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Effect of hemin and carbon monoxide releasing molecule (CORM-3) on cGMP in rat penile tissue.

The journal of sexual medicine (2008-01-09)
M Talaat Abdel Aziz, M Farid El-Asmar, Taymour Mostafa, Hazem Atta, Hanan H Fouad, Nagwa K Roshdy, Laila A Rashed, Eman A Obaia, Dina A Sabry, Ahmed T Abdel Aziz, George Drummond, Rafal Olszanecki
RESUMEN

Cyclic guanosine monophosphate (cGMP) levels can be regulated by heme oxygenase-1 and 2 (HO-1 and HO-2)-derived carbon monoxide (CO). Assessment of the effect of upregulating CO in rat corpora cavernosa (CC) on cavernous cGMP. Three experimental groups were studied: first group (N = 40), short-term HO induction over 2 weeks by injection of intraperitoneal increasing doses of hemin; the second group (N = 40) was subjected to intracavernosal injection of CO donor, CORM-3, or its inactive form (iCORM-3) over 2 weeks; the third group (N = 60) was subdivided into three subgroups: the first one received a combined hemin and CORM-3, the second one received hemin and its inhibitor stannus mesoporphyrin (SnMP), and third one received a combined hemin, CORM-3, and SnMP. In CC, HO-1 and HO-2 gene expression, Northern blot and Western blot, cGMP levels, and HO enzyme activity. In the first group, maximum induction of HO-1 gene expression, HO enzyme activity, and cGMP occurred with 4-mg hemin dose with a successive increase over 2 weeks. In the second group, CORM-3 increased cGMP by twofold compared with iCORM-3, and also increased HO-1 protein. In the third group, SnMP inhibited the enhancing effect of CORM-3 and HO on erectile signaling molecules; i.e., HO-1 gene, enzyme activity, and cGMP. CORM-3- or hemin-mediated CO release could increase cavernous tissue cGMP.

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Sigma-Aldrich
Mesoporphyrin IX dihydrochloride, synthetic, 95%