Your search keyword '"Roberts, Bruce A."' showing total 4 results

1. Alemtuzumab induction of intracellular signaling and apoptosis in malignant B lymphocytes.

Author

Nguyen, Tri-Hung, Havari, Evis, McLaren, Rajashree, Zhang, Mindy, Jiang, Yide, Madden, Stephen L., Roberts, Bruce, Kaplan, Johanne, and Shankara, Srinivas

Subjects

ALEMTUZUMAB, TUMORS, APOPTOSIS, B cells, CELL receptors

Abstract

The molecular changes induced by alemtuzumab following binding of CD52 on B tumor cells were investigated. Alemtuzumab alone had no detectable impact on cell signaling but cross-linking of alemtuzumab on the surface of B tumor lines with anti-human Fc antibodies induced a transient Ca2 ++ flux followed by phosphorylation of several kinases involved in stress and survival pathways, and expression of associated proteins including TNF-α. Cross-linking of alemtuzumab also induced capping and caspase-dependent apoptosis of the tumor lines. When using primary cells from B-CLL patients, alemtuzumab alone was capable of inducing protein phosphorylation and apoptosis through the cross-linking of alemtuzumab by FcγRIIb receptors on B-CLL cells. Apoptosis was prevented by blocking of FcγRIIb receptors with anti-CD32 antibody. Overall, our results indicate that cross-linking of alemtuzumab on B tumor cells can occur naturally through Fc receptor interaction and leads to the activation of specific cellular pathways and induction of apoptosis. [ABSTRACT FROM AUTHOR]

Published

2012

2. Investigation of the mechanism of action of alemtuzumab in a human CD52 transgenic mouse model.

Author

Yanping Hu, Turner, Michael J., Shields, Jacqueline, Gale, Matthew S., Hutto, Elizabeth, Roberts, Bruce L., Siders, William M., and Kaplan, Johanne M.

Subjects

MONOCLONAL antibodies, ANTIGENS, TRANSGENIC mice, LABORATORY mice, LYMPHOCYTES

Abstract

Alemtuzumab is a humanized monoclonal antibody against CD52, an antigen found on the surface of normal and malignant lymphocytes. It is approved for the treatment of B-cell chronic lymphocytic leukaemia and is undergoing Phase III clinical trials for the treatment of multiple sclerosis. The exact mechanism by which alemtuzumab mediates its biological effects in vivo is not clearly defined and mechanism of action studies have been hampered by the lack of cross-reactivity between human and mouse CD52. To address this issue, a transgenic mouse expressing human CD52 (hCD52) was created. Transgenic mice did not display any phenotypic abnormalities and were able to mount normal immune responses. The tissue distribution of hCD52 and the level of expression by various immune cell populations were comparable to those seen in humans. Treatment with alemtuzumab replicated the transient increase in serum cytokines and depletion of peripheral blood lymphocytes observed in humans. Lymphocyte depletion was not as profound in lymphoid organs, providing a possible explanation for the relatively low incidence of infection in alemtuzumab-treated patients. Interestingly, both lymphocyte depletion and cytokine induction by alemtuzumab were largely independent of complement and appeared to be mediated by neutrophils and natural killer cells because removal of these populations with antibodies to Gr-1 or asialo-GM-1, respectively, strongly inhibited the activity of alemtuzumab whereas removal of complement by treatment with cobra venom factor had no impact. The hCD52 transgenic mouse appears to be a useful model and has provided evidence for the previously uncharacterized involvement of neutrophils in the activity of alemtuzumab. [ABSTRACT FROM AUTHOR]

Published

2009

3. Reduction of inflammation and preservation of neurological function by anti-CD52 therapy in murine experimental autoimmune encephalomyelitis.

Author

Turner, Michael J., Pang, Petti T., Chretien, Nathalie, Havari, Evis, LaMorte, Michael J., Oliver, Julian, Pande, Nilesh, Masterjohn, Elizabeth, Carter, Karen, Reczek, David, Brondyk, William, Roberts, Bruce L., Kaplan, Johanne M., and Siders, William M.

Subjects

*NERVOUS system injuries, *DRUG therapy, *ENCEPHALOMYELITIS, *AUTOIMMUNE diseases, *NEUROLOGY

Abstract

Alemtuzumab, a monoclonal antibody directed against human CD52, is used in the treatment of MS. To characterize the impact of anti-CD52 administration, a monoclonal antibody to mouse CD52 (anti-muCD52) was generated and evaluated in EAE mouse models of MS. A single course of anti-muCD52 provided a therapeutic benefit accompanied by a reduction in the frequency of autoreactive T lymphocytes and production of pro-inflammatory cytokines. Examination of the CNS revealed a decrease in infiltrating lymphocytes, demyelination and axonal loss. Electrophysiological assessment showed preservation of axonal conductance in the spinal cord. These findings suggest that anti-CD52 therapy may help preserve CNS integrity. [ABSTRACT FROM AUTHOR]

Published

2015

4. Immune status following alemtuzumab treatment in human CD52 transgenic mice.

Author

Turner, Michael J., LaMorte, Michael J., Chretien, Nathalie, Havari, Evis, Roberts, Bruce L., Kaplan, Johanne M., and Siders, William M.

Subjects

*ALEMTUZUMAB, *CD antigens, *LABORATORY mice, *MULTIPLE sclerosis, *MONOCLONAL antibodies, *LYMPHOCYTES, *NATURAL immunity, *MULTIPLE sclerosis treatment, *PATIENTS

Abstract

Abstract: Alemtuzumab is a monoclonal antibody against the CD52 antigen present at high levels on the surface of lymphocytes. While treatment of multiple sclerosis patients with alemtuzumab results in marked depletion of lymphocytes from the circulation, it has not been associated with a high incidence of serious infections. In a human CD52 transgenic mouse, alemtuzumab treatment showed minimal impact on the number and function of innate immune cells. A transient decrease in primary adaptive immune responses was observed post-alemtuzumab but there was little effect on memory responses. These results potentially help explain the level of immunocompetence observed in alemtuzumab-treated MS patients. [Copyright &y& Elsevier]

Published

2013