Your search keyword '"Chatterjee, Aditi"' showing total 8 results

1. Molecular alterations associated with chronic exposure to cigarette smoke and chewing tobacco in normal oral keratinocytes

Author

Rajagopalan, Pavithra, Patel, Krishna, Jain, Ankit P, Nanjappa, Vishalakshi, Datta, Keshava K, Subbannayya, Tejaswini, Mangalaparthi, Kiran K, Kumari, Anjali, Manoharan, Malini, Coral, Karunakaran, Murugan, Sakthivel, Nair, Bipin, Prasad, TS Keshava, Mathur, Premendu P, Gupta, Ravi, Gupta, Rohit, Khanna-Gupta, Arati, Califano, Joseph, Sidransky, David, Gowda, Harsha, and Chatterjee, Aditi

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Dental/Oral and Craniofacial Disease, Tobacco Smoke and Health, Tobacco, Prevention, Cancer, Aetiology, 2.1 Biological and endogenous factors, Good Health and Well Being, Biomarkers, Cell Transformation, Neoplastic, Environmental Exposure, Gene Expression Profiling, Humans, Keratinocytes, Mouth Mucosa, Phenotype, Proteome, Proteomics, Smoking, Tobacco Use, Transcriptome, Exome Sequencing, Orbitrap Fusion, high-throughput, carcinogenesis, smoking, chronic exposure, Oncology & Carcinogenesis, Biochemistry and cell biology, Oncology and carcinogenesis

Abstract

Tobacco usage is a known risk factor associated with development of oral cancer. It is mainly consumed in two different forms (smoking and chewing) that vary in their composition and methods of intake. Despite being the leading cause of oral cancer, molecular alterations induced by tobacco are poorly understood. We therefore sought to investigate the adverse effects of cigarette smoke/chewing tobacco exposure in oral keratinocytes (OKF6/TERT1). OKF6/TERT1 cells acquired oncogenic phenotype after treating with cigarette smoke/chewing tobacco for a period of 8 months. We employed whole exome sequencing (WES) and quantitative proteomics to investigate the molecular alterations in oral keratinocytes chronically exposed to smoke/ chewing tobacco. Exome sequencing revealed distinct mutational spectrum and copy number alterations in smoke/ chewing tobacco treated cells. We also observed differences in proteomic alterations. Proteins downstream of MAPK1 and EGFR were dysregulated in smoke and chewing tobacco exposed cells, respectively. This study can serve as a reference for fundamental damages on oral cells as a consequence of exposure to different forms of tobacco.

Published

2018

2. JAK-STAT inhibitor as a potential therapeutic opportunity in AML patients resistant to cytarabine and epigenetic therapy

Author

Babu, Govind, primary, Chaudhuri, Padmaparna, additional, Rajappa, Manoj, additional, Biswas, Manjusha, additional, Sansar, Bipinesh, additional, Rajegowda, Chethan, additional, Radhakrishnan, Aneesha, additional, Advani, Jayshree, additional, Tewary, Biplab, additional, Radhakrishnan, Padhma, additional, Thiyagarajan, Saravanan, additional, Chatterjee, Aditi, additional, Upadhayaya, Ram Shankar, additional, and Majumder, Pradip K, additional

Published

2020

3. JAK-STAT inhibitor as a potential therapeutic opportunity in AML patients resistant to cytarabine and epigenetic therapy.

Author

Babu, Govind, Chaudhuri, Padmaparna, Rajappa, Manoj, Biswas, Manjusha, Sansar, Bipinesh, Rajegowda, Chethan, Radhakrishnan, Aneesha, Advani, Jayshree, Tewary, Biplab, Radhakrishnan, Padhma, Thiyagarajan, Saravanan, Chatterjee, Aditi, Upadhayaya, Ram Shankar, and Majumder, Pradip K

Subjects

CYTARABINE, ACUTE myeloid leukemia, DNA methyltransferases, HISTONE deacetylase, EPIGENETICS, TUMOR microenvironment

Abstract

The prognosis of AML is generally poor, with 5-year survival rate of 25%. There has been substantial progress in identification of new therapeutic targets, along with approval of at least three targeted therapies for AML in recent years. Nevertheless, treatment has largely remained unchanged over couple of decades, with ~40% patients not achieving remission. AML is a highly heterogenous disease and there is a need for a preclinical platform to understand the heterogeneity and tumor microenvironment that can guide therapy selection. In this study, we employed an ex vivo tumor explant model to study tumor microenvironment and to select a treatment course for AML patients. Our data reveal dysregulation of DNA methyltransferase (DNMT) and histone deacetylase (HDAC) in a subset of AML patients. Based on this observation, epigenetic modulators azacitidine and panobinostat alone and in combination, were evaluated as treatment regimens in cytarabine refractory tumors. More than 50% of the treated samples showed response to the combination therapy. In order to explore alternate treatment modalities for tumors refractory to these epigenetic modulators, TCGA data analysis was done which revealed increased expression and hypomethylation of IFNGR1/2, suggesting activation of JAK/STAT pathway in AML. This was further interrogated ex vivo, with p-STAT3 expression in patients' samples. Fedratinib, a JAK/STAT inhibitor was evaluated and 78% tumor efficacy response was achieved. Taken together, our data indicate that ex vivo platform derived from patient samples is capable in guiding optimal therapy selection for various classes of drugs including identification of novel targeted therapies. [ABSTRACT FROM AUTHOR]

