Antagonists of oxytocin featuring replacement with modified β‐mercaptopropionic acids at position 1

“…Stepwise improvement of OT-R binding affinity, and antagonist potency, as well as OT/AVP receptor selectivity [238,239,240], led to a final compound, 18, termed Antag III, or TT-235 [241] [see Fig. (7)], which is reported to have 90-fold higher affinity for the OT-R than atosiban [242], and to be 50-fold more efficacious in a baboon model of uterine contractions [243].…”

Section: Peptide Antagonistsmentioning

confidence: 98%

Preterm Labour: An Overview of Current and Emerging Therapeutics

Schwarz¹,

Page²

2003

CMC

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Preterm labour is a major cause of perinatal mortality and morbidity. However, during the past 40 years of clinical studies and despite the use of multiple therapeutic agents, the rate of preterm birth has not drastically declined. In 1991, it was estimated that in the US approximately 116,000 women admitted with acute episodes of preterm labour were treated each year with ritodrine, which is the first drug approved by the US FDA and still remains the standard therapy for treating preterm labour. Ritodrine (Yutopar( trade mark )) stimulates the beta(2)-adrenergic receptor throughout the body, causing an inhibitory action in different tissues that, among other side effects, also leads to an attenuation of uterine contractility. More recently, a new therapeutic agent, atosiban (Tractocile( trade mark )), a peptidic oxytocin receptor antagonist, has been introduced to the market. However, the use of the various pharmacological agents to treat preterm labour remains restricted, due to lack of uterine selectivity, low efficacy and potentially serious side effects for the mother or the foetus. Therefore, there is an urgent need to develop drugs with myometrial selectivity that would allow long-lasting inhibition of labour and prolong pregnancy up to a stage when good foetal maturation raises the chances of survival. One of the major obstacles hampering the development of new therapeutic agents is the marked inter-species difference in terms of preterm labour physiology, which complicates the preclinical evaluation of new candidate molecules in animal models of disease. In this review, the authors will provide a comprehensive update of past, current and new approaches for the management of preterm labour, including beta(2)-adrenergic agonists, calcium channel blockers, oxytocin antagonists, prostaglandin antagonists and other potential therapeutics. For each of the therapies used today, the review will cover the mechanism of action, benefit and adverse effects, and discuss the promise and potential benefits of new emerging therapeutic agents.

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“…[18] In contrast, our present method can accomplish the S-benzylation of unprotected mercaptobenzoica cids with benzylic alcohols in water, which is chemoselective andl eaves the carboxyl group intact. However, benzyl halides are chemically unstablea nd their synthesis from benzyla lcohols is achieved by halogenation, which is undesirablef rom an environmental point of view.F urthermore,t he use of excess benzyl halides leads to over-reaction of reactivef unctional groups.…”

Section: Scale-up Experimentsmentioning

confidence: 99%

Direct Use of Benzylic Alcohols for Gold(III)‐Catalyzed S‐Benzylation of Mercaptobenzoic Acids in Water

et al. 2016

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We demonstrate the gold(III)-catalyzed direct substitution of benzylic alcohols in water. These atom economic and environmentally benign protocols afford S-benzylated productsi nm oderate to excellent yields.I nc ontrast, common Lewis or Brønsted acids as catalyst, ando rganic solventss uch as dichloromethane or toluene were ineffectivef or the S-benzylation of mercaptobenzoic acids.W ater can be an attractive toolf or newt ransitionm etalcatalyzed reactions.AHammetts tudy for the rate constants with various substituted alcohols shows ag ood correlation (R 2 = 0.97) between the log(k X / k H )a nd the s + + value of the respective substituents. From the slope negative 1 valueso f2 .35 are ob-tained,s uggesting that there is ab uild-up of positive charge in the transitions tate.O ur catalytic system can be performed with the use of only 2mol% of gold(III) catalyst without any other additives in water, and scaled up to 10 mmol scale (85% isolated yield). Notably,t he present method can accomplish the S-benzylation of unprotected mercaptobenzoic acids,w hich is chemoselective andl eaves the carboxyl group intact. Furthermore,t he direct substitution of allylica nd propargylic alcohols also proceeded smoothlyi ngoody ields.

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Antagonists of oxytocin featuring replacement with modified β‐mercaptopropionic acids at position 1

Cited by 17 publications

References 39 publications

The Lipophilic Bullet Hits the Targets: Medicinal Chemistry of Adamantane Derivatives

The Lipophilic Bullet Hits the Targets: Medicinal Chemistry of Adamantane Derivatives

Preterm Labour: An Overview of Current and Emerging Therapeutics

Direct Use of Benzylic Alcohols for Gold(III)‐Catalyzed S‐Benzylation of Mercaptobenzoic Acids in Water

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