Your search keyword '"Chigurupati, Srinivasulu"' showing total 4 results

1. Targeting DUSPs in glioblastomas - wielding a double-edged sword?

Author

Prabhakar, Sheila, Asuthkar, Swapna, Lee, William, Chigurupati, Srinivasulu, Zakharian, Eleonora, Tsung, Andrew J., and Velpula, Kiran Kumar

Subjects

BRAIN cancer research, GLIOBLASTOMA multiforme, PHOSPHATASES, MITOGEN-activated protein kinases, CANCER invasiveness

Abstract

Several dual-specificity phosphatases (DUSPs) that play key roles in the direct or indirect inactivation of different MAP kinases (MAPKs) have been implicated in human cancers over the past decade. This has led to a growing interest in identifying DUSPs and their specific inhibitors for further testing and validation as therapeutic targets in human cancers. However, the lack of understanding of the complex regulatory mechanisms and cross-talks between MAPK signaling pathways, combined with the fact that DUSPs can act as a double-edged sword in cancer progression, calls for a more careful and thorough investigation. Among the various types of brain cancer, glioblastoma multiforme (GBM) is notorious for its aggressiveness and resistance to current treatment modalities. This has led to the search for new molecular targets, particularly those involving various signaling pathways. DUSPs appear to be a promising target, but much more information on DUSP targets and their effects on GBM is needed before potential therapies can be developed, tested, and validated. This review identifies and summarize the specific roles of DUSP1, DUSP4, DUSP6 and DUSP26 that have been implicated in GBM. [ABSTRACT FROM AUTHOR]

Published

2014

2. 3,6′-dithiothalidomide improves experimental stroke outcome by suppressing neuroinflammation.

Author

Yoon, Jeong Seon, Lee, Jong‐Hwan, Tweedie, David, Mughal, Mohamed R., Chigurupati, Srinivasulu, Greig, Nigel H., and Mattson, Mark P.

Published

2013

3. Dietary restriction mitigates cocaine-induced alterations of olfactory bulb cellular plasticity and gene expression, and behavior.

Author

Xiangru Xu, Mughal, Mohamed R., Scott Hall, F., Perona, Maria T. G., Pistell, Paul J., Lathia, Justin D., Chigurupati, Srinivasulu, Becker, Kevin G., Ladenheim, Bruce, Niklason, Laura E., Uhl, George R., Cadet, Jean Lud, and Mattson, Mark P.

Subjects

GENE expression, OLFACTORY nerve, COCAINE, MICE, DOPAMINE, ENERGY metabolism, ANIMAL nutrition

Abstract

J. Neurochem. (2010) 114, 323–334. Because the olfactory system plays a major role in food consumption, and because ‘food addiction’ and associated morbidities have reached epidemic proportions, we tested the hypothesis that dietary energy restriction can modify adverse effects of cocaine on behavior and olfactory cellular and molecular plasticity. Mice maintained on an alternate day fasting (ADF) diet exhibited increased baseline locomotion and increased cocaine-sensitized locomotion during cocaine conditioning, despite no change in cocaine conditioned place preference, compared with mice fed ad libitum. Levels of dopamine and its metabolites in the olfactory bulb (OB) were suppressed in mice on the ADF diet compared with mice on the control diet, independent of acute or chronic cocaine treatment. The expression of several enzymes involved in dopamine metabolism including tyrosine hydroxylase, monoamine oxidases A and B, and catechol-O-methyltransferase were significantly reduced in OBs of mice on the ADF diet. Both acute and chronic administration of cocaine suppressed the production of new OB cells, and this effect of cocaine was attenuated in mice on the ADF diet. Cocaine administration to mice on the control diet resulted in up-regulation of OB genes involved in mitochondrial energy metabolism, synaptic plasticity, cellular stress responses, and calcium- and cAMP-mediated signaling, whereas multiple olfactory receptor genes were down-regulated by cocaine treatment. ADF abolished many of the effects of cocaine on OB gene expression. Our findings reveal that dietary energy intake modifies the neural substrates underlying some of the behavioral and physiological responses to repeated cocaine treatment, and also suggest novel roles for the olfactory system in addiction. The data further suggest that modification of dietary energy intake could provide a novel potential approach to addiction treatments. [ABSTRACT FROM AUTHOR]

Published

2010

4. Calcitonin stimulates the secretion of urokinase-type plasminogen activator from prostate cancer cells: Its possible implications on tumor cell invasion.

Author

Sabbisetti, Venkata, Chigurupati, Srinivasulu, Thomas, Shibu, and Shah, Girish

Abstract

Calcitonin (CT) is synthesized and secreted in prostate epithelium, and its secretion from malignant prostates is several folds higher than that in benign prostates. CT receptor (CTR) is expressed in malignant prostate epithelium, and its activation increases invasiveness of prostate cancer (PC) cells via activation of protein kinase A. Since the role of urokinase-type plasminogen activator (uPA) in invasion of PC has been established, we tested the hypothesis that CT increases invasion of PC cells by stimulating uPA secretion from PC cells. Exogenously added CT stimulated the secretion of uPA from PC-3M cells in a dose-dependent manner, which was blocked by Rp.cAMP, a competitive inhibitor of protein kinase A. CT stimulated the secretion of MMP-2 and MMP-9 from PC-3M cells, and also increased their invasiveness. Both these actions of CT were blocked by uPA-neutralizing antibodies. Immunofluorescence studies with PC-3M cells suggest that CT stimulated redistribution of cellular uPA to focal adhesion sites, which was further confirmed by co-immunoprecipitation of uPA with focal adhesion kinase (FAK) in response to CT. These results suggest that CT increases invasiveness of PC cells by stimulating PKA-mediated uPA secretion and by redirecting the secreted uPA to focal adhesion sites. The results also suggest that uPA may, at least in part, mediate proinvasive actions of CT on PC cells by stimulating the secretion of gelatinases and degradation of focal adhesion sites. © 2005 Wiley-Liss, Inc. [ABSTRACT FROM AUTHOR]

Published

2006