T

Trung Van Nguyen

St. Jude Children's Research Hospital

ORCID: 0000-0003-3363-5064

Publishes on Sperm and Testicular Function, Reproductive Biology and Fertility, Gastrointestinal motility and disorders. 94 papers and 2.9k citations.

94Publications
2.9kTotal Citations
Sperm and Testicular FunctionReproductive Biology and FertilityGastrointestinal motility and disordersOvarian function and disordersNeuroscience and Neuropharmacology Research

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Top publicationsby citations

Engineered Thio-Trastuzumab-DM1 Conjugate with an Improved Therapeutic Index to Target Human Epidermal Growth Factor Receptor 2–Positive Breast Cancer
Jagath R. Junutula, Kelly M. Flagella, Richard Graham et al.|Clinical Cancer Research|2010
Cited by 292

PURPOSE: Antibody drug conjugates (ADCs) combine the ideal properties of both antibodies and cytotoxic drugs by targeting potent drugs to the antigen-expressing tumor cells, thereby enhancing their antitumor activity. Successful ADC development for a given target antigen depends on optimization of antibody selection, linker stability, cytotoxic drug potency, and mode of linker-drug conjugation to the antibody. Here, we systematically examined the in vitro potency as well as in vivo preclinical efficacy and safety profiles of a heterogeneous preparation of conventional trastuzumab-mcc-DM1 (TMAb-mcc-DM1) ADC with that of a homogeneous engineered thio-trastuzumab-mpeo-DM1 (thioTMAb-mpeo-DM1) conjugate. EXPERIMENTAL DESIGN AND RESULTS: To generate thioTMAb-mpeo-DM1, one drug maytansinoid 1 (DM1) molecule was conjugated to an engineered cysteine residue at Ala114 (Kabat numbering) on each trastuzumab-heavy chain, resulting in two DM1 molecules per antibody. ThioTMAb-mpeo-DM1 retained similar in vitro anti-cell proliferation activity and human epidermal growth factor receptor 2 (HER2) binding properties to that of the conventional ADC. Furthermore, it showed improved efficacy over the conventional ADC at DM1-equivalent doses (μg/m(2)) and retained efficacy at equivalent antibody doses (mg/kg). An improved safety profile of >2-fold was observed in a short-term target-independent rat safety study. In cynomolgus monkey safety studies, thioTMAb-mpeo-DM1 was tolerated at higher antibody doses (up to 48 mg/kg or 6,000 μg DM1/m(2)) compared with the conventional ADC that had dose-limiting toxicity at 30 mg/kg (6,000 μg DM1/m(2)). CONCLUSIONS: The engineered thioTMAb-mpeo-DM1 with broadened therapeutic index represents a promising antibody drug conjugate for future clinical development of HER2-positive targeted breast cancer therapies.

The Enteric Nervous System and Its Extrinsic Connections
John B. Furness, Trung Van Nguyen, Kulmira Nurgali et al.|Textbook of Gastroenterology|2008
Cited by 97Open Access

This chapter contains sections titled: Structural organization of the enteric nervous system Microscopic structure of the enteric nervous system Histochemical profiles and transmitter multiplicity of enteric neurons Physiological characteristics of enteric neurons Functionally defined enteric neurons Enteric control of motility Enteric control of secretion and vasodilation Enteric nervous system responses to noxious stimuli Sympathetic effects on motility and secretion Summary References