Role of UEV-1, an Inactive Variant of the E2 UbiquitinConjugating Enzymes, in In Vitro Differentiation and Cell Cycle Behavior of HT-29-M6 Intestinal Mucosecretory Cells

Author:

Sancho Elena1,Vilá Maya R.1,Sánchez-Pulido Luis2,Lozano Juan José3,Paciucci Rosanna1,Nadal Marga4,Fox Margaret5,Harvey Clare15,Bercovich Brenda6,Loukili Nourredine1,Ciechanover Aaron6,Lin Stanley L.7,Sanz Ferran3,Estivill Xavier4,Valencia Alfonso2,Thomson Timothy M.1

Affiliation:

1. Departamento de Biologı́a Molecular, Instituto de Biologı́a del Cáncer, IMIM-CSIC,1

2. Protein Design Group, Centro Nacional de Biotecnologı́a-CSIC, Cantoblanco, Madrid, 2 Spain;

3. Grup de Recerca en Informàtica Mèdica, IMIM-UAB, Barcelona, 3 and

4. Departamento de Genètica Humana, Institut de Recerca Oncològica, 4 Barcelona, and

5. MRC Human Biochemical Genetics Unit, University College London, London, England 5 ;

6. Department of Biochemistry, Faculty of Medicine, Technion-Israel Institute of Technology, Haifa, Israel 6 ; and

7. Department of Psychiatry, UMDNJ-Robert Wood Johnson Medical School, Piscataway, New Jersey7

Abstract

ABSTRACT By means of differential RNA display, we have isolated a cDNA corresponding to transcripts that are down-regulated upon differentiation of the goblet cell-like HT-29-M6 human colon carcinoma cell line. These transcripts encode proteins originally identified as CROC-1 on the basis of their capacity to activate transcription of c- fos . We show that these proteins are similar in sequence, and in predicted secondary and tertiary structure, to the ubiquitin-conjugating enzymes, also known as E2. Despite the similarities, these proteins lack a critical cysteine residue essential for the catalytic activity of E2 enzymes and, in vitro, they do not conjugate or transfer ubiquitin to protein substrates. These proteins constitute a distinct subfamily within the E2 protein family and are highly conserved in phylogeny from yeasts to mammals. Therefore, we have designated them UEV (ubiquitin-conjugating E2 enzyme variant) proteins, defined as proteins similar in sequence and structure to the E2 ubiquitin-conjugating enzymes but lacking their enzymatic activity (HW/GDB-approved gene symbol, UBE2V). At least two human genes code for UEV proteins, and one of them, located on chromosome 20q13.2, is expressed as at least four isoforms, generated by alternative splicing. All human cell types analyzed expressed at least one of these isoforms. Constitutive expression of exogenous human UEV in HT-29-M6 cells inhibited their capacity to differentiate upon confluence and caused both the entry of a larger proportion of cells in the division cycle and an accumulation in G 2 -M. This was accompanied with a profound inhibition of the mitotic kinase, cdk1. These results suggest that UEV proteins are involved in the control of differentiation and could exert their effects by altering cell cycle distribution.

Publisher

American Society for Microbiology

Subject

Cell Biology,Molecular Biology

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