Abstract

Two different types of human mast cells have been identified and distinguished from basophils based primarily on the neutral protease composition of their secretory granules. The MCrc type of mast cell contains tryptase, chymase, cathepsin 6-like protease and mast cell carboxypeptidase; the MCr type contains only tryptase; and basophils contain negligible to undetectable amounts of these proteases. Each cell type also exhibits special ultrastructural features and distributions within their host.
Aim 1 will investigate the special constituents of human mast cells and basophils. The proteoglycan type(s) will be determined along with the expression of tryptase and chymase protein and mRNA in different types of human mast cells and basophils. We expect to determine whether mature and developing MCt and MCrc cells contain the same proteoglycan species, whether these mast cell subtypes differ in chymase mRNA content, like protein content, and whether in situ hybridization for tryptase or chymase mRNA identifies committed mast cell progenitors prior to protein expression and distinguishes activated from resting mast cells, and to clone and sequence an apparently unique constituent of human basophils.
Aim 2 will examine the growth, differentiation and survival of different types of human mast cells and basophils. These studies are based in part on the important new finding that stem cell factor (Kit ligand) is a major growth factor for human mast cells. Initially the focus will be on IL-4, interferons alpha and gamma and various steroids. Effects on FcepsilonRI and Kit expression, on proteases and histamine, and selectivity for MCt cells, MCrc cells and basophils will be studied. Finally, the capacity of murine and human fibroblasts to complete the maturation of stem cell factor-dependent mast cells will be examined.
Aim 3 will determine the involvement of different types of human mast cells and basophils in human diseases, using techniques developed in previous aims. Also, a means by which mast cell progenitor frequency in the peripheral blood can be assessed will be devised and used to analyze peripheral blood patients with diseases with mast cell hyperplasia (systemic mastocytosis), depletion (AIDS) and activation (allergic rhinitis). Better characterization of mast cells and basophils will provide more precise means to measure and monitor. their involvement in human disease, and better strategies for therapeutic interventions.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI027517-07
Application #
2063884
Study Section
Allergy and Immunology Study Section (ALY)
Project Start
1988-12-01
Project End
1999-03-31
Budget Start
1995-04-01
Budget End
1996-03-31
Support Year
7
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
Virginia Commonwealth University
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
City
Richmond
State
VA
Country
United States
Zip Code
23298

  Publications

Le, Quang Trong; Lotfi-Emran, Sahar; Min, Hae-Ki et al. (2014) A simple, sensitive and safe method to determine the human ?/?-tryptase genotype. PLoS One 9:e114944
Alvarez-Twose, I; Vano-Galvan, S; Sanchez-Munoz, L et al. (2012) Increased serum baseline tryptase levels and extensive skin involvement are predictors for the severity of mast cell activation episodes in children with mastocytosis. Allergy 67:813-21
Ward, Brant R; Arslanian, Silva A; Andreatta, Elisa et al. (2012) Obesity is not linked to increased whole-body mast cell burden in children. J Allergy Clin Immunol 129:1164-6
Le, Quang T; Gomez, Gregorio; Zhao, Wei et al. (2011) Processing of human protryptase in mast cells involves cathepsins L, B, and C. J Immunol 187:1912-8
Le, Quang T; Min, Hae-Ki; Xia, Han-Zhang et al. (2011) Promiscuous processing of human alphabeta-protryptases by cathepsins L, B, and C. J Immunol 186:7136-43
Teodosio, Cristina; García-Montero, Andrés C; Jara-Acevedo, María et al. (2010) Mast cells from different molecular and prognostic subtypes of systemic mastocytosis display distinct immunophenotypes. J Allergy Clin Immunol 125:719-26, 726.e1-726.e4
Zhao, Wei; Gomez, Gregorio; Yu, Shao-Hua et al. (2008) TGF-beta1 attenuates mediator release and de novo Kit expression by human skin mast cells through a Smad-dependent pathway. J Immunol 181:7263-72
Fukuoka, Yoshihiro; Xia, Han-Zhang; Sanchez-Munoz, Laura B et al. (2008) Generation of anaphylatoxins by human beta-tryptase from C3, C4, and C5. J Immunol 180:6307-16
Sabato, M Fernanda; Irani, Anne-Marie; Bukaveckas, Bonny L et al. (2008) A simple and rapid genotyping assay for simultaneous detection of two ADRB2 allelic variants using fluorescence resonance energy transfer probes and melting curve analysis. J Mol Diagn 10:258-64
Gomez, Gregorio; Jogie-Brahim, Sherryline; Shima, Mika et al. (2007) Omalizumab reverses the phenotypic and functional effects of IgE-enhanced Fc epsilonRI on human skin mast cells. J Immunol 179:1353-61

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