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Increases in placental nitric oxide, but not nitric oxide‐mediated relaxation, underlie the improvement in placental efficiency and antihypertensive effects of hydrogen sulphide donor in hypertensive pregnancy
Author(s) -
PossomatoVieira Jose S.,
Chimini Jessica S.,
Silva Maria L. S.,
DiasJunior Carlos A.
Publication year - 2018
Publication title -
clinical and experimental pharmacology and physiology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.752
H-Index - 103
eISSN - 1440-1681
pISSN - 0305-1870
DOI - 10.1111/1440-1681.13000
Subject(s) - nitric oxide , endocrinology , medicine , pregnancy , placenta , blood pressure , preeclampsia , fetus , sodium nitroprusside , chemistry , biology , genetics
Summary Dysregulation of hydrogen sulphide (H 2 S) producing enzymes has been related to hypertensive pregnancy, and H 2 S donor, sodium hydrosulphide (Na HS ) exerts antihypertensive effects, modulates angiogenic factors production and acts as an antioxidant. Moreover, reduction in nitric oxide ( NO ) bioavailability is related to hypertensive pregnancy and H 2 S may interact with NO , modulating its production. We aimed to investigate the Na HS effects in hypertension‐in‐pregnancy and also in feto‐placental parameters. Female Wistar rats (200‐250 g) were mated and desoxycorticosterone acetate injections followed by replacement of water by 0.9% saline solution were used to induce hypertensive pregnancy. Rats were divided into four groups: normal pregnant (Norm‐Preg), pregnant + Na HS (Preg+Na HS ), hypertensive pregnant ( HTN ‐Preg) and HTN ‐Preg+Na HS . Systolic blood pressure was increased in HTN ‐Preg and this increase was blunted in HTN ‐Preg+Na HS . Fetal and placental weights were decreased in HTN ‐Preg animals, while fetal growth restriction was improved in HTN ‐Preg+Na HS . Placental weight was lower in HTN ‐Preg+Na HS than in HTN ‐Preg; however, placental efficiency was re‐established in HTN ‐Preg+Na HS rats. We observed that a partial contribution of placental NO , but not changes in anti‐angiogenic factors may mediate the increases in placental efficiency in HTN ‐Preg+Na HS . HTN ‐Preg presented thoracic aorta hyperreactivity to phenylephrine while Na HS treatment blunted this hyperreactivity, which seems not to be related to NO ‐mediated relaxation induced by acetylcholine. Therefore, changes in vascular responsiveness promoted by Na HS treatment may underlie the beneficial effects in systolic blood pressure and feto‐placental parameters in our study.

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