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An Increase in Circulating Mast Cell Colony-Forming Cells in Asthma
Author(s) -
Hadija Hemed Mwamtemi,
Kenichi Koike,
Tatsuya Kinoshita,
Susumu Ito,
Shuichi Ishida,
Yozo Nakazawa,
Yumi Kurokawa,
Koji Shinozaki,
Kazuo Sakashita,
Kouichi Takeuchi,
Masaaki Shiohara,
Takehiko Kamijo,
Yozo Yasui,
Akira Ishiguro,
Yoshifumi Kawano,
Kiyoshi Kitano,
Hiroshi Miyazaki,
Takashi Kato,
Shozo Sakuma,
Atsushi Komiyama
Publication year - 2001
Publication title -
the journal of immunology
Language(s) - Uncategorized
Resource type - Journals
SCImago Journal Rank - 2.737
H-Index - 372
eISSN - 1550-6606
pISSN - 0022-1767
DOI - 10.4049/jimmunol.166.7.4672
Subject(s) - stem cell factor , cd34 , tryptase , chymase , degranulation , mast cell , haematopoiesis , progenitor cell , histamine , immunology , stem cell , biology , chemistry , medicine , endocrinology , microbiology and biotechnology , receptor
We compared a potential to generate mast cells among various sources of CD34(+) peripheral blood (PB) cells in the presence of stem cell factor (SCF) with or without thrombopoietin (TPO), using a serum-deprived liquid culture system. From the time course of relative numbers of tryptase-positive and chymase-positive cells in the cultured cells grown by CD34(+) PB cells of nonasthmatic healthy individuals treated with G-CSF, TPO appears to potentiate the SCF-dependent growth of mast cells without influencing the differentiation into mast cell lineage. CD34(+) PB cells from asthmatic patients in a stable condition generated significantly more mast cells under stimulation with SCF alone or SCF+TPO at 6 wk of culture than did steady-state CD34(+) PB cells of normal controls. Single-cell culture studies showed a substantial difference in the number of SCF-responsive or SCF+TPO-responsive mast cell progenitors in CD34(+) PB cells between the two groups. In the presence of TPO, CD34(+) PB cells from asthmatic children could respond to a suboptimal concentration of SCF to a greater extent, compared with the values obtained by those of normal controls. Six-week cultured mast cells of asthmatic subjects had maturation properties (intracellular histamine content and tryptase/chymase enzymatic activities) similar to those derived from mobilized CD34(+) PB cells of nonasthmatic subjects. An increase in a potential of circulating hemopoietic progenitors to differentiate into mast cell lineage may contribute to the recruitment of mast cells toward sites of asthmatic mucosal inflammation.

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