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Dive into the research topics where Vu Truong-Le is active.

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Featured researches published by Vu Truong-Le.


Journal of Pharmaceutical Sciences | 2011

Biophysical Characterization and Conformational Stability of Ebola and Marburg Virus-Like Particles

Lei Hu; Jared M. Trefethen; Yuhong Zeng; Luisa Yee; Satoshi Ohtake; David Lechuga-Ballesteros; Kelly L. Warfield; M. Javad Aman; Sergey Shulenin; Robert Unfer; Sven Enterlein; Vu Truong-Le; David B. Volkin; Sangeeta B. Joshi; C. Russell Middaugh

The filoviruses, Ebola virus and Marburg virus, cause severe hemorrhagic fever with up to 90% human mortality. Virus-like particles of EBOV (eVLPs) and MARV (mVLPs) are attractive vaccine candidates. For the development of stable vaccines, the conformational stability of these two enveloped VLPs produced in insect cells was characterized by various spectroscopic techniques over a wide pH and temperature range. Temperature-induced aggregation of the VLPs at various pH values was monitored by light scattering. Temperature/pH empirical phase diagrams (EPDs) of the two VLPs were constructed to summarize the large volume of data generated. The EPDs show that both VLPs lose their conformational integrity above about 50°C-60°C, depending on solution pH. The VLPs were maximally thermal stable in solution at pH 7-8, with a significant reduction in stability at pH 5 and 6. They were much less stable in solution at pH 3-4 due to increased susceptibility of the VLPs to aggregation. The characterization data and conformational stability profiles from these studies provide a basis for selection of optimized solution conditions for further vaccine formulation and long-term stability studies of eVLPs and mVLPs.


Journal of Pharmaceutical Sciences | 2011

Formulation and Stabilization of Francisella tularensis Live Vaccine Strain

Satoshi Ohtake; Russell A. Martin; Atul Saxena; David Lechuga-Ballesteros; Araceli E. Santiago; Eileen M. Barry; Vu Truong-Le

Francisella tularensis live vaccine strain (F. tularensis LVS), a promising vaccine candidate for protection against F. tularensis exposure, is a particularly thermolabile vaccine and difficult to stabilize sufficiently for storage under refrigerated conditions. Our preliminary data show that F. tularensis LVS can be stabilized in the dried state using foam drying, a modified freeze drying method, with sugar-based formulations. The process was conducted under mild drying conditions, which resulted in a good titer retention following processing. The inclusion of osmolytes in the growth media resulted in an acceleration of growth kinetics, although no change in osmotolerance was observed. The optimized F. tularensis formulation, which contained trehalose, gelatin, and Pluronic F68 demonstrated stability for approximately 1.5 weeks at 37°C (i.e., time required for the vaccine to decrease in potency by 1 log(10) colony forming unit) and for 12 weeks at 25°C. At refrigerator storage condition (4°C), stabilized F. tularensis LVS vaccine exhibited no activity loss for at least 12 weeks. This stabilization method utilizes conventional freeze dryers and pharmaceutically approved stabilizers, and thus can be readily implemented at many manufacturing sites for large-scale production of stabilized vaccines. The improved heat stability of the F. tularensis LVS could mitigate risks of vaccine potency loss during long-term storage, shipping, and distribution.


Archive | 2003

Preservation of bioactive materials by spray drying

Vu Truong-Le; Binh Pham


Journal of Pharmaceutical Sciences | 2007

Drying-induced variations in physico-chemical properties of amorphous pharmaceuticals and their impact on stability (I): stability of a monoclonal antibody.

Ahmad M. Abdul‐Fattah; Vu Truong-Le; Luisa Yee; Lauren Nguyen; Devendra S. Kalonia; Marcus T. Cicerone; Michael J. Pikal


Pharmaceutical Research | 2007

Drying-induced variations in physico-chemical properties of amorphous pharmaceuticals and their impact on Stability II: stability of a vaccine.

Ahmad M. Abdul-Fattah; Vu Truong-Le; Luisa Yee; Emilie Pan; Yi Ao; Devendra S. Kalonia; Michael J. Pikal


Protein Expression and Purification | 2005

Expression and characterization of a low molecular weight recombinant human gelatin: development of a substitute for animal-derived gelatin with superior features

David R. Olsen; Jenny Jiang; Robert C. Chang; Robert Duffy; Masahiro Sakaguchi; Scott D. Leigh; Robert P. Lundgard; Julia Ju; Frank Buschman; Vu Truong-Le; Binh Pham; James W. Polarek


Vaccine | 2011

Room Temperature Stabilization of Oral, Live Attenuated Salmonella enterica serovar Typhi-Vectored Vaccines

Satoshi Ohtake; Russell A. Martin; Atul Saxena; Binh Pham; Gary Chiueh; Manuel Osorio; Dennis J. Kopecko; De-Qi Xu; David Lechuga-Ballesteros; Vu Truong-Le


Advanced Drug Delivery Reviews | 2015

Stabilization Challenges and Formulation Strategies Associated with Oral Biologic Drug Delivery Systems

Vu Truong-Le; Phillip M. Lovalenti; Ahmad M. Abdul‐Fattah


Archive | 2004

Methods of producing inflenza vaccine compositions

George Robert Trager; George Kemble; Richard Schwartz; Harshvardhan Mehta; Vu Truong-Le; Zhongying Chen; Alfred A. Pan; Eric Tsao; Chiaoyin Kathy Wang; Luisa Yee; Palani Balu


Archive | 2010

Methods and Compositions for Stabilization of a Virus Vaccine

Satoshi Ohtake; Vu Truong-Le; Luisa Yee; Russell A. Martin; David Lechuga-Ballesteros

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Satoshi Ohtake

University of Wisconsin-Madison

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