Julius Remenar
Cornell University
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Featured researches published by Julius Remenar.
Molecular Pharmaceutics | 2014
Julius Remenar
There are now long-acting versions of six antipsychotic drugs on the U.S. market, and with them, five unique combinations of molecular form and delivery strategy long-acting-injectable-antipsychotics (LAIAs) show evidence of reduced relapses of schizophrenia, but their introduction has been slow, taking at least nine years after the approval of each oral drug. Oily solutions of lipophilic prodrugs were the first to enter the LAIA market, but they relied on esterification of a hydroxyl handle that was lost with the emergence of the atypical antipsychotics. A review of the literature and patents shows that companies tested many different approaches before reaching the currently marketed versions, including aqueous suspensions of poorly soluble salts, polymeric microspheres, and new approaches to making prodrugs. Yet, very little has been published to support faster development of safe long-acting injectables (LAIs). This review introduces some of the critical considerations in creating an LAI; then it analyzes the existing products and discusses areas where further research is needed. The available literature suggests that lipophilic prodrugs may be inherently safer than poorly soluble salts as LAIs. Other areas needing additional study include (1) the range of physical properties acceptable for LAIs and the effect of prodrug tail length in achieving them, and (2) the role of physiological responses at the injection site in the release of drug from a depot.
Current Opinion in Infectious Diseases | 2015
Magali B. Hickey; Elaine Merisko-Liversidge; Julius Remenar; Mark Namchuk
Purpose of review Treatment of chronic disease in a manner that promotes compliance and patient adherence has necessitated the consideration for drug delivery approaches that reduce the burden of regimens requiring daily treatment. Long-acting injectable (LAI) products have been developed in many disease areas and are now being exploited for the treatment of infectious disease, most notably HIV. Recent findings Research published over the past 3 years has shown that LAI nanosuspensions of nonnucleoside reverse transcriptase inhibitors and integrase inhibitors provide extended exposure to the active drug over a period of days to weeks. Some of these candidates are currently in clinical study and are highly anticipated medications for the prevention of HIV. Summary LAIs represent a growing need in the treatment of chronic infections. To date, the approach has been most successfully applied in the treatment of HIV, but could certainly be expanded into other diseases like tuberculosis. Most importantly, LAIs can provide a means to help prevent the emergence of resistance which may be attributed to lack of compliance to regimens requiring daily, oral administration.
Journal of the American Chemical Society | 2003
Julius Remenar; Sherry L. Morissette; Matthew L. Peterson; Brian Moulton; J. Michael Macphee; and Héctor R. Guzmán; Orn Almarsson
European Journal of Pharmaceutics and Biopharmaceutics | 2007
Magali B. Hickey; Matthew L. Peterson; Lisa Scoppettuolo; Sherry L. Morrisette; Anna Vetter; Hector Guzmán; Julius Remenar; Zhong Zhang; Mark Tawa; Sean Haley; Michael J. Zaworotko; Orn Almarsson
Journal of Pharmaceutical Sciences | 2007
Hector Guzman; Mark Tawa; Zhong Zhang; Pasut Ratanabanangkoon; Paul E. Shaw; Colin R. Gardner; Hongming Chen; Jean‐Pierre Moreau; Orn Almarsson; Julius Remenar
Molecular Pharmaceutics | 2007
Julius Remenar; Matthew L. Peterson; Peter W. Stephens; Zhong Zhang; Yuri Zimenkov; Magali B. Hickey
Journal of the American Chemical Society | 1997
Julius Remenar; Brett L. Lucht; David B. Collum
Archive | 2005
Hector Guzman; Julius Remenar; Orn Almarsson
Archive | 2003
Mark Tawa; Oern Almarsson; Julius Remenar
Archive | 2003
Mark Tawa; Julius Remenar; Matthew L. Peterson; Orn Almarsson; Hector Guzman; Hongming Chen; Mark Oliveira