Published

2021

4. Dysregulation of splicing proteins in head and neck squamous cell carcinoma

Author

Radhakrishnan, Aneesha, primary, Nanjappa, Vishalakshi, additional, Raja, Remya, additional, Sathe, Gajanan, additional, Chavan, Sandip, additional, Nirujogi, Raja Sekhar, additional, Patil, Arun H., additional, Solanki, Hitendra, additional, Renuse, Santosh, additional, Sahasrabuddhe, Nandini A., additional, Mathur, Premendu P., additional, Prasad, T. S. Keshava, additional, Kumar, Prashant, additional, Califano, Joseph A., additional, Sidransky, David, additional, Pandey, Akhilesh, additional, Gowda, Harsha, additional, and Chatterjee, Aditi, additional

Published

2016

5. Chronic exposure to chewing tobacco selects for overexpression of stearoyl-CoA desaturase in normal oral keratinocytes

Author

Nanjappa, Vishalakshi, primary, Renuse, Santosh, additional, Sathe, Gajanan J, additional, Raja, Remya, additional, Syed, Nazia, additional, Radhakrishnan, Aneesha, additional, Subbannayya, Tejaswini, additional, Patil, Arun, additional, Marimuthu, Arivusudar, additional, Sahasrabuddhe, Nandini A, additional, Guerrero-Preston, Rafael, additional, Somani, Babu L, additional, Nair, Bipin, additional, Kundu, Gopal C, additional, Prasad, T Keshava, additional, Califano, Joseph A, additional, Gowda, Harsha, additional, Sidransky, David, additional, Pandey, Akhilesh, additional, and Chatterjee, Aditi, additional

Published

2015

6. Calcium calmodulin dependent kinase kinase 2 - a novel therapeutic target for gastric adenocarcinoma

Author

Subbannayya, Yashwanth, primary, Syed, Nazia, additional, Barbhuiya, Mustafa A, additional, Raja, Remya, additional, Marimuthu, Arivusudar, additional, Sahasrabuddhe, Nandini, additional, Pinto, Sneha M, additional, Manda, Srikanth Srinivas, additional, Renuse, Santosh, additional, Manju, HC, additional, Zameer, Mohammed Abdul Lateef, additional, Sharma, Jyoti, additional, Brait, Mariana, additional, Srikumar, Kotteazeth, additional, Roa, Juan Carlos, additional, Vijaya Kumar, M, additional, Kumar, KV Veerendra, additional, Prasad, TS Keshava, additional, Ramaswamy, Girija, additional, Kumar, Rekha Vijay, additional, Pandey, Akhilesh, additional, Gowda, Harsha, additional, and Chatterjee, Aditi, additional

Published

2015

7. Pancreatic Cancer Database

Author

Thomas, Joji Kurian, primary, Kim, Min-Sik, additional, Balakrishnan, Lavanya, additional, Nanjappa, Vishalakshi, additional, Raju, Rajesh, additional, Marimuthu, Arivusudar, additional, Radhakrishnan, Aneesha, additional, Muthusamy, Babylakshmi, additional, Khan, Aafaque Ahmad, additional, Sakamuri, Sruthi, additional, Tankala, Shantal Gupta, additional, Singal, Mukul, additional, Nair, Bipin, additional, Sirdeshmukh, Ravi, additional, Chatterjee, Aditi, additional, Prasad, T S Keshava, additional, Maitra, Anirban, additional, Gowda, Harsha, additional, Hruban, Ralph H, additional, and Pandey, Akhilesh, additional

Published

2014

8. Pancreatic Cancer Database: An integrative resource for pancreatic cancer.

Author

Thomas, Joji Kurian, Min-Sik Kim, Balakrishnan, Lavanya, Nanjappa, Vishalakshi, Raju, Rajesh, Marimuthu, Arivusudar, Radhakrishnan, Aneesha, Muthusamy, Babylakshmi, Khan, Aafaque Ahmad, Sakamuri, Sruthi, Tankala, Shantal Gupta, Singal, Mukul, Nair, Bipin, Sirdeshmukh, Ravi, Chatterjee, Aditi, Prasad, T. S. Keshava, Maitra, Anirban, Gowda, Harsha, Hruban, Ralph H., and Pandey, Akhilesh

Abstract

Pancreatic cancer is the fourth leading cause of cancer-related death in the world. The etiology of pancreatic cancer is heterogeneous with a wide range of alterations that have already been reported at the level of the genome, transcriptome, and proteome. The past decade has witnessed a large number of experimental studies using high-throughput technology platforms to identify genes whose expression at the transcript or protein levels is altered in pancreatic cancer. Based on expression studies, a number of molecules have also been proposed as potential biomarkers for diagnosis and prognosis of this deadly cancer. Currently, there are no repositories which provide an integrative view of multiple Omics data sets from published research on pancreatic cancer. Here, we describe the development of a web-based resource, Pancreatic Cancer Database (http://www.pancreaticcancerdatabase.org), as a unified platform for pancreatic cancer research. PCD contains manually curated information pertaining to quantitative alterations in miRNA, mRNA, and proteins obtained from small-scale as well as high-throughput studies of pancreatic cancer tissues and cell lines. We believe that PCD will serve as an integrative platform for scientific community involved in pancreatic cancer research. [ABSTRACT FROM AUTHOR]

Published

2014