AFAP-110 is overexpressed in prostate cancer and contributes to tumorigenic growth by regulating focal contacts
Jing Zhang, … , Daniel C. Flynn, Gary E. Gallick
Jing Zhang, … , Daniel C. Flynn, Gary E. Gallick
Published October 1, 2007
Citation Information: J Clin Invest. 2007;117(10):2962-2973. https://doi.org/10.1172/JCI30710.
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Research Article Oncology

AFAP-110 is overexpressed in prostate cancer and contributes to tumorigenic growth by regulating focal contacts

Abstract

The actin filament–associated protein AFAP-110 is an actin cross-linking protein first identified as a substrate of the viral oncogene v-Src. AFAP-110 regulates actin cytoskeleton integrity but also functions as an adaptor protein that affects crosstalk between Src and PKC. Here we investigated the roles of AFAP-110 in the tumorigenic process of prostate carcinoma. Using immunohistochemistry of human tissue arrays, we found that AFAP-110 was absent or expressed at very low levels in normal prostatic epithelium and benign prostatic hyperplasia but significantly increased in prostate carcinomas. The level of AFAP-110 in carcinomas correlated with the Gleason scores. Downregulation of AFAP-110 in PC3 prostate cancer cells inhibited cell proliferation in vitro and tumorigenicity and growth in orthotopic nude mouse models. Furthermore, downmodulation of AFAP-110 resulted in decreased cell-matrix adhesion and cell migration, defective focal adhesions, and reduced integrin β1 expression. Reintroduction of avian AFAP-110 or a mutant disabling its interaction with Src restored these properties. However, expression of an AFAP-110 lacking the PKC-interacting domain failed to restore properties of parental cells. Thus, increased expression of AFAP-110 is associated with progressive stages of prostate cancer and is critical for tumorigenic growth, in part by regulating focal contacts in a PKC-dependent mechanism.

Authors

Jing Zhang, Serk In Park, Marlene C. Artime, Justin M. Summy, Ami N. Shah, Joshua A. Bomser, Andrea Dorfleutner, Daniel C. Flynn, Gary E. Gallick

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Figure 7

Model for effects of AFAP-110 overexpression on deregulation of prostate cancer cell functions.

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Model for effects of AFAP-110 overexpression on deregulation of prostate...
(A) AFAP-110 directly associates with PKC and the actin cytoskeleton. Overexpression of AFAP-110 interferes with PKC signaling pathways that affect integrin expression and intracellular localization, which are essential for focal adhesion formation, and subsequent cell activities. (B) In normal and benign hyperplasic epithelium, AFAP-110 is expressed at a very low level, and mainly in the basal layer cells, facilitating the formation of focal adhesions where these cells interact with basal membrane components. During the development of prostate cancer, the expression of AFAP-110 increases, contributing to the alteration in the expression and function of integrins, which mediate cancer cell–ECM interactions and propagate signaling pathways essential in tumorigenic growth and invasive progression.