TRIM37 defective in mulibrey nanism is a novel RING finger ubiquitin E3 ligase

Kallijaervi, Jukka; Lahtinen, Ulla; Haemaelaeinen, Riikka; Lipsanen-Nyman, Marita; Palvimo, Jorma J; Lehesjoki, Anna-Elina

doi:10.1016/j.yexcr.2005.04.001

Title: TRIM37 defective in mulibrey nanism is a novel RING finger ubiquitin E3 ligase

Journal Article · Mon Aug 01 00:00:00 EDT 2005 · Experimental Cell Research

DOI:https://doi.org/10.1016/j.yexcr.2005.04.001· OSTI ID:20717636

Kallijaervi, Jukka ^[1]; Lahtinen, Ulla ^[1]; Haemaelaeinen, Riikka ^[1]; Lipsanen-Nyman, Marita ^[2]; Palvimo, Jorma J ^[3]; Lehesjoki, Anna-Elina ^[1]

Folkhaelsan Institute of Genetics, Department of Medical Genetics and Neuroscience Center, Biomedicum Helsinki, 00014 University of Helsinki (Finland)
The Hospital for Children and Adolescents and Helsinki University Central Hospital (Finland)
Institute of Biomedicine, 00014 University of Helsinki (Finland)

Mulibrey nanism is an autosomal recessive prenatal-onset growth disorder characterized by dysmorphic features, cardiomyopathy, and hepatomegaly. Mutations in TRIM37 encoding a tripartite motif (TRIM, RING-B-box-coiled-coil)-family protein underlie mulibrey nanism. We investigated the ubiquitin ligase activity predicted for the RING domain of TRIM37 by analyzing its autoubiquitination. Full-length TRIM37 and its TRIM domain were highly polyubiquitinated when co-expressed with ubiquitin. Polyubiquitination was decreased in a mutant protein with disrupted RING domain (Cys35Ser;Cys36Ser) and in the Leu76Pro mutant protein, a disease-associated missense mutation affecting the TRIM domain of TRIM37. Bacterially produced GST-TRIM domain fusion protein, but not its Cys35Ser;Cys36Ser or Leu76Pro mutants, were polyubiquitinated in cell-free conditions, implying RING-dependent modification. Ubiquitin was also identified as an interaction partner for TRIM37 in a yeast two-hybrid screen. Ectopically expressed TRIM37 rapidly formed aggregates that were ubiquitin-, proteasome subunit-, and chaperone-positive in immunofluorescence analysis, defining them as aggresomes. The Cys35Ser;Cys36Ser mutant and the Leu76Pro and Gly322Val patient mutant proteins were markedly less prone to aggregation, implying that aggresomal targeting reflects a physiological function of TRIM37. These findings suggest that TRIM37 acts as a TRIM domain-dependent E3 ubiquitin ligase and imply defective ubiquitin-dependent degradation of an as-yet-unidentified target protein in the pathogenesis of mulibrey nanism.

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OSTI ID:: 20717636

Journal Information:: Experimental Cell Research, Vol. 308, Issue 1; Other Information: DOI: 10.1016/j.yexcr.2005.04.001; PII: S0014-4827(05)00165-5; Copyright (c) 2005 Elsevier Science B.V., Amsterdam, The Netherlands, All rights reserved; Country of input: International Atomic Energy Agency (IAEA); ISSN 0014-4827

Country of Publication:: United States

Language:: English

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