Your search keyword '"Rachagani, Satyanarayana"' showing total 7 results

1. Differential gene expression analysis of peripheral blood mononuclear cells reveals novel test for early detection of pancreatic cancer.

Author

Baine, Michael J., Menning, Melanie, Smith, Lynette M., Mallya, Kavita, Kaur, Sukhwinder, Rachagani, Satyanarayana, Chakraborty, Subhankar, Sasson, Aaron R., Brand, Randall E., and Batra, Surinder K.

Subjects

PANCREATIC cancer, GENE expression, CANCER patients, GENES, MULTIVARIATE analysis

Abstract

Background: We sought to validate global microarray results indicating the differential expression of 383 genes in Peripheral Blood Mononuclear Cells (PBMCs) from patients with pancreatic cancer (PC) and to further evaluate their PC diagnostic potential. Methods and materials: In total, 177 patients were recruited (47 healthy controls (HC), 35 chronic pancreatitis (CP) patients, and 95 PC patients). PBMC expressions of six genes from our previous study (ANXA3, ARG1, CA5B, F5, SSBP2, and TBC1D8) along with four new genes (MIC1, NGAL, MUC1, and MUC16) were analyzed using multiplex Q-RT PCR. Results: Differential expressions of 5 of the 6 genes previously identified by PBMC microarray were validated in this study. Multivariate models for PBMC gene expression were attempted to determine if any combination was diagnostically superior to CA19-9 alone. We found that addition of PBMC CA5B, F5, SSBP2, and MIC1 expression levels to CA19-9 significantly improved CA19-9's diagnostic abilities when comparing resectable PC to CP patients (p=0.023). Conclusions: Results of our previous study were validated, indicating reproducibility of PC-associated PBMC expression profiling. We identified a score-based model that can differentiate resectable PC from CP better than CA19-9, potentiating that PBMC differential expression analysis may offer a novel tool for early PC diagnosis. [ABSTRACT FROM AUTHOR]

Published

2012

2. Graviola: A novel promising natural-derived drug that inhibits tumorigenicity and metastasis of pancreatic cancer cells in vitro and in vivo through altering cell metabolism

Author

Torres, María P., Rachagani, Satyanarayana, Purohit, Vinee, Pandey, Poomy, Joshi, Suhasini, Moore, Erik D., Johansson, Sonny L., Singh, Pankaj K., Ganti, Apar K., and Batra, Surinder K.

Subjects

*MEDICAL botany, *METASTASIS, *PANCREATIC cancer, *CANCER cells, *CELL metabolism, *CANCER chemotherapy, *GENE expression

Abstract

Abstract: Pancreatic tumors are resistant to conventional chemotherapies. The present study was aimed at evaluating the potential of a novel plant-derived product as a therapeutic agent for pancreatic cancer (PC). The effects of an extract from the tropical tree Annona Muricata, commonly known as Graviola, was evaluated for cytotoxicity, cell metabolism, cancer-associated protein/gene expression, tumorigenicity, and metastatic properties of PC cells. Our experiments revealed that Graviola induced necrosis of PC cells by inhibiting cellular metabolism. The expression of molecules related to hypoxia and glycolysis in PC cells (i.e. HIF-1α, NF-κB, GLUT1, GLUT4, HKII, and LDHA) were downregulated in the presence of the extract. In vitro functional assays further confirmed the inhibition of tumorigenic properties of PC cells. Overall, the compounds that are naturally present in a Graviola extract inhibited multiple signaling pathways that regulate metabolism, cell cycle, survival, and metastatic properties in PC cells. Collectively, alterations in these parameters led to a decrease in tumorigenicity and metastasis of orthotopically implanted pancreatic tumors, indicating promising characteristics of the natural product against this lethal disease. [Copyright &y& Elsevier]

Published

2012

3. Myostatin genotype regulates muscle-specific miRNA expression in mouse pectoralis muscle.

Author

Rachagani, Satyanarayana, Ye Cheng, and Reecy, James M.

