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Different Role of cAMP Pathway on the Human Mast Cells HMC‐1 560 and HMC‐1 560,816 Activation
Author(s) -
BarreiroCosta Olalla,
Tobío Araceli,
Alfonso Amparo,
Botana Luis M.
Publication year - 2014
Publication title -
journal of cellular biochemistry
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.028
H-Index - 165
eISSN - 1097-4644
pISSN - 0730-2312
DOI - 10.1002/jcb.24732
Subject(s) - rolipram , ibmx , histamine , forskolin , ionomycin , histamine h2 receptor , chemistry , wortmannin , microbiology and biotechnology , camp dependent pathway , endocrinology , medicine , signal transduction , protein kinase a , receptor , biology , phosphodiesterase , kinase , biochemistry , enzyme , pi3k/akt/mtor pathway , in vitro , antagonist
HMC‐1 are inflammatory cells that release vasoactive substances such as histamine. These cells have the c‐kit receptor permanently activated in the membrane due to mutations in the proto‐oncogene c‐kit: Val‐560 → Gly and Asp‐816 → Val. Thus, there are two known cellular lines: HMC‐1 560 and HMC‐1 560,816 . These mutations are involved in a disease called mastocitosys. In the present paper both lines were used to study the influence of cAMP/PKA/PDEs pathway on the histamine release and Ca 2+ signaling since this pathway is often involved in these process. For this, the cells were preincubated with cAMP/PKA/PDEs modulators such as dibutyryl cAMP (dbcAMP), forskolin, H89, rolipram, IBMX, or imidazole and then stimulated with ionomycin. When cells were stimulated with agents that increase cAMP levels, the histamine release was not modified in HMC‐1 560 but decreased in HMC‐1 560,816 cells. The same happened when PKA was blocked. Furthermore, PDEs role on histamine release was independent of cAMP in HMC‐1 560 cells and possibly also in HMC‐1 560,816 cells. By contrast, the modulation of PKA and PDEs together changed the response in both cellular lines, therefore a relationship between them was suggested. All these modulatory effects on histamine release are Ca 2+ ‐independent. On the other hand, the effect of c‐kit modulation on the cAMP/PKA/PDEs pathway was also checked. This receptor was blocked with STI571 (imatinib) and BMS‐354825 (dasatinib), but only the last one caused a decrease in the cellular response to ionomycin. This article demonstrates for the first time than the cAMP/PKA/PDEs pathway is involved in the activation of HMC‐1 560 and HMC‐1 560,816 cells. J. Cell. Biochem. 115: 896–909, 2014. © 2013 Wiley Periodicals, Inc.