A Phase 2, randomized, partially blinded, active-controlled study assessing the efficacy and safety of variable anticoagulation reversal using the REG1 system in patients with acute coronary syndromes: results of the RADAR trial

Povsic, Thomas J.; Vavalle, John P.; Aberle, Laura H.; Kasprzak, Jarosław D.; Cohen, Mauricio G.; Mehran, Roxana; Bode, Christoph; Buller, Christopher E.; Montalescot, Gilles; Cornel, Jan H.; Rynkiewicz, Andrzej; Ring, Michael E.; Zeymer, Uwe; Natarajan, Madhu K.; Delarche, Nicolas; Zelenkofske, Steven L.; Becker, Richard C.; Alexander, John H.

doi:10.1093/eurheartj/ehs232

Cited by 87 publications

(65 citation statements)

References 29 publications

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…Частота тром-ботических осложнений в течение 30 дней в группе RB006/RB007 (все подгруппы) была не-сколько ниже, чем в группе гепарина, однако эти отличия не достигали достоверного уров-ня -3,0% и 5,1% соответственно (p = 0,1). К важным наблюдениям этого исследования сле-дует отнести регистрацию 3 случаев развития аллергических осложнений среди больных, получавших RB006 [21].…”

Section: новые направления в антитромботической терапииunclassified

Aptamers Are New Pharmacological Substances for the Development of Anticoagulants

Мазуров¹,

Спиридонова²

2017

Aterotromboz

View full text Add to dashboard Cite

Аптамеры представляют собой одноце-почечные, короткие ДНК или РНК оли-гонуклеотиды (обычно не более 50-60 нуклеотидных остатков), которые благодаря возможности образовывать сложные простран-ственные конформации обладают способно-стью к специфическому взаимодействию с различными молекулами. Некоторые аптаме-ры могут также ингибировать функциональ-ную активность своих молекулярных мише-ней. Название «аптамер» происходит от латин-ского слова «aptus» -подходить, соответство-вать [1][2][3].Первичные аптамеры получают с помощью метода SELEX (Systematic Evolution of Ligands by EXponential enrichment, системная эволю-ция лигандов с помощью экспоненциального обогащения) путем их отбора из библиотеки случайно синтезированных олигонуклеотидов по способности к связыванию с молекулой-мишенью. Библиотеки со случайной (рандо- АПТАМЕРЫ -НОВЫЕ ФАРМАКОЛОГИЧЕСКИЕ

show abstract

Section: новые направления в антитромботической терапииunclassified

Aptamers Are New Pharmacological Substances for the Development of Anticoagulants

Мазуров¹,

Спиридонова²

2017

Aterotromboz

View full text Add to dashboard Cite

show abstract

“…This dual system allows precise control of the pharmaceutical effects on blood clotting and was designed for the prevention of bleeding within surgical interventions. Early clinical evaluations showed promising results for use as anticoagulation agent during interventions for acute coronary syndrome [66]. A comprehensive Phase III trial, however, had to be terminated in late 2014 because of occurrences of severe anaphylactic reactions.…”

Section: Aptamersmentioning

confidence: 99%

“…A comprehensive Phase III trial, however, had to be terminated in late 2014 because of occurrences of severe anaphylactic reactions. Although a clear proof is lack- 10.4155/fmc.15.94 www.future-science.com future science group Therapeutic oligonucleotides with polyethylene glycol modifications Review ing, it can be speculated that a PEG-reactive antibody mediated mechanism is responsible for the allergic reactions [66]. As stated before, a considerable share of individuals carry antiPEG antibodies, possibly caused by the increasing use of PEG not only in drugs, but also in cosmetics and other consumer products.…”

Section: Aptamersmentioning

confidence: 99%

Therapeutic Oligonucleotides with Polyethylene Glycol Modifications

Winkler

2015

Future Med. Chem.

View full text Add to dashboard Cite

In the field of oligonucleotide drugs, the attachment of PEG is a well-established strategy to prevent enzymatic degradation and avoid renal elimination. Pegaptanib and other oligonucleotides in clinical development utilize the attachment of linear or branched high molecular weight PEG chains for increase of accumulation and duration of the effect after local or systemic application. The length of PEG chains is decisive for the pharmacokinetic and pharmacodynamic effects. Longer chains increase circulation times, but generally decrease gene-silencing efficiencies for antisense and siRNA agents and binding affinities for aptamers. Shorter chains are less efficient in preventing renal filtration, but have also less impact on the gene-silencing machinery and binding kinetics.

show abstract

“…Although this approach does not necessarily lead to a better risk/benefit ratio, its anticoagulant activity can be rapidly and easily controlled by developing a complementary, anti-sense oligonucleotide to neutralize the aptamer. On a clinical basis, this approach has been most fully studied with the factor IX aptamer known as the REG 1 or 2 Anticoagulation System (REG2; Regado Biosciences, Inc., Basking Ridge, NJ) [13,14]. Studies have shown that factor IXa inhibition provides a clinically useful antithrombotic signal [15].…”

Section: Improving the Benefit/risk Of Anticoagulant Drugsmentioning

confidence: 99%

“…In the REG system, pegnivacogin, a nuclease-stabilized RNA aptamer, when given subcutaneously, binds to and inhibits factor IXa with high affinity and specificity and is reversed by its complementary oligonucleotide, anivamersen. Initial studies with intravenous pegnivacogin (REG 1) showed its ability to anticoagulate patients and be reversed by anivamersen in a Phase 2 trial in patients with acute coronary syndromes [13]. A recent first-inhuman study of REG 2 (subcutaneous pegnivacogin) demonstrated its ability to neutralize thrombin generation in a dose response manner with reversal by anivamersen without evidence of rebound effect [14].…”

Section: Improving the Benefit/risk Of Anticoagulant Drugsmentioning

confidence: 99%

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

Ansell

2015

Expert Review of Cardiovascular Therapy

View full text Add to dashboard Cite

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.

show abstract

A Phase 2, randomized, partially blinded, active-controlled study assessing the efficacy and safety of variable anticoagulation reversal using the REG1 system in patients with acute coronary syndromes: results of the RADAR trial

Cited by 87 publications

References 29 publications

Aptamers Are New Pharmacological Substances for the Development of Anticoagulants

Aptamers Are New Pharmacological Substances for the Development of Anticoagulants

Therapeutic Oligonucleotides with Polyethylene Glycol Modifications

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

Contact Info

Product

Resources

About