Role of Dimerization of the Membrane-associated Growth Factor Kit Ligand in Juxtacrine Signaling: The Sl (17H) Mutation Affects Dimerization and Stability—Phenotypes in Hematopoiesis

The Kit ligand (KL)/Kit receptor pair functions in hematopoiesis, gametogenesis, and melanogenesis. KL is encoded at the murine steel (Sl) locus and encodes a membrane growth factor which may be proteolytically processed to produce soluble KL. The membrane-associated form of KL is critical in mediat...

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Autores principales: Tajima, Youichi, Huang, Eric J., Vosseller, Keith, Ono, Masao, Moore, Malcolm A.S., Besmer, Peter
Formato: Texto
Lenguaje:English
Publicado: The Rockefeller University Press 1998
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2212272/
https://www.ncbi.nlm.nih.gov/pubmed/9565637
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author Tajima, Youichi
Huang, Eric J.
Vosseller, Keith
Ono, Masao
Moore, Malcolm A.S.
Besmer, Peter
author_facet Tajima, Youichi
Huang, Eric J.
Vosseller, Keith
Ono, Masao
Moore, Malcolm A.S.
Besmer, Peter
author_sort Tajima, Youichi
collection PubMed
description The Kit ligand (KL)/Kit receptor pair functions in hematopoiesis, gametogenesis, and melanogenesis. KL is encoded at the murine steel (Sl) locus and encodes a membrane growth factor which may be proteolytically processed to produce soluble KL. The membrane-associated form of KL is critical in mediating Kit function in vivo. Evidence for a role of cytoplasmic domain sequences of KL comes from the Sl (17H) mutation, a splice site mutation that replaces the cytoplasmic domain with extraneous amino acids. Using deletion mutants and the Sl (17H) allele, we have investigated the role of the cytoplasmic domain sequences of KL in biosynthetic processing and cell surface presentation. The normal KL protein products are processed for cell surface expression, where they form dimers. Both Sl (17H) and the cytoplasmic deletion mutants of KL were processed to the cell surface; however, the rate of transport and protein stability were affected by the mutations. Deletion of cytoplasmic domain sequences of KL did not affect dimerization of KL. In contrast, dimerization of the Sl (17H) protein was reduced substantially. In addition, we have characterized the hematopoietic cell compartment in Sl (17H) mutant mice. The Sl (17H) mutation has only minor effects on hematopoiesis. Tissue and peritoneal mast cell numbers were reduced in mutant mice as well as in myeloid progenitors. Interestingly, long-term bone marrow cultures from Sl (17H) mice did not sustain the long-term production of hematopoietic cells. In addition, homing of normal hematopoietic progenitors to the spleen of irradiated Sl (17H)/Sl (17H) recipient mice was diminished in transplantation experiments, providing evidence for a role of Kit in homing or lodging. These results demonstrate that the membrane forms of KL exist as homodimers on the cell surface and that dimerization may play an important role in KL/Kit-mediated juxtacrine signaling.
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spelling pubmed-22122722008-04-16 Role of Dimerization of the Membrane-associated Growth Factor Kit Ligand in Juxtacrine Signaling: The Sl (17H) Mutation Affects Dimerization and Stability—Phenotypes in Hematopoiesis Tajima, Youichi Huang, Eric J. Vosseller, Keith Ono, Masao Moore, Malcolm A.S. Besmer, Peter J Exp Med Article The Kit ligand (KL)/Kit receptor pair functions in hematopoiesis, gametogenesis, and melanogenesis. KL is encoded at the murine steel (Sl) locus and encodes a membrane growth factor which may be proteolytically processed to produce soluble KL. The membrane-associated form of KL is critical in mediating Kit function in vivo. Evidence for a role of cytoplasmic domain sequences of KL comes from the Sl (17H) mutation, a splice site mutation that replaces the cytoplasmic domain with extraneous amino acids. Using deletion mutants and the Sl (17H) allele, we have investigated the role of the cytoplasmic domain sequences of KL in biosynthetic processing and cell surface presentation. The normal KL protein products are processed for cell surface expression, where they form dimers. Both Sl (17H) and the cytoplasmic deletion mutants of KL were processed to the cell surface; however, the rate of transport and protein stability were affected by the mutations. Deletion of cytoplasmic domain sequences of KL did not affect dimerization of KL. In contrast, dimerization of the Sl (17H) protein was reduced substantially. In addition, we have characterized the hematopoietic cell compartment in Sl (17H) mutant mice. The Sl (17H) mutation has only minor effects on hematopoiesis. Tissue and peritoneal mast cell numbers were reduced in mutant mice as well as in myeloid progenitors. Interestingly, long-term bone marrow cultures from Sl (17H) mice did not sustain the long-term production of hematopoietic cells. In addition, homing of normal hematopoietic progenitors to the spleen of irradiated Sl (17H)/Sl (17H) recipient mice was diminished in transplantation experiments, providing evidence for a role of Kit in homing or lodging. These results demonstrate that the membrane forms of KL exist as homodimers on the cell surface and that dimerization may play an important role in KL/Kit-mediated juxtacrine signaling. The Rockefeller University Press 1998-05-04 /pmc/articles/PMC2212272/ /pubmed/9565637 Text en This article is distributed under the terms of an Attribution–Noncommercial–Share Alike–No Mirror Sites license for the first six months after the publication date (see http://www.rupress.org/terms). After six months it is available under a Creative Commons License (Attribution–Noncommercial–Share Alike 4.0 Unported license, as described at http://creativecommons.org/licenses/by-nc-sa/4.0/).
spellingShingle Article
Tajima, Youichi
Huang, Eric J.
Vosseller, Keith
Ono, Masao
Moore, Malcolm A.S.
Besmer, Peter
Role of Dimerization of the Membrane-associated Growth Factor Kit Ligand in Juxtacrine Signaling: The Sl (17H) Mutation Affects Dimerization and Stability—Phenotypes in Hematopoiesis
title Role of Dimerization of the Membrane-associated Growth Factor Kit Ligand in Juxtacrine Signaling: The Sl (17H) Mutation Affects Dimerization and Stability—Phenotypes in Hematopoiesis
title_full Role of Dimerization of the Membrane-associated Growth Factor Kit Ligand in Juxtacrine Signaling: The Sl (17H) Mutation Affects Dimerization and Stability—Phenotypes in Hematopoiesis
title_fullStr Role of Dimerization of the Membrane-associated Growth Factor Kit Ligand in Juxtacrine Signaling: The Sl (17H) Mutation Affects Dimerization and Stability—Phenotypes in Hematopoiesis
title_full_unstemmed Role of Dimerization of the Membrane-associated Growth Factor Kit Ligand in Juxtacrine Signaling: The Sl (17H) Mutation Affects Dimerization and Stability—Phenotypes in Hematopoiesis
title_short Role of Dimerization of the Membrane-associated Growth Factor Kit Ligand in Juxtacrine Signaling: The Sl (17H) Mutation Affects Dimerization and Stability—Phenotypes in Hematopoiesis
title_sort role of dimerization of the membrane-associated growth factor kit ligand in juxtacrine signaling: the sl (17h) mutation affects dimerization and stability—phenotypes in hematopoiesis
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2212272/
https://www.ncbi.nlm.nih.gov/pubmed/9565637
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