Your search keyword '"Chappa, Prasanthi"' showing total 2 results

1. Renal protection by atorvastatin in a murine model of sickle cell nephropathy.

Author

Zahr, Rima S., Chappa, Prasanthi, Yin, Hong, Brown, Lou A., Ataga, Kenneth I., and Archer, David R.

Subjects

*STATINS (Cardiovascular agents), *KIDNEY diseases, *SICKLE cell anemia, *ATORVASTATIN, *ALBUMINURIA

Abstract

Summary: Recent studies have demonstrated pleiotropic effects of statins in various mouse models of kidney disease. In this study, Townes humanized sickle cell mice were treated for 8 weeks with atorvastatin at a dose of 10 mg/kg/day starting at 10 weeks of age. Treatment with atorvastatin significantly reduced albuminuria, and improved both urine concentrating ability and glomerular filtration rate. Atorvastatin also decreased markers of kidney injury and endothelial activation, and ameliorated oxidant stress in renal tissues and peripheral macrophages. Atorvastatin downregulated the expression of mRNA levels of the NADPH oxidases, Cybb (also termed Nox2) and Nox4, which are major sources of oxidant stress in the kidney. These findings highlight the pleiotropic effects of atorvastatin and suggest that it may provide beneficial effects in sickle cell nephropathy. [ABSTRACT FROM AUTHOR]

Published

2018

2. Alloimmunization to transfused HOD red blood cells is not increased in mice with sickle cell disease.

Author

Hendrickson, Jeanne E., Hod, Eldad A., Perry, Jennifer R., Ghosh, Samit, Chappa, Prasanthi, Adisa, Olufolake, Kean, Leslie S., Ofori-Acquah, Solomon F., Archer, David R., Spitalnik, Steven L., and Zimring, James C.

Subjects

ERYTHROCYTES, SICKLE cell anemia, PATHOLOGICAL physiology, CYTOKINES, ANTIGENS, BLOOD diseases

Abstract

BACKGROUND: Increased rates of red blood cell (RBC) alloimmunization in patients with sickle cell disease may be due to transfusion frequency, genetic predisposition, or immune dysregulation. To test the hypothesis that sickle cell pathophysiology influences RBC alloimmunization, we utilized two transgenic mouse models of sickle cell disease. STUDY DESIGN AND METHODS: Transgenic sickle mice, which express human α and βS globin, were transfused with fresh or 14-day-stored RBCs containing the HOD (hen egg lysozyme, ovalbumin, and human Duffyb) antigen; some recipients were inflamed with poly(I : C) before transfusion. Anti-HOD alloantibody responses were subsequently measured by enzyme-linked immunosorbent assay and flow crossmatch; a cohort of recipients had posttransfusion serum cytokines measured by bead array. RESULTS: Both Berkeley and Townes homozygous (SS) and heterozygous (AS) mice had similar rates and magnitude of anti-HOD RBC alloimmunization after fresh HOD RBC transfusion compared with control animals; under no tested condition did homozygous SS recipients make higher levels of alloantibodies than control animals. Unexpectedly, homozygous SS recipients had blunted cytokine responses and lower levels of anti-HOD alloantibodies after transfusion of 14-day stored RBCs, compared with control animals. CONCLUSIONS: In sum, homozygous βS expression and the ensuing disease state are not alone sufficient to enhance RBC alloimmunization to transfused HOD RBCs in two distinct humanized murine models of sickle cell disease under the conditions examined. These data suggest that other factors may contribute to the high rates of RBC alloimmunization observed in humans with sickle cell disease. [ABSTRACT FROM AUTHOR]

Published

2012