Your search keyword '"Agrawal, Manas"' showing total 7 results

1. Immune checkpoint proteins: Signaling mechanisms and molecular interactions in cancer immunotherapy.

Author

Gaikwad, Shreyas, Agrawal, Manas Yogendra, Kaushik, Itishree, Ramachandran, Sharavan, and Srivastava, Sanjay K.

Subjects

*IMMUNE checkpoint proteins, *MOLECULAR interactions, *IPILIMUMAB, *IMMUNOTHERAPY, *IMMUNE checkpoint inhibitors, *CELL populations

Abstract

Immune checkpoint proteins (ICP) are currently one of the most novel and promising areas of immune-oncology research. This novel way of targeting tumor cells has shown favorable success over the past few years with some FDA approvals such as Ipilimumab, Nivolumab, Pembrolizumab etc. Currently, more than 3000 clinical trials of immunotherapeutic agents are ongoing with majority being ICPs. However, as the number of trials increase so do the challenges. Some challenges such as adverse side effects, non-specific binding on healthy tissues and absence of response in some subset populations are critical obstacles. For a safe and effective further therapeutic development of molecules targeting ICPs, understanding their mechanism at molecular level is crucial. Since ICPs are mostly membrane bound receptors, a number of downstream signaling pathways divaricate following ligand-receptor binding. Most ICPs are expressed on more than one type of immune cell populations. Further, the expression varies within a cell type. This naturally varied expression pattern adds to the difficulty of targeting specific effector immune cell types against cancer. Hence, understanding the expression pattern and cellular mechanism helps lay out the possible effect of any immunotherapy. In this review, we discuss the signaling mechanism, expression pattern among various immune cells and molecular interactions derived using interaction database analysis (BioGRID). [ABSTRACT FROM AUTHOR]

Published

2022

2. Research Trend and Detailed Insights into the Molecular Mechanisms of Food Bioactive Compounds against Cancer: A Comprehensive Review with Special Emphasis on Probiotics.

Author

Agrawal, Manas Yogendra, Gaikwad, Shreyas, Srivastava, Sangeeta, and Srivastava, Sanjay K.

Subjects

*THERAPEUTIC use of probiotics, *ORGANIC compounds, *PROBIOTICS, *MOLECULAR biology, *TUMORS, *MOLECULAR structure, TUMOR prevention

Abstract

Simple Summary: Cancer is one of the leading causes of death worldwide. Treatment of cancer has long been a challenge. While researchers have been searching for many options for the cure, mother nature has blessed us with natural bioactive components with anticancer potential. Since the 1800s, scientists have been studying the efficacy of the bioactive agents present in our food for the treatment of cancer. This review summarizes the molecular mechanisms responsible for these effects. Moreover, owing to the increased intake of probiotics in daily diets, this review also explains how they can be helpful in cancer prevention and treatment. In an attempt to find a potential cure for cancer, scientists have been probing the efficacy of the food we eat and its bioactive components. Over the decades, there has been an exponentially increasing trend of research correlating food and cancer. This review explains the molecular mechanisms by which bioactive food components exhibit anticancer effects in several cancer models. These bioactive compounds are mainly plant based or microbiome based. While plants remain the primary source of these phytochemicals, little is known about probiotics, i.e., microbiome sources, and their relationships with cancer. Thus, the molecular mechanisms underlying the anticancer effect of probiotics are discussed in this review. The principal mode of cell death for most food bioactives is found to be apoptosis. Principal oncogenic signaling axes such as Akt/PI3K, JAK/STAT, and NF-κB seem to be modulated due to these bioactives along with certain novel targets that provide a platform for further oncogenic research. It has been observed that probiotics have