John C. Resendez scite author profile

John C. Resendez

5Publications

40Citation Statements Received

0Citation Statements Given

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Affiliations

MPI Research (United States), Charles River Laboratories (United States)

Publications

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Barusiban, A New Highly Potent and Long-Acting Oxytocin Antagonist: Pharmacokinetic and Pharmacodynamic Comparison with Atosiban in a Cynomolgus Monkey Model of Preterm Labor

Reinheimer

Bee²,

Resendez³

et al. 2005

The Journal of Clinical Endocrinology & Metabolism

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Preterm labor (PTL) represents a significant unmet clinical need that affects up to 20% of all pregnancies and is a leading cause of preterm delivery and associated neonatal morbidity and mortality. Therapeutic options are limited, with existing drug therapy (tocolytics) compromised by side effects and limited efficacy. Because oxytocin (OT) is likely to be involved causally in PTL, this study compared two OT receptor antagonists, barusiban and atosiban, for their tocolytic effects. OT was given to instrumented pregnant cynomolgus monkeys to induce contractions and simulate PTL. Barusiban or atosiban was then given iv (bolus or infusion) to evaluate inhibitory effects on uterine contractions, measured by telemetric recording of intrauterine pressure. Both antagonists had high efficacy (96-98% inhibition of intrauterine pressure) and rapid onset of action (0.5-1.5 h). Barusiban was three to four times more potent than atosiban, which was attributed to its higher affinity and selectivity for the OT receptor. Barusiban also had a much longer duration of action (>13-15 h, compared with 1-3 h for atosiban). The inhibitory effects of barusiban were reversible within 1.5-2.5 h by high-dose OT infusion. Overall, barusiban's improved potency, long duration of action, and reversibility may provide an improved tocolytic for treatment of PTL.

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Barusiban, An Effective Long-Term Treatment of Oxytocin-Induced Preterm Labor in Nonhuman Primates1

Reinheimer

Chellman

Resendez

et al. 2006

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Preterm labor (PTL) affects up to 25% of human pregnancies in developing countries, but there are few therapeutic options. Based on the key role of oxytocin (OXT) in labor and parturition, OXT antagonists are a potentially useful class of drugs for PTL. Barusiban is a new selective, potent, and long-acting OXT receptor antagonist. In this study barusiban was given by continuous i.v. infusion to monkeys during the last 3 wk of pregnancy; the monkeys were also given daily doses of OXT to induce uterine contractions and simulate PTL. Barusiban effectively suppressed OXT-induced PTL-like contractions and prevented early delivery. In contrast, fenoterol (a beta2-adrenoceptor [beta2-AR] agonist used as a comparative control) did not inhibit uterine contractions in this model. Barusiban was particularly effective in maintaining low intrauterine pressure (IUP) near the end of pregnancy, which is when IUP in both OXT controls and fenoterol-treated females increased substantially. Although barusiban delayed the onset of labor, it did not prevent normal delivery. These data demonstrate the safety and efficacy of barusiban in reducing uterine contractility in response to repeated OXT challenge, and suggest that barusiban may be therapeutically effective in long-term treatment of PTL.

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Telemetric uterine contraction model in preterm cynomolgus monkeys

Chellman¹,

Bee²,

Resendez³

et al. 2004

Reproductive Toxicology

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VALIDATION OF METHODS TO ASSESS RESPIRATORY FUNCTION, PLEURAL PRESSURE AND DIAPHRAGM EMGs IN NHPs

Gauvin

Resendez

Moddrelle

et al. 2007

Journal of Pharmacological and Toxicological Methods

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Lymphocyte immunophenotyping and t-dependent antibody response in naïve and KLH-challenged juvenile cynomolgus monkeys

2011

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John C. Resendez

Barusiban, A New Highly Potent and Long-Acting Oxytocin Antagonist: Pharmacokinetic and Pharmacodynamic Comparison with Atosiban in a Cynomolgus Monkey Model of Preterm Labor

Barusiban, An Effective Long-Term Treatment of Oxytocin-Induced Preterm Labor in Nonhuman Primates1

Telemetric uterine contraction model in preterm cynomolgus monkeys

VALIDATION OF METHODS TO ASSESS RESPIRATORY FUNCTION, PLEURAL PRESSURE AND DIAPHRAGM EMGs IN NHPs

Lymphocyte immunophenotyping and t-dependent antibody response in naïve and KLH-challenged juvenile cynomolgus monkeys

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