Polycystin-2 Interacts with Troponin I, an Angiogenesis Inhibitor

19 December 2002

journal article
Published by American Chemical Society (ACS) in Biochemistry

Vol. 42 (2) , 450-457
https://doi.org/10.1021/bi0267792

Abstract

Polycystin-2 (PC2), encoded by the PKD2 gene, is mutated in 10−15% of autosomal dominant polycystic kidney disease (ADPKD) patients. PC2 is a Ca²⁺-permeable nonselective cation channel and is present in kidney and many other organs. Likewise, PKD2-mutated patients and mice exhibit extrarenal abnormalities. In comparison with cysts in the kidney, liver, and pancreas, abnormalities in the heart, brain, and vascular vessels are less understood. In particular, roles of PC2 in muscle and endothelia remain largely unknown. In the present study, using a yeast two-hybrid screening, we discovered that the PC2 carboxyl terminal domain (D682-V968) interacts with the cardiac troponin I, an important regulatory component of the actin microfilament in cardiac muscle cells. This interaction was demonstrated by GST pull-down and microtiter binding assays. Dose-dependent binding between PC2 and troponin I followed a Michaelis−Menten relationship, indicating a 1:1 binding stoichiometry. The interacting domains were located to the R872−H927 segment of PC2 and the M1−V107 and K106−L158 segments of troponin I. Co-immunoprecipitation experiments demonstrated that the cardiac and two skeletal isoforms of troponin I were all associated with PC2, when coexpressed in mouse fibroblast NIH 3T3 cells and Xenopus oocytes. Furthermore, reciprocal co-immunoprecipitation verified the interaction between the native polycystin-2 and troponin I in human adult heart tissues. This study thus provides new evidence for a direct attachment of PC2 to the actin microfilament network, in addition to the recently identified association between PC2 and trypomyosin-1. Troponin I functions as an inhibitory subunit of the troponin complex for calcium-dependent regulation of muscle contraction and as an inhibitor of angiogenesis seen in ADPKD. It is possible that altered interaction due to pathogenic polycystin-1 or -2 mutations can account for angiogenesis in ADPKD and may be corrected to some extent by exogenous troponin I.

Keywords

This publication has 12 references indexed in Scilit:

Identification, Characterization, and Localization of a Novel Kidney Polycystin-1-Polycystin-2 Complex
Journal of Biological Chemistry, 2002
Troponin I converts the skeletal muscle ryanodine receptor into a rectifying calcium release channel
FEBS Letters, 2002
Troponin I Inhibits Capillary Endothelial Cell Proliferation by Interaction with the Cell's bFGF Receptor
Microvascular Research, 2002
Angiogenesis in autosomal-dominant polycystic kidney disease
Kidney International, 2001
In Vivo Interaction of the Adapter Protein CD2-associated Protein with the Type 2 Polycystic Kidney Disease Protein, Polycystin-2
Journal of Biological Chemistry, 2000
Cardiac Troponin I Gene Knockout
Circulation Research, 1999
Carbonic Anhydrase II Binds to the Carboxyl Terminus of Human Band 3, the Erythrocyte Cl−/HCO3−Exchanger
Journal of Biological Chemistry, 1998
Isolation and Characterization of the Human Cardiac Troponin I Gene (TNNI3)
Genomics, 1996
Autosomal Dominant Polycystic Kidney Disease
New England Journal of Medicine, 1993
Molecular cloning of human cardiac troponin I using polymerase chain reaction
FEBS Letters, 1990