Literature DB >> 2553734

Arsenite inhibits two steps in the ubiquitin-dependent proteolytic pathway.

N S Klemperer1, C M Pickart.   

Abstract

Eukaryotic cells possess a multienzyme ATP-dependent proteolytic pathway in which the small, highly conserved protein ubiquitin (Ub) acts as a cofactor. In this pathway, formation of a covalent Ub-substrate conjugate precedes ATP-dependent degradation of the substrate. Inorganic arsenite (AsO2-) inhibited Ub-dependent protein degradation in a concentration-dependent fashion, both in intact rabbit reticulocytes and in a reticulocyte lysate (fraction II). Concentrations of arsenite causing half-maximal inhibition in fraction II varied with the substrate, ranging from 0.025 mM (bovine alpha-lactalbumin) to 3.3 mM (reduced/carboxymethylated bovine serum albumin). Inhibition was rapidly reversed upon addition of dithiothreitol. Arsenite inhibited the Ub-dependent proteolytic pathway at one or both of two steps, depending on the substrate. 1) Proteins with acidic amino termini must be amino terminally arginylated, in a tRNA-dependent reaction, prior to becoming conjugated to Ub (Ferber, S., and Ciechanover, A. (1987) Nature 326, 808-811). Arsenite inhibited substrate arginylation, and therefore also inhibited Ub conjugation. The inhibited species appeared to be arginyl aminoacyl-tRNA transferase, since arsenite was without strong effect on the rate or extent of arginyl-tRNA formation in fraction II, yet almost completely inhibited arginine transfer from arginyl-tRNA to reduced/carboxymethylated bovine serum albumin. 2) Arsenite also inhibited Ub-substrate conjugate turnover, as shown in pulse-chase experiments. For a given substrate, degradative (protease-dependent) and Ub regenerative (isopeptidase-dependent) components of conjugate turnover were similarly inhibited by arsenite. The potency of this inhibition varied for different substrates. Monosubstituted trivalent arsenicals such as arsenite typically interact with sites containing vicinal sulfhydryl groups. Inhibition by arsenite of two steps in the Ub-dependent proteolytic pathway suggests that the relevant pathway components could possess this kind of structural/catalytic feature.

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Year:  1989        PMID: 2553734

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  12 in total

1.  Suppression of sodium arsenite-potentiated cytotoxicity of ultraviolet light by cycloheximide in Chinese hamster ovary cells.

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3.  Effects of Arsenic on Trichloroethene-Dechlorination Activities of Dehalococcoides mccartyi 195.

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4.  A Na+:H+ antiporter and a molybdate transporter are essential for arsenite oxidation in Agrobacterium tumefaciens.

Authors:  Des R Kashyap; Lina M Botero; Corinne Lehr; Daniel J Hassett; Timothy R McDermott
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Review 6.  Molecular mechanisms of arsenic carcinogenesis.

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7.  Mitotic arrest-associated apoptosis induced by sodium arsenite in A375 melanoma cells is BUBR1-dependent.

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8.  A novel UBA and UBX domain protein that binds polyubiquitin and VCP and is a substrate for SAPKs.

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9.  Examining the function and regulation of hsp 70 in cells subjected to metabolic stress.

Authors:  R P Beckmann; M Lovett; W J Welch
Journal:  J Cell Biol       Date:  1992-06       Impact factor: 10.539

10.  Overexpression of ubiquitin and amino acid permease genes in association with antimony resistance in Leishmania tropica field isolates.

Authors:  Elham Kazemi-Rad; Mehdi Mohebali; Mohammad Bagher Khadem-Erfan; Homa Hajjaran; Ramtin Hadighi; Ali Khamesipour; Sassan Rezaie; Mojtaba Saffari; Reza Raoofian; Mansour Heidari
Journal:  Korean J Parasitol       Date:  2013-08-30       Impact factor: 1.341

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