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Dive into the research topics where Michael I. Jesson is active.

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Featured researches published by Michael I. Jesson.


Cancer Research | 2004

PT-100, a Small Molecule Dipeptidyl Peptidase Inhibitor, Has Potent Antitumor Effects and Augments Antibody-Mediated Cytotoxicity via a Novel Immune Mechanism

Sharlene Adams; Glenn T. Miller; Michael I. Jesson; Takeshi Watanabe; Barry Jones; Barbara P. Wallner

The amino boronic dipeptide, PT-100 (Val-boro-Pro), a dipeptidyl peptidase (DPP) inhibitor, has been shown to up-regulate gene expression of certain cytokines in hematopoietic tissue via a high-affinity interaction, which appears to involve fibroblast activation protein. Because fibroblast activation protein is also expressed in stroma of lymphoid tissue and tumors, the effect of PT-100 on tumor growth was studied in mice in vivo. PT-100 has no direct cytotoxic effect on tumors in vitro. Oral administration of PT-100 to mice slowed growth of syngeneic tumors derived from fibrosarcoma, lymphoma, melanoma, and mastocytoma cell lines. In WEHI 164 fibrosarcoma and EL4 and A20/2J lymphoma models, PT-100 caused regression and rejection of tumors. The antitumor effect appeared to involve tumor-specific CTL and protective immunological memory. PT-100 treatment of WEHI 164-inoculated mice increased mRNA expression of cytokines and chemokines known to promote T-cell priming and chemoattraction of T cells and innate effector cells. The role of innate activity was further implicated by observation of significant, although reduced, inhibition of WEHI 164 and A20/2J tumors in immunodeficient mice. PT-100 also demonstrated ability to augment antitumor activity of rituximab and trastuzumab in xenograft models of human CD20+ B-cell lymphoma and HER-2+ colon carcinoma where antibody-dependent cytotoxicity can be mediated by innate effector cells responsive to the cytokines and chemokines up-regulated by PT-100. Although CD26/DPP-IV is a potential target for PT-100 in the immune system, it appeared not to be involved because antitumor activity and stimulation of cytokine and chemokine production was undiminished in CD26−/− mice.


Archive | 2003

Methods and compositions relating to isoleucine boroproline compounds

Sharlene Adams; Glenn T. Miller; Michael I. Jesson; Barry Jones


Blood | 2003

Hematopoietic stimulation by a dipeptidyl peptidase inhibitor reveals a novel regulatory mechanism and therapeutic treatment for blood cell deficiencies.

Barry Jones; Sharlene Adams; Glenn T. Miller; Michael I. Jesson; Takeshi Watanabe; Barbara P. Wallner


Archive | 2003

Boroproline compound combination therapy

Sharlene Adams; Glenn T. Miller; Michael I. Jesson; Barry Jones


Archive | 1995

Soluble single chain t cell receptors

Julian Banerji; Sanjay S. Khandekar; Brian Bettencourt; Jerome Naylor; Barry Jones; Michael I. Jesson; Donard S. Dwyer


Cancer Research | 1987

Effects of 3′-(3-Cyano-4-morpholinyl)-3′-deaminoadriamycin and Structural Analogues on DNA in HT-29 Human Colon Carcinoma Cells

Michael I. Jesson; James B. Johnston; Cynthia D. Anhalt; Asher Begleiter


Cancer Research | 1989

Characterization of the DNA-DNA Cross-Linking Activity of 3′-(3-Cyano-4-morpholinyl)-3′-deaminoadriamycin

Michael I. Jesson; James B. Johnston; Erica Robotham; Asher Begleiter


International Immunology | 1998

The immune response to soluble D10 TCR: analysis of antibody and T cell responses.

Michael I. Jesson; Sanjay S. Khandekar; John R. Newcomb; Jerome Naylor; Paul Gregory; Pamela P. Brauer; Brian Bettencourt; Julian Banerji; Barry Jones


Archive | 2005

Methods and compositions for treating glucose-associated conditions, metabolic syndrome, dyslipidemias and other conditions

Nazneen Aziz; Michael I. Jesson; Paul A. Mclean; Glenn T. Miller; Barry Jones


Archive | 1995

Soluble heterodimeric t cell receptors and their antibodies

Julian Banerji; Sanjay S. Khandekar; Pamela P. Brauer; Jerome Naylor; Michael I. Jesson; Barry Jones

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