First-in-Human Experience of an Antidote-Controlled Anticoagulant Using RNA Aptamer Technology. A Phase 1a Pharmacodynamic Evaluation of a Drug-Antidote Pair for the Controlled Regulation of Factor IXa Activity

doi:10.1161/CIRCULATIONAHA.106.668434

Published Online
on November 13, 2006

Circulation. 2006
Published online before print November 13, 2006, doi: 10.1161/CIRCULATIONAHA.106.668434

A more recent version of this article appeared on December 5, 2006
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Submitted on October 5, 2006
Revised on October 24, 2006
Accepted on October 27, 2006

First-in-Human Experience of an Antidote-Controlled Anticoagulant Using RNA Aptamer Technology. A Phase 1a Pharmacodynamic Evaluation of a Drug-Antidote Pair for the Controlled Regulation of Factor IXa Activity

Christopher K. Dyke MD^*, Steven R. Steinhubl MD, Neal S. Kleiman MD, Richard O. Cannon MD, Laura G. Aberle MS, Min Lin PhD, Shelley K. Myles BS, RN, Chiara Melloni MD, Robert A. Harrington MD, John H. Alexander MD, Richard C. Becker MD, and Christopher P. Rusconi PhD

From the Duke Clinical Research Institute, Durham, NC (C.K.D., L.G.A., A.L., S.K.M., C.M., R.A.H., J.H.A., R.C.B.); University of Kentucky, Lexington (S.R.S.); Methodist DeBakey Heart Center, Houston, Tex (N.S.K.); National Heart, Lung, and Blood Institute, Bethesda, Md (R.O.C.); and Regado Biosciences, Inc, Durham, NC (C.P.R). Dr Dyke is now affiliated with the Alaska Heart Institute, Anchorage, Alaska.

^* To whom correspondence should be addressed. E-mail: cdyke{at}alaskaheart.com.

Background--Selectivity, titratability, rapidity of onset, andactive reversibility are desirable pharmacological propertiesof anticoagulant therapy administered for acute indicationsand collectively represent an attractive platform to maximizepatient safety. A novel anticoagulation system (REG1, RegadoBiosciences), developed using a protein-binding oligonucleotideto factor IXa (drug, RB006) and its complementary oligonucleotideantidote (RB007), was evaluated in healthy volunteers. The primaryobjective was to determine the safety profile and to characterizethe pharmacodynamic responses in this first-in-human study.

Methodsand Results--Regado 1a was a subject-blinded, dose-escalation,placebo-controlled study that randomized 85 healthy volunteersto receive a bolus of drug or placebo followed 3 hours laterby a bolus of antidote or placebo. Pharmacodynamic samples werecollected serially. Subject characteristics were the following:median age, 32 years (interquartile range, 23 to 39 years);female gender, 35%; and median weight, 79 kg (interquartilerange, 70 to 87 kg). No significant differences were found inmedian hemoglobin, platelet, creatinine, or liver function studies.There were no significant bleeding signals associated with RB006,and overall, both drug and antidote were well tolerated. Oneserious adverse event, an episode of transient encephalopathy,occurred in a subject receiving the low intermediate dose ofRB006. The subject’s symptoms resolved rapidly, and nofurther sequelae occurred. A predictable dose-pharmacodynamicresponse, reflected in activated partial thromboplastin timemeasurements, was seen after administration of the bolus ofdrug, with a clear correlation between the peak posttreatmentactivated partial thromboplastin time and post hoc weight-adjusteddose of drug (correlation coefficient, 0.725; P<0.001). Insubjects treated with drug, antidote administration reversedthe pharmacological activity of the drug, with a rapid (meantime, 1 to 5 minutes across all dose levels) and sustained returnof activated partial thromboplastin time to within the normalrange. The activated clotting time followed a similar anticoagulantresponse and reversal pattern. As anticipated, prothrombin timeremained unchanged compared with baseline.

Conclusions--Theseobservations represent a first-in-human experience of an RNAaptamer and its complementary oligonucleotide antidote usedas an anticoagulant system. The findings contribute to an emergingplatform of selective, actively reversible anticoagulant drugsfor use among patients with thrombotic disorders of the venousand arterial circulations.

Key words: anticoagulants • coagulation • pharmacology • aptamers, nucleotide • thrombosis • trials

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