| Literature DB >> 25503118 |
Pamela Ehrenfeld1, Lorella Manso2, María F Pavicic3, Carola E Matus3, Carlos Borquez3, Alejandro Lizama3, José Sarmiento4, María T Poblete3, Kanti D Bhoola5, Anupan Naran2, Carlos D Figueroa3.
Abstract
The sera of patients with breast cancer have higher levels of des[Arg(9)]bradykinin, a kinin B1 receptor (B1R) agonist, than that from healthy individuals. Stimulation of breast cancer cells with the analog Lys-des[Arg(9)]bradykinin causes release of metalloproteinases-2 and -9 and increases cell proliferation. We examined the possibility that breast cancer cells, in addition to B1R, express the kinin-forming protease true tissue kallikrein (KLK1) and the endogenous proteins termed kininogens from which kinins are enzymatically released. Furthermore, we investigated whether stimulation of breast cancer cells with a B1R agonist would modify the cellular levels of KLK6, KLK10 and KLK11, three kallikrein-related peptidases with a still poorly-understood biological role in breast cancer. We found that breast cancer cells expressed KLK1 and kininogens, and that stimulation of estrogen-sensitive breast cancer cells with the B1R agonist produced down-regulation of KLK10 (a protease associated with growth suppression) but up-regulation of KLK11 and KLK6 (peptidases related to increased cell proliferation and invasiveness, respectively). Furthermore, we showed that the B1R agonist acts as a functional stimulus for the secretion of KLK1 and KLK6, an event relevant for kinin production and cell invasion, respectively. CopyrightEntities:
Keywords: Breast cancer; KLK10; KLK11; KLK6; estrogen; kallikrein-related peptidases; kinin B1 receptor; tissue kallikrein (KLK1)
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Year: 2014 PMID: 25503118
Source DB: PubMed Journal: Anticancer Res ISSN: 0250-7005 Impact factor: 2.480