Subjects

*GENETIC polymorphisms, *GENETIC research, *RODENTS, *GENOTYPE-environment interaction, *MICE, *PECTORALIS muscle, *TISSUES, *GENE expression

Abstract

Background: Loss of functional Myostatin results in a dramatic increase in skeletal muscle mass. It is unknown what role miRNAs play in Myostatin mediated repression of skeletal muscle mass. We hypothesized that Myostatin genotype would be associated with the differential expression of miRNAs in skeletal muscle. Findings: Loss of functional Myostatin resulted in a significant increase (p < .001) in miR-1, miR-133a, miR-133b, and miR-206 expression. In contrast, Myostatin genotype had no effect (P > .2) on miR-24 expression level. Myostatin genotype did not affect the expression level of MyoD or Myogenin (P > 0.5). Conclusions: Myostatin may regulates the expression of miRNAs such as miR-133a, miR-133b, miR-1, and miR-206 in skeletal muscle as it has been observed that the expression of those miRNAs are significantly higher in myostatin null mice compared to wild type and heterozygous mice. In contrast, expression of myogenic factors such as MyoD or Myogenin has not been affected by myostatin in the muscle tissue. [ABSTRACT FROM AUTHOR]

Published

2010

4. RNA Polymerase II Associated Factor 1/PD2 Maintains Self-Renewal by Its Interaction with Oct3/4 in Mouse Embryonic Stem Cells.

Author

Ponnusamy, Moorthy P., Deb, Shonali, Dey, Parama, Chakraborty, Subhankar, Rachagani, Satyanarayana, Senapati, Shantibhusan, and Batra, Surinder K.

Subjects

RNA polymerases, GENOTYPE-environment interaction, GENE expression, EMBRYONIC stem cells, NUCLEIC acids, LABORATORY mice

Abstract

Embryonic stem cells (ESCs) maintain self-renewal while ensuring a rapid response to differentiation signals, but the exact mechanism of this process remains unknown. PD2 is the human homolog of the RNA polymerase II-associated factor 1 (Paf1). The Paf1/PD2 is a member of the human PAF complex that consists of four other subunits, hCdc73, hLeo1, hCtr9, and hSki8, and is involved in the regulation of transcriptional elongation and further downstream events. Here, we show that Paf1/PD2 is overexpressed in mouse ESCs and is involved in the maintenance of mouse ESCs. The Paf1/PD2 knockdown and knockout ESCs grown under self-renewal conditions express substantially reduced levels of self-renewal regulators, including Oct3/4, SOX2, Nanog, and Shh. We observed that the level of Paf1/PD2 expression is much higher in self-renewing mouse embryonic carcinoma cells than in the differentiating cells. Knockout of Paf1/PD2 altered ESC phenotype by increasing apoptosis and decreasing the percentage of cells in S-phase of the cell cycle. Interestingly, we found that the key genes that regulate endodermal differentiation (Gata4, Gata6, and Fgf8) are induced in the Paf1/PD2 heterozygous knockout ESCs. This suggests that Paf1/PD2 plays a specific role in regulating early commitment of ESCs to endodermal differentiation. Furthermore, for the first time, we showed that Paf1/PD2 protein interacts with Oct3/4 and RNA polymerase II, and through this interaction Paf1/PD2 may regulate Oct3/4-mediated gene expression. Thus, the Paf1/PD2 protein is a newly discovered element of the interconnected regulatory network that maintains the self-renewal of mouse ESCs. [ABSTRACT FROM AUTHOR]

Published

2009

5. Amyloid Precursor-like Protein 2 Expression Increases during Pancreatic Cancer Development and Shortens the Survival of a Spontaneous Mouse Model of Pancreatic Cancer.

Author

Poelaert, Brittany J., Knoche, Shelby M., Larson, Alaina C., Pandey, Poomy, Seshacharyulu, Parthasarathy, Khan, Nuzhat, Maurer, H. Carlo, Olive, Kenneth P., Sheinin, Yuri, Ahmad, Rizwan, Singh, Amar B., Batra, Surinder K., Rachagani, Satyanarayana, Solheim, Joyce C., Sahni, Sumit, Mittal, Anubhav, and Samra, Jaswinder

Subjects

PANCREATIC tumors, THERAPEUTICS, SURVIVAL, BIOLOGICAL models, DISEASE progression, ANIMAL experimentation, IMMUNOHISTOCHEMISTRY, PROTEIN precursors, METASTASIS, GENE expression, EPITHELIUM, DUCTAL carcinoma, EPITHELIAL cells, MICE

Abstract

Simple Summary: As pancreatic cancer is a disease with a high fatality rate, a better understanding of how it develops and the identification of new potential targets for its treatment are greatly needed. In this current study, we showed that the expression of amyloid precursor-like protein 2 (APLP2) in pancreatic cancer epithelial cells is higher than in precursor lesion epithelial cells, thus indicating that APLP2 increases during human pancreatic cancer development. We also generated a new mouse model that demonstrated the deletion of APLP2 expression specifically within the pancreas prolongs survival and decreases metastasis for mice with pancreatic cancer. Taken together, these findings open a new avenue toward comprehending and treating pancreatic cancer. In the United States, pancreatic cancer is a major cause of cancer-related deaths. Although substantial efforts have been made to understand pancreatic cancer biology and improve therapeutic efficacy, patients still face a bleak chance of survival. A greater understanding of pancreatic cancer development and the identification of novel treatment targets are desperately needed. Our analysis of gene expression data from patient samples showed an increase in amyloid precursor-like protein 2 (APLP2) expression within primary tumor epithelium relative to pancreatic intraepithelial neoplasia (PanIN) epithelial cells. Augmented expression of APLP2 in primary tumors compared to adjacent stroma was also observed. Genetically engineered mouse models of spontaneous pancreatic ductal adenocarcinoma were used to investigate APLP2′s role in cancer development. We found that APLP2 expression intensifies significantly during pancreatic cancer initiation and progression in the LSL-KrasG12D/+; LSL-Trp53R172H/+; Pdx-1-Cre (KPC) mouse model, as shown by immunohistochemistry analysis. In studies utilizing pancreas-specific heterozygous and homozygous knockout of APLP2 in the KPC mouse model background, we observed significantly prolonged survival and reduced metastatic progression of pancreatic cancer. These results demonstrate the importance of APLP2 in pancreatic cancer initiation and metastasis and indicate that APLP2 should be considered a potential therapeutic target for this disease. [ABSTRACT FROM AUTHOR]

Published

2021

6. Smoking and microRNA dysregulation: a cancerous combination.

Author

Momi, Navneet, Kaur, Sukhwinder, Rachagani, Satyanarayana, Ganti, Apar K., and Batra, Surinder K.

Subjects

*MICRORNA genetics, *GENE expression, *TUMOR suppressor genes, *HEALTH, *SMOKING, *CANCER genetics

Abstract

Highlights: [•] The unique miRNA-based signatures distinguish healthy controls from cancer cases with high sensitivity and specificity. [•] Differential expression pattern of miRNAs in various malignancies varies with smoking status of individuals. [•] Smoking mediates its impact by modulating tumor-suppressive miRNAs during neoplastic transformation and oncogenic miRNAs at later stages of cancer. [•] miRNAs are probably involved in smoking-induced modulation of signaling cascades in various cancers. [ABSTRACT FROM AUTHOR]

Published

2014

7. Human intestinal MUC17 mucin augments intestinal cell restitution and enhances healing of experimental colitis

Author

Luu, Ying, Junker, Wade, Rachagani, Satyanarayana, Das, Srustidhar, Batra, Surinder K., Heinrikson, Robert L., Shekels, Laurie L., and Ho, Samuel B.

Subjects

*MUCINS, *INTESTINES, *WOUND healing, *COLITIS treatment, *CELL membranes, *LABORATORY mice, *GENE expression, *CELL migration, *BIOMARKERS, *EPIDERMAL growth factor

Abstract

Abstract: The membrane-bound mucins, MUC17 (human) and Muc3 (mouse), are highly expressed on the apical surface of intestinal epithelia and are thought to be cytoprotective. The extracellular regions of these mucins contain EGF-like Cys-rich segments (CRD1 and CRD2) connected by an intervening linker domain (L). The purpose of this study was to determine the functional activity of human MUC17 membrane-bound mucin. Methods: Endogenous MUC17 was inhibited in LS174T colon cells by stable transfection of a small hairpin RNA targeting MUC17 (LSsi cells). The effect of recombinant MUC17-CRD1-L-CRD2 protein on migration, apoptosis, and experimental colitis was determined. Results: Reduced MUC17 expression in LSsi cells was associated with visibly reduced cell aggregation, reduced cell–cell adherence, and reduced cell migration, but no change in tumorigenicity. LSsi cells also demonstrated a 3.7-fold increase in apoptosis rates compared with control cells following treatment with etoposide. Exposure of colonic cell lines to exogenous recombinant MUC17-CRD1-L-CRD2 protein significantly increased cell migration and inhibited apoptosis. As a marker of biologic activity, MUC17-CRD1-L-CRD2 proteins stimulate ERK phosphorylation in colonic cell lines; and inhibition of ERK phosphorylation reduced the anti-apoptosis and migratory effect of MUC17-CRD1-L-CRD2. Finally, mice treated with MUC17-CRD1-L-CRD2 protein given per rectum demonstrated accelerated healing in acetic acid and dextran sodium sulfate induced colitis in vivo. These data indicate that both native MUC17 and the exogenous recombinant cysteine-rich domain of MUC17 play a role in diverse cellular mechanisms related to cell restitution, and suggest a potential role for MUC17-CRD1-L-CRD2 recombinant protein in the treatment of mucosal inflammatory diseases. [Copyright &y& Elsevier]

Published

2010