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Target Concepts:
Gene/Protein
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Query: UNIPROT:P04141 (
granulocyte-macrophage colony-stimulating factor
)
6,790
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
In mouse dorsal skin multistage carcinogenesis models, tumor promotion can be mediated by chemical agents, but also by wounding or abrasion of the epidermis, suggesting that endogenous growth factors mediate this process.
Granulocyte-macrophage colony-stimulating factor
(
GM-CSF
) is one such factor that has been reported to be produced by keratinocytes in vitro, and has been suggested both to stimulate keratinocyte proliferation, and also to be a chemoattractant for neutrophils and macrophages. In this study we examined the expression and function of
GM-CSF
in mouse skin following the application of tumor-promoting agents. Both single and multiple applications of 12-O-tetradecanoylphorbol-13-acetate (TPA) resulted in accumulation of
GM-CSF
mRNA in the epidermis. Various phorbol and non-phorbol ester tumor promoters were found to induce increases in epidermal
GM-CSF
mRNA levels commensurate with their relative tumor promoting capabilities. Fluocinolone acetonide (FA) and tosyl phenylalanine chloromethyl ketone (TPCK), inhibitors of tumor promotion, inhibited tumor promoter-mediated
GM-CSF
accumulation, whereas all-trans-retinoic acid (RA) enhanced the TPA-induced increase. The retinoic acid analogue RO-109359 which, unlike RA, does not have tumor promoting activity per se, inhibited the TPA-induced increase in epidermal
GM-CSF
mRNA levels. When an antibody specific to
GM-CSF
was administered prior to TPA, the promoter-induced dermal inflammation and increase in epidermal dark cell number were reduced, yet promoter-induced epidermal hyperplasia was not. These findings implied that elevation of
GM-CSF
levels plays an important role in chemically-mediated mouse
skin tumor
promotion and principally via effects on promoter-induced inflammation and increased epidermal dark cell number.
...
PMID:Granulocyte-macrophage colony-stimulating factor (GM-CSF) is expressed in mouse skin in response to tumor-promoting agents and modulates dermal inflammation and epidermal dark cell numbers. 814 76
The role of
granulocyte-macrophage colony-stimulating factor
(
GM-CSF
) in tumorigenesis is complex. On the one hand,
GM-CSF
can promote tumor cell growth, survival, and even metastasis. On the other hand, it can stimulate tumor cell rejection. In skin, it is early expressed after topic application of tumor-promoting agents and therefore may be responsible for changes that correlate with
skin tumor
promotion (e.g., epidermal hyperproliferation and inflammation). To analyze
GM-CSF
function in skin tumorigenesis, we generated transgenic mice epidermally overexpressing either
GM-CSF
or a
GM-CSF
antagonist. Both types of transgenic mice exhibited significantly increased numbers of benign tumors in a two-step skin carcinogenesis experiment using 7',12'-dimethylbenz[a]anthracene (DMBA) as initiator and 12-O-tetradecanoylphorbol-CSF displayed a significantly elevated carcinoma burden following a single-step carcinogenesis protocol consisting of tumor initiation only. Therefore, endogenous promotion is responsible for elevated tumor development in
GM-CSF
-overexpressing mice. In antagonist transgenic animals, an increased tumorigenicity of modified B16 tumor cells after cutaneous transplantation as compared with nontransgenic or
GM-CSF
transgenic mice was observed. Thus, the antitumor activity leading to the repression of tumor cell growth in control mice is
GM-CSF
dependent and is compromised in mice expressing the antagonist. We suggest that both, up-regulation and down-regulation of
GM-CSF
activity in skin, increase the incidence and growth of tumors via two independent mechanisms: endogenous tumor promotion in the case of increased
GM-CSF
activity and compromised tumor cell rejection in the case of decreased
GM-CSF
activity.
...
PMID:Up- and down-regulation of granulocyte/macrophage-colony stimulating factor activity in murine skin increase susceptibility to skin carcinogenesis by independent mechanisms. 1128 Aug 4
