A small-molecule factor XIa inhibitor produces antithrombotic efficacy with minimal bleeding time prolongation in rabbits

Wong, Pancras C.; Crain, Earl J.; Watson, Carol A.; Schumacher, William A.

doi:10.1007/s11239-011-0599-0

Cited by 69 publications

(51 citation statements)

References 44 publications

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“…Strategies to inhibit FXI are illustrated in Table 2 and include (1) ASOs that reduce hepatic synthesis of the clotting protein 27,33,44 ; (2) monoclonal antibodies that block FXI activation, FXIa activity, or both 25,45,46 ; (3) aptamers that block FXI activation or activity 47,48 ; and (4) small molecules that block the active site of FXIa [49][50][51] or induce allosteric modulation.…”

Section: Strategies To Inhibit Fximentioning

confidence: 99%

2017 Scientific Sessions Sol Sherry Distinguished Lecture in Thrombosis

Weitz

Fredenburgh

2018

ATVB

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Abstract-The goal of anticoagulant therapy is to attenuate thrombosis without compromising hemostasis. Although the direct oral anticoagulants are associated with less intracranial hemorrhage than vitamin K antagonists, bleeding remains their major side effect. Factor XI has emerged as a promising target for anticoagulants that may be safer than those currently available. The focus on factor XI stems from epidemiological evidence of its role in thrombosis, the observation of attenuated thrombosis in factor XI-deficient mice, identification of novel activators, and the fact that factor XI deficiency is associated with only a mild bleeding diathesis. Proof-of-concept comes from the demonstration that compared with enoxaparin, factor XI knockdown reduces venous thromboembolism without increasing bleeding after elective knee arthroplasty. This article rationalizes the selection of factor XI as a target for new anticoagulants, reviews the agents under development, and outlines a potential path forward for their development. Visual Overview-An online visual overview is available for this article. (Arterioscler Thromb Vasc Biol. 2018;38: 304-310.

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Section: Strategies To Inhibit Fximentioning

confidence: 99%

2017 Scientific Sessions Sol Sherry Distinguished Lecture in Thrombosis

Weitz

Fredenburgh

2018

ATVB

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“…It is well known that factor XI deficiency is not associated with a major bleeding phenotype [19], but clinical evidence also supports the finding that factor XI deficiency is associated with a reduced risk of stroke and deep vein thrombosis [20]. Based on these clinical insights, investigators have studied the effect of inhibiting [21] or lowering factor XI levels [22]. The latter effort is achieved by specific antisense Factor XI oligonucleotides that selectively inhibit factor XI mRNA expression [22,23].…”

Section: Improving the Benefit/risk Of Anticoagulant Drugsmentioning

confidence: 96%

Is there a need for an alternative in the era of novel anticoagulants?

Ansell

2015

Expert Review of Cardiovascular Therapy

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With the development of the new direct oral anticoagulants, many of the unmet needs of the vitamin K antagonists were fulfilled, such as the absence of dietary interactions, few drug interactions, predictable effects and no need for monitoring. However, growing experience with the direct oral anticoagulants indicates there is still room for improvement. Developing antithrombotic agents that optimize their antithrombotic effect while producing little or no risk of bleeding is a long sought after goal. This and other enhanced attributes of candidate drugs are on the horizon.

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“…The lead BMS-3543326 (48) was deeply studied as inhibitor of Factor XIa and it was evaluated in vivo on arterial thrombosis and hemostasis in rat and rabbits, as above reported [58]. This new compound has the potential to complement established parenteral anticoagulants [60]. In a recent review, the pharmacology of some new parenteral anticoagulants, the results of clinical studies, the newly planned or ongoing clinical trials with these compounds, and their potential advantages and drawbacks over existing therapies were discussed [61].…”

Section: N-acyl-azetidinonesmentioning

confidence: 98%

Monocyclic β-Lactams: New Structures for New Biological Activities

Galletti

Giacomini

2011

CMC

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The azetidinone core-structure offers a unique approach to the design and synthesis of new derivatives with unique biological properties. During the last two decades researches convincingly demonstrated that the prospect of structural modifications of monocyclic β-lactams with specific substituents is an effective procedure for the detection and improvement of important pharmacological effects different from antibacterial activity. As a matter of fact, new β-lactam compounds demonstrated biological activity as inhibitors of a wide range of enzymes. This review reports the latest developments on monocyclic β-lactam compounds activity as anticancer, antitubercular, HFAAH inhibitors, HDAC inhibitors, anti-inflammatory drugs (tryptase inhibitors), Cathepsin K inhibitors, and vasopressin inhibitors. We attempted to highlight the intertwined relationships between structural features and biological activities, by analysing groups anchored on the three positions of the azetidinone ring as sources of molecular diversity.

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A small-molecule factor XIa inhibitor produces antithrombotic efficacy with minimal bleeding time prolongation in rabbits

Cited by 69 publications

References 44 publications

2017 Scientific Sessions Sol Sherry Distinguished Lecture in Thrombosis

2017 Scientific Sessions Sol Sherry Distinguished Lecture in Thrombosis

Is there a need for an alternative in the era of novel anticoagulants?

Monocyclic β-Lactams: New Structures for New Biological Activities

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A small-molecule factor XIa inhibitor produces antithrombotic efficacy with minimal bleeding time prolongation in rabbits

Cited by 69 publications

References 44 publications

2017 Scientific Sessions Sol Sherry Distinguished Lecture in Thrombosis

2017 Scientific Sessions Sol Sherry Distinguished Lecture in Thrombosis

Is there a need for an alternative in the era of novel anticoagulants?

Monocyclic &#946;-Lactams: New Structures for New Biological Activities

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Monocyclic β-Lactams: New Structures for New Biological Activities