Abstract

1 The long-term goal of this proposal is to understand how specific protein:protein interactions regulate the localization and function of protein kinase C (PKC) and protein kinase D (PKD). These two kinase families play pivotal roles in transducing the myriad of extracellular signals that promote phospholipid hydrolysis or, in the case of atypical PKC isozymes, 3'-phosphoinositide generation. We will focus on 1] the C-terminus of PKC as a paradigm for a molecular switch that controls kinase function through specific protein interactions, 2] identifying scaffolds for the atypical PKC isozymes and PKD isozymes, testing the hypothesis that these kinases have PDZ-binding motifs, and 3] uncovering mechanisms for lipid second messenger signaling in the matrix of mitochondria. Specifically, the following Aims are proposed: 1. The C-terminus of PKC as a molecular switch -The goal of this section is to understand how the interaction of specific binding partners with the C-terminal tail of PKC controls the lifecycle of this kinase. In the current funding period, and in collaboration with Pat Jennings (Project 4), we discovered that the prolyl isomerase Pin1 converts PKC into a species that can be degraded following activation.
This Aim focuses on understanding the structural (with Project 4), biochemical, and cellular mechanisms underlying the molecular switch in the C-terminus of PKC. 2. Regulation of atypical PKC and PKD signaling by protein scaffolds - The goal of this section is to understand how protein interactions confer specificity in signaling by atypical PKC isozymes and PKD isozymes. We propose to identify PDZ domain scaffolds for these kinases and test how disruption of scaffolding interactions impact signaling. 3. Signaling at intracellular organelles: the mitochondria! matrix - The hypothesis driving this aim is that lipid second messenger signaling is a key component in mitochondria! function. Taking advantage of the novel genetically-encoded kinase activity reporters we developed in the current funding period, we aim to unambiguously demonstrate kinase activity in the matrix of mitochondria, an unexplored signaling terrain. We ask how disrupting kinase function at this location compromises mitochondria! function.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Program Projects (P01)
Project #
5P01DK054441-13
Application #
8293371
Study Section
Special Emphasis Panel (ZDK1)
Project Start
Project End
2013-03-31
Budget Start
2011-07-01
Budget End
2013-06-30
Support Year
13
Fiscal Year
2011
Total Cost
$360,187
Indirect Cost

  Institution

Name
University of California San Diego
Department
Type
DUNS #
804355790
City
La Jolla
State
CA
Country
United States
Zip Code
92093

  Publications

Flippo, Kyle H; Gnanasekaran, Aswini; Perkins, Guy A et al. (2018) AKAP1 Protects from Cerebral Ischemic Stroke by Inhibiting Drp1-Dependent Mitochondrial Fission. J Neurosci 38:8233-8242
Sengupta, Soham; Nechushtai, Rachel; Jennings, Patricia A et al. (2018) Phylogenetic analysis of the CDGSH iron-sulfur binding domain reveals its ancient origin. Sci Rep 8:4840
Haushalter, Kristofer J; Casteel, Darren E; Raffeiner, Andrea et al. (2018) Phosphorylation of protein kinase A (PKA) regulatory subunit RI? by protein kinase G (PKG) primes PKA for catalytic activity in cells. J Biol Chem 293:4411-4421
Sastri, Mira; Darshi, Manjula; Mackey, Mason et al. (2017) Sub-mitochondrial localization of the genetic-tagged mitochondrial intermembrane space-bridging components Mic19, Mic60 and Sam50. J Cell Sci 130:3248-3260
Smith, F Donelson; Esseltine, Jessica L; Nygren, Patrick J et al. (2017) Local protein kinase A action proceeds through intact holoenzymes. Science 356:1288-1293
Parker, Seth J; Svensson, Robert U; Divakaruni, Ajit S et al. (2017) LKB1 promotes metabolic flexibility in response to energy stress. Metab Eng 43:208-217
Nystoriak, Matthew A; Nieves-CintrĂ³n, Madeline; Patriarchi, Tommaso et al. (2017) Ser1928 phosphorylation by PKA stimulates the L-type Ca2+ channel CaV1.2 and vasoconstriction during acute hyperglycemia and diabetes. Sci Signal 10:
Ilouz, Ronit; Lev-Ram, Varda; Bushong, Eric A et al. (2017) Isoform-specific subcellular localization and function of protein kinase A identified by mosaic imaging of mouse brain. Elife 6:
Nygren, Patrick J; Mehta, Sohum; Schweppe, Devin K et al. (2017) Intrinsic disorder within AKAP79 fine-tunes anchored phosphatase activity toward substrates and drug sensitivity. Elife 6:
Aggarwal-Howarth, Stacey; Scott, John D (2017) Pseudoscaffolds and anchoring proteins: the difference is in the details. Biochem Soc Trans 45:371-379

Showing the most recent 10 out of 216 publications