C L; Schubert, C et al. (1999) How does arrestin respond to the phosphorylated state of rhodopsin? J Biol Chem 274:11451-4
Apanovitch, D M; Slep, K C; Sigler, P B et al. (1998) Sst2 is a GTPase-activating protein for Gpa1: purification and characterization of a cognate RGS-Galpha protein pair in yeast. Biochemistry 37:4815-22
Xu, Z; Sigler, P B (1998) GroEL/GroES: structure and function of a two-stroke folding machine. J Struct Biol 124:129-41
Bohm, A; Gaudet, R; Sigler, P B (1997) Structural aspects of heterotrimeric G-protein signaling. Curr Opin Biotechnol 8:480-7
Gaudet, R; Bohm, A; Sigler, P B (1996) Crystal structure at 2.4 angstroms resolution of the complex of transducin betagamma and its regulator, phosducin. Cell 87:577-88
Jiang, Y; Nock, S; Nesper, M et al. (1996) Structure and importance of the dimerization domain in elongation factor Ts from Thermus thermophilus. Biochemistry 35:10269-78

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