Clonal Character of F1 Hybrid Lymphocyte Subset Recognition of Parental Cells in One-way Mixed Lymphocyte Cultures

Overview

Journal J Exp Med

Specialties Allergy & Immunology
General Medicine

Date 1974 Aug 1

PMID 4276945

Citations 2

Authors

B M Gebhardt

Y Nakao

R T Smith

Affiliations

Soon will be listed here.

Abstract

Proliferation of F(1) hybrid lymphocytes in mixed lymphocyte cultures is stimulated by mitomycin-blocked parental cells. The demonstration of this phenomenon using F(1) hybrids derived from congenic lines of mice establishes that the stimulation is controlled by genes in or closely linked to the major histocompatibility locus chromosome region. In agreement with the finding that tumor-bearing mice have an increased capacity for primary alloantigen recognition, it was observed that the F(1) hybrid response to parent was also augmented by tumor bearing. Chromosomal analysis of dividing cells in one-way mixed cultures confirms that F(1) cells, and not the blocked parental cells, enter mitosis. Stimulation of F(1) cells by a soluble mediator liberated by the parental cells was not observed and mitomycin blocking of parental cells seems to be a completely effective blocking agent ensuring that parental cells can not enter DNA synthesis. The specificity and clonal nature of F(1) recognition of parent was demonstrated using a 5-bromodeoxyuridine-suicide procedure. Distinct clones of lymphocytes in F(1) spleen cell populations seem to recognize one or the other parent, but not both, in such experiments. These observations and others in tumor systems suggest that most or all heterozygous organisms may possess potentially self-reactive clones of lymphocytes.

Citing Articles

Study of the cells proliferating in parent versus F hybrid mixed lymphocyte culture.

Piguet P, Dewey H, Vassalli P J Exp Med. 1975; 141(4):775-87.

PMID: 1092790 PMC: 2189745.

Tumor-secific immunity to chemically induced tumors. Evidence for immunologic specificity and shared antigenicity in lymphocyte responses to soluble tumor antigens.

Frbes J, Nakaw Y, Smith R J Exp Med. 1975; 141(5):1181-200.

PMID: 47896 PMC: 2189780. DOI: 10.1084/jem.141.5.1181.

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