Journal
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA
Volume 112, Issue 23, Pages E3000-E3009Publisher
NATL ACAD SCIENCES
DOI: 10.1073/pnas.1504671112
Keywords
VEPH1; TGF-beta; SMAD2/3; Melted; ALK5
Categories
Funding
- Canadian Institutes of Health Research Grant [MOP74726]
- Kristi Piia Callum Memorial Fellowship
- Frank Fletcher Memorial Fund
- Teresina Florio Graduate Scholarship
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Drosophila melted encodes a pleckstrin homology (PH) domain-containing protein that enables normal tissue growth, metabolism, and photoreceptor differentiation by modulating Forkhead box O (FOXO), target of rapamycin, and Hippo signaling pathways. Ventricular zone expressed PH domain-containing 1 (VEPH1) is the mammalian ortholog of melted, and although it exhibits tissue-restricted expression during mouse development and is potentially amplified in several human cancers, little is known of its function. Here we explore the impact of VEPH1 expression in ovarian cancer cells by gene-expression profiling. In cells with elevated VEPH1 expression, transcriptional programs associated with metabolism and FOXO and Hippo signaling were affected, analogous to what has been reported for Melted. We also observed altered regulation of multiple transforming growth factor-beta (TGF-beta) target genes. Global profiling revealed that elevated VEPH1 expression suppressed TGF-beta-induced transcriptional responses. This inhibitory effect was verified on selected TGF-beta target genes and by reporter gene assays in multiple cell lines. We further demonstrated that VEPH1 interacts with TGF-beta receptor I (T beta RI) and inhibits nuclear accumulation of activated Sma- and Mad-related protein 2 (SMAD2). We identified two T beta RI- interacting regions TIRs) with opposing effects on TGF-beta signaling. TIR1, located at the N terminus, inhibits canonical TGF-beta signaling and promotes SMAD2 retention at TaRI, similar to full-length VEPH1. In contrast, TIR2, located at the C-terminal region encompassing the PH domain, decreases SMAD2 retention at TaRI and enhances TGF-beta signaling. Our studies indicate that VEPH1 inhibits TGF-beta signaling by impeding the release of activated SMAD2 from T beta RI and may modulate TGF-beta signaling during development and cancer initiation or progression.
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