Your search keyword '"Mannan, Poonam"' showing total 4 results

1. Biological Profile of the Less Lipophilic and Synthetically More Accessible Bryostatin 7 Closely Resembles That of Bryostatin 1

Author

Kedei, Noemi, Lewin, Nancy E., Géczy, Tamás, Selezneva, Julia, Braun, Derek C., Chen, Jinqiu, Herrmann, Michelle A., Heldman, Madeleine R., Lim, Langston, Mannan, Poonam, Garfield, Susan H., Poudel, Yam B., Cummins, Thomas J., Rudra, Arnab, Blumberg, Peter M., and Keck, Gary E.

Abstract

The bryostatins are a group of 20 macrolides isolated by Pettit and co-workers from the marine organism Bugula neritina. Bryostatin 1, the flagship member of the family, has been the subject of intense chemical and biological investigations due to its remarkably diverse biological activities, including promising indications as therapy for cancer, Alzheimer’s disease, and HIV. Other bryostatins, however, have attracted far less attention, most probably due to their relatively low natural abundance and associated scarcity of supply. Among all macrolides in this family, bryostatin 7 is biologically the most potent protein kinase C (PKC) ligand (in terms of binding affinity) and also the first bryostatin to be synthesized in the laboratory. Nonetheless, almost no biological studies have been carried out on this agent. We describe herein the total synthesis of bryostatin 7 based on our pyran annulation technology, which allows for the first detailed biological characterizations of bryostatin 7 with side-by-side comparisons to bryostatin 1. The results suggest that the more easily synthesized and less lipophilic bryostatin 7 may be an effective surrogate for bryostatin 1.

Published

2013

2. Interspecies Comparative Genomic Hybridization (I-CGH): A New Twist to Study Animal Tumor Models

Author

Jaikumar, Sivakumar, Zhuang, Zhengping, Mannan, Poonam, Vortmeyer, Alexander O., Furuta, Makoto, Dickerman, Rob, Bedanova, Julia, Lonser, Russell R., Walbridge, Stuart, Weil, Robert J., Lobanenkov, Victor V., Oldfield, Edward H., and Pack, Svetlana D.

Abstract

Animal models of human diseases are widely used to address questions of tumor development. Selection of a particular animal model depends upon a variety of factors, among them: animal cost, species lifespan, and hardiness; availability of biomolecular and genetic tools for that species; and evolutionary distance from humans. In spite of the growth in genomic data in the past several years, many animal models cannot yet be studied extensively due to gaps in genetic mapping, sequencing and functional analyses. Thus, alternative molecular genetic approaches are needed. We have designed an interspecies comparative genomic hybridization approach to analyze genetic changes in radiation-induced brain tumors in the non-human primate, Macaca mulatta. Using homologies between the primate and human genomes, we adapted widely-available CGH techniques to generate cytogenetic profiles of malignant gliomas in 4 monkey tumors. Losses and gains were projected onto the corresponding homologous chromosomal regions in the human genome, thus directly translating the status of the monkey gliomas into human gene content. This represents a novel method of comparative interspecies cytogenetic mapping that permits simultaneous analysis of genomic imbalance of unknown sequences in disparate species and correlation with potential or known human disease-related genes.

Published

2007

3. Plasminogen activator inhibitor-1 is a determinant of coronary thrombosis in sudden cardiac death

Author

Farb, Andrew, Burke, Allen P., Kolodgie, Frank D., Mannan, Poonam, Liang, You-hui, Smialek, John, and V ani, Renu

Published

1996

4. 797-5 Ulceration of Smooth Muscle Cell-Rich Plaques: A Frequent Cause of Coronary Artery Thrombosis That is not Mediated by HLA-DR Expression

Author

Farb, Andrew, Tang, Anita L., Burke, Allen P., Liang, Youhai, Mannan, Poonam, Smialek, John, and Virmani, Renu

Abstract

Coronary artery thrombosis (CAT) is reported to occur primarily from plaque rupture (PRI involving disruption of a fibrous cap over a necrotic core. However, CAT associated with superficial ulceration ISUI of predominately fibromuscular plaques without rupture of a necrotic core is under-reported. We performed post-mortem angiography, detailed coronary histology, morphometry, and immunohistochemistry in 42 cases (33 men, 9 women) of sudden death due to CAT. All individuals died≤6 hours of symptom onset. Histo- and immunochemical stains consisted of Movat pentachrome, H&E, smooth muscle specific actin, KP-1 (for macrophages). UCHL1 (for T-cells), Leder stain Ifor neutrophils). and HLA-DR.

Published

1995