Vern L. Schramm, Ph.D.
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Albert Einstein College of Medicine Jack and Pearl Resnick Campus 1300 Morris Park Avenue Forchheimer Building, Room 308 Bronx, NY 10461 Tel: (718) 430-2813 Fax: (718) 430-8565 Email: vern@aecom.yu.edu
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| Professor, Department of Biochemistry | ||
| Chair, Department of Biochemistry | ||
| Ruth Merns Chair in Biochemistry | ||
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| Professional Interests | ||
Overview of Professional InterestsEnzymes catalyze virtually all of the chemical transformations necessary for biological life. Knowledge of the transition-state structure of enzymatic reactions permits the design of powerful inhibitors. Methods have been developed in this laboratory for the experimental determination of the geometric and charge features which characterize enzymatic transition states. This information is then used for the logical design of transition-state inhibitors which have the potential to be new biologically active agents. Specific projects include: Human genetic deficiency of purine nucleoside phosphorylase causes a specific T-cell insufficiency. Our inhibitors of this enzyme are powerful anti T-cell agents. Two inhibitors are now in human clinical trials against human T-cell cancers and autoimmune disorders. Three T-cell cancer indications for these drugs have received orphan drug status from the FDA and several phase II trials are in progress. A phase II clinical trial has been initiated for psoriasis using our second-generation inhibitor. Third-generation and fourth-generation inhibitors are now being characterized. Angiogenesis is required for tumor growth. One angiogenetic factor is thymidine phosphorylase, an enzyme that synthesizes deoxyribose 1-phosphase, a precursor to deoxyribose, the angiogenic molecule. We have solved the transition state structure of this enzyme and are now designing transition state analogues. It is hypothesized that such inhibitors will be useful as anticancer agents. Purine salvage is essential for growth of parasitic protozoa. A family of powerful inhibitors has been prepared against these enzymes from the malaria parasite. Promising results have been obtained in cell culture studies. One of these inhibitors stops the growth of malaria parasites in primate malaria. Plans are underway to initiate human trials in the next few years. Experimental cancer chemotherapy uses plant toxins coupled to a recognition element for cancer cells. The transition state structure of ricin has been determined to guide the design of inhibitors. These will limit the side-effects of the toxin molecules remaining in the circulation or released from lysed cancer cells. Inhibitors are being synthesized and tested for efficiency, and constructs the plant toxins ricin, saporin and gelosin are being investigated as anticancer agents. Additional projects involve S-adenosylmethionine recycling and methyl transfer reactions in bacterial quorum sensing, cancer and DNA methylation reactions. Students in this laboratory can receive training in enzymology, catalysis, protein expression, inhibitor design, computer modeling, inhibitor synthesis, and in drug metabolism studies in cells and animals. Active collaborations occur with laboratories specializing in NMR, X-ray crystallography, mass spectroscopy, synthetic organic chemistry, cancer and medicine. Projects can be designed to include several of these research approaches through active collaborative research programs. |
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Selected Publications
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Pubmed Search |
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Overview of Professional Interests
Selected Publications