An Unexpectedly Labile Mitochondrially Encoded Protein is Required for Mta Expression

Overview

Journal Immunogenetics

Specialties Allergy & Immunology
Genetics

Date 1989 Jan 1

PMID 2703259

Citations 3

Authors

A C Han

J R Rodgers

R R Rich

Affiliations

Soon will be listed here.

Abstract

Maternally transmitted antigen (Mta) is a mouse major histocompatibility antigen recognized by cytotoxic T lymphocytes. A role for mitochondria in expression of this class I-like cell surface antigen has been previously established. We now show that a labile product of mitochondrial protein synthesis is required for Mta expression. Reexpression of Mta determinants after enzymatic removal occurred within 24 h, and the regeneration process was sensitive to chloramphenicol (CAP), a selective inhibitor of mitochondrial protein synthesis. Additionally, target cells treated with CAP for as little as 18 h showed diminished expression of Mta. The estimated half-life for Mtf products ranged from 6 to 15 h, less than the half-lives of known mitochondrial translation products. This suggests that the Mtf product is not generated by the normal turnover of stable mitochondrial respiratory proteins. Instead, these results indicate the existence of either labile unknown mitochondrially encoded peptides or a rapid turnover pathway for known mitochondrial products.

Citing Articles

Specialized functions of MHC class I molecules. I. An N-formyl peptide receptor is required for construction of the class I antigen Mta.

Shawar S, Cook R, Rodgers J, Rich R J Exp Med. 1990; 171(3):897-912.

PMID: 2307936 PMC: 2187787. DOI: 10.1084/jem.171.3.897.

Specialized function of the nonclassical MHC class I molecule Hmt: a specific receptor for N-formylated peptides.

Shawar S, Rodgers J, Cook R, Rich R Immunol Res. 1991; 10(3-4):365-75.

PMID: 1835490 DOI: 10.1007/BF02919723.

Generation of T cells with lytic specificity for atypical antigens. I. A mitochondrial antigen in the rat.

Davies J, Wilson D, Hermel E, Lindahl K, Butcher G, Wilson D J Exp Med. 1991; 173(4):823-32.

PMID: 1672544 PMC: 2190809. DOI: 10.1084/jem.173.4.823.

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