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Dive into the research topics where Alex V. Trevino is active.

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Featured researches published by Alex V. Trevino.


Biochemical Pharmacology | 2003

Apoptosis induction by the dual-action DNA- and protein-reactive antitumor drug irofulven is largely Bcl-2-independent

Maryanne C. Herzig; Alex V. Trevino; Huiyun Liang; Richard Salinas; Stephen J. Waters; John R. MacDonald; Barbara A. Woynarowska; Jan M. Woynarowski

The overexpression of Bcl-2 is implicated in the resistance of cancer cells to apoptosis. This study explored the potential of irofulven (hydroxymethylacylfulvene, HMAF, MGI 114, NSC 683863), a novel DNA- and protein-reactive anticancer drug, to overcome the anti-apoptotic properties of Bcl-2 in HeLa cells with controlled Bcl-2 overexpression. Irofulven treatment resulted in rapid (12hr) dissipation of the mitochondrial membrane potential, phosphatidylserine externalization, and apoptotic DNA fragmentation, with progressive changes after 24hr. Bcl-2 overexpression caused marginal or partial inhibition of these effects after treatment times ranging from 12 to 48hr. Both Bcl-2-dependent and -independent responses to irofulven were abrogated by a broad-spectrum caspase inhibitor. Despite the somewhat decreased apoptotic indices, cell growth inhibition by irofulven was unaffected by Bcl-2 status. In comparison, Bcl-2 overexpression drastically reduced apoptotic DNA fragmentation by etoposide, acting via topoisomerase II-mediated DNA damage, but had no effect on apoptotic DNA fragmentation by helenalin A, which reacts with proteins but not DNA. Irofulven retains its pro-apoptotic and growth inhibitory potential in cell lines that have naturally high Bcl-2 expression. Collectively, the results implicate multiple mechanisms of apoptosis induction by irofulven, which may differ in time course and Bcl-2 dependence. It is possible that the sustained ability of irofulven to induce profound apoptosis and to block cell growth despite Bcl-2 overexpression may be related to its dual reactivity with both DNA and proteins.


Molecular Pharmacology | 2000

Oxaliplatin-Induced Damage of Cellular DNA

Jan M. Woynarowski; Sandrine Faivre; Maryanne C. Herzig; Brenda Arnett; William G. Chapman; Alex V. Trevino; Eric Raymond; Stephen G. Chaney; Alexandra Vaisman; Maria Varchenko; Paul Juniewicz


Journal of Biological Chemistry | 2001

AT-rich Islands in Genomic DNA as a Novel Target for AT-specific DNA-reactive Antitumor Drugs

Jan M. Woynarowski; Alex V. Trevino; Karl A. Rodriguez; Stephen C. Hardies; Craig J. Benham


Cancer Biology & Therapy | 2004

Cell cycle effects and induction of premitotic apoptosis by irofulven in synchronized cancer cells

Jan M. Woynarowski; Barbara A. Woynarowska; Alex V. Trevino; Richard Salinas; Terence S. Herman; Stephen J. Waters; John R. MacDonald


Nucleic Acids Research | 2003

Matrix attachment region (MAR) properties and abnormal expansion of AT island minisatellites in FRA16B fragile sites in leukemic CEM cells

Jennifer A. Jackson; Alex V. Trevino; Maryanne C. Herzig; Terence S. Herman; Jan M. Woynarowski


Biochemistry | 2000

Region-specific DNA damage by AT-specific DNA-reactive drugs is predicted by drug binding specificity.

Jan M. Woynarowski; Cheryl Napier; Alex V. Trevino; Brenda Arnett


Biochemistry | 2002

The genome factor in region-specific DNA damage: the DNA-reactive drug U-78779 prefers mixed A/T-G/C sequences at the nucleotide level but is region-specific for long pure AT islands at the genomic level.

Maryanne C. Herzig; Karl A. Rodriguez; Alex V. Trevino; Jaroslaw Dziegielewski; Brenda Arnett; Laurence H. Hurley; Jan M. Woynarowski


Biochemistry | 1999

Tallimustine lesions in cellular DNA are AT sequence-specific but not region-specific.

Maryanne C. Herzig; Alex V. Trevino; Brenda Arnett; Jan M. Woynarowski


Molecular Cancer Therapeutics | 2004

Enhanced topoisomerase II targeting by annamycin and related 4-demethoxy anthracycline analogues

Alex V. Trevino; Barbara A. Woynarowska; Terence S. Herman; Waldemar Priebe; Jan M. Woynarowski


Biochemical and Biophysical Research Communications | 1999

ENZYMATIC ACTIVITY OF ENDOGENOUS TELOMERASE ASSOCIATED WITH INTACT NUCLEI FROM HUMAN LEUKEMIA CEM CELLS

Terace M. Fletcher; Alex V. Trevino; Jan M. Woynarowski

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Jan M. Woynarowski

University of Texas Health Science Center at San Antonio

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Maryanne C. Herzig

University of Texas Health Science Center at San Antonio

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Barbara A. Woynarowska

University of Texas Health Science Center at San Antonio

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Brenda Arnett

University of Texas Health Science Center at San Antonio

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Terence S. Herman

University of Oklahoma Health Sciences Center

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John R. MacDonald

University of Texas Health Science Center at San Antonio

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Karl A. Rodriguez

University of Texas Health Science Center at San Antonio

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Richard Salinas

University of Texas Health Science Center at San Antonio

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Stephen J. Waters

University of Texas Health Science Center at San Antonio

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Alexandra Vaisman

National Institutes of Health

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