Nifedipine kinetics in the rat and relationship between its serum concentrations and uterine and cardiovascular effects

Downing, Sandra J.; Hollingsworth, Michael A.

doi:10.1111/j.1476-5381.1988.tb16544.x

Cited by 9 publications

(15 citation statements)

References 24 publications

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“…Such differences have to be considered since we want to compare free concentrations in humans and rats in vivo with that in cow serum in vitro. Species differences in protein binding have been documented for NIF at least between man and dog (Rosenkranz et al 1974), but not between rat and man (cited in Downing and Hollingsworth 1988), and for DIL, i.e. with 300 ng/ml, between rat plasma (84%) and human plasma (63%) and human serum albumin (40%) and bovine serum albumin (66%) (Nakamura et al 1987).…”

Section: Unsolved Problems and Drawbacks When Attempting Extrapolatiomentioning

confidence: 96%

Effects of calcium channel blockers on the development of early rat postimplantation embryos in culture

et al. 1990

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Rat embryos (9.5-day-old) were cultured for 48 h in the presence of nifedipine (NIF), nimodipine (NIM), nitrendipine (NIT), gallopamil HCl (GAL), verapamil HCl (VER) and diltiazem HCl (DIL). The effects on growth and morphogenetic differentiation in vitro were monitored. Dose-response relationships were evaluated, including an assessment of the "no-observed-effect-level" (NOEL) or the "lowest-observed-effect-level" (LOEL), and the lowest concentration tested inducing abnormalities in 100% of the embryos ("100% EL"). The morphological alterations observed at the highest concentrations were very similar for all six drugs. The abnormalities concerned yolk sac circulation and morphology, as well as heartbeat, the morphology of the heart, head, neural tube, or forelimbs, and the shape of the embryo. The abnormal embryos were also growth retarded (decrease in protein content and crown-rump length). Interference with calcium channel functions seems to represent an interesting model for studying a special kind of abnormal prenatal development, especially the differentiation of certain mesenchymal structures. The concentration ranges between NOELs and 100% ELs were found to be: NIM = 0.1-1 microgram/ml; NIT and VER = 1-10 micrograms/ml; DIL = 1-30 micrograms/ml, and LOELs-100% ELs were: GAL = 1-10 micrograms/ml; NIF = 10-30 micrograms/ml.

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Section: Unsolved Problems and Drawbacks When Attempting Extrapolatiomentioning

confidence: 96%

Effects of calcium channel blockers on the development of early rat postimplantation embryos in culture

et al. 1990

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“…), subjected to bilateral ovariectomy by dorsal laparotomy and equipped with a small latex pressure-recording bal¬ loon inserted into one uterine horn as described pre¬ viously (Downing et al 1987). The rats were then given one of the following treatments commencing on the day of surgery: (a) 0-05 ml corn oil s.c. on days 1 and 2 plus an empty s.c. implant consisting of a 5 cm length of Silastic tubing (internal diameter 1-5 mm outside diameter 200mm; Dow Corning, Midland, MI, U.S.A.) inserted at surgery (control rats); (b) 1-5 nmol oestradiol/kg (Sigma Chemical Co., Poole, Dorset, U.K.) s.c. in 005 ml corn oil on days 1 and 2 plus an empty implant s.c; (c) 005ml corn oil s.c. on days 1 and 2 plus an implant containing approximately 0-2 mmol cystalline progesterone (Sigma Chemical Co.) s.c; (d) 1-5 nmol oestradiol/ kg in 0-05 ml corn oil s.c. on days 1 and 2 plus a progesterone implant s.c.…”

Section: Surgery and Hormone Treatmentmentioning

confidence: 99%

“…The increase in potency of diltiazem observed in rats in late pregnancy, however, is due to factors other than oestrogen and progesterone. The lack of effect of hormonal INTRODUCTION Calcium entry blockers are potent inhibitors of ten¬ sion development by rat uterine smooth muscle in vitro (Granger, Hollingsworth & Weston, 1985, 1986Edwards, Good, Granger et al 1986) and in vivo (Abel & Hollingsworth, 1985, 1986Downing, Edwards & Hollingsworth, 1987; Hollingsworth Downing . We have recently demonstrated a twofold increase in the potency of nifedipine against uterine contractions in rats during late pregnancy compared with nonpregnant rats .…”

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confidence: 99%

The influence of oestrogen and progesterone on the actions of two calcium entry blockers in the rat uterus

Downing

Hollingsworth²,

Miller³

1988

Journal of Endocrinology

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The potency and maximum effect of the calcium entry blocker nifedipine as an inhibitor of uterine contractions in vivo are increased in rats in late pregnant compared with non-pregnant rats. The influence of ovarian steroids produced during pregnancy (oestrogen and progesterone) on the potency and maximum effect of two calcium entry blockers (nifedipine and diltiazem) against uterine contractions during i.v. infusion was therefore investigated in anaesthetized non-pregnant rats. The influence of pregnancy on the relationship between serum concentrations of diltiazem during i.v. infusion and uterine and cardiovascular effects was also investigated. A twofold increase in the potency of nifedipine as an inhibitor of uterine contractions was observed in rats treated with oestrogen or oestrogen plus progesterone compared with rats treated with corn oil. There was no change in potency in rats receiving progesterone alone. Maximum inhibition of uterine contractions by nifedipine was significantly increased by all three hormone treatments. A twofold increase in the potency of diltiazem and a significant increase in maximum inhibition of uterine contractions was observed in rats in late pregnancy compared with non-pregnant rats. No increase in potency of diltiazem in reducing blood pressure or heart rate was observed in rats in late pregnancy. No significant difference in potency of diltiazem against uterine contractions was observed in rats treated with oestrogen, progesterone or oestrogen plus progesterone.(ABSTRACT TRUNCATED AT 250 WORDS)

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“…We planned administration of a dose regimen via osmotic pumps which provided a plasma nifedipine concentration of ~1.5 µg/ml (estimated). Downing and Hollingsworth (1998) concluded that this plasma level of the drug did not cause significant changes in heart rate or blood pressure, but elicited a well-defined uterus-relaxing effect. We found that treatment with nifedipine alone started on pregnancy day 16 was more effective in delaying delivery than salmeterol treatment alone (in the earlier study) (Gálik et al, 2008).…”

Section: Discussionmentioning

confidence: 99%

“…The in vivo dose for the tocolytic effect was calculated by using the pharmacokinetic parameters reported for nifedipine in pregnant rats by Downing et al (Downing and Hollingsworth, 1998). We planned administration of a dose regimen via osmotic pumps which provided a plasma nifedipine concentration of ~1.5 µg/ml (estimated).…”

Section: Discussionmentioning

confidence: 99%

Modification of the myometrial relaxing effect of nifedipine in vitro and in vivo

Hajagos-Tóth¹

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Nifedipine kinetics in the rat and relationship between its serum concentrations and uterine and cardiovascular effects

Cited by 9 publications

References 24 publications

Effects of calcium channel blockers on the development of early rat postimplantation embryos in culture

Effects of calcium channel blockers on the development of early rat postimplantation embryos in culture

The influence of oestrogen and progesterone on the actions of two calcium entry blockers in the rat uterus

Modification of the myometrial relaxing effect of nifedipine in vitro and in vivo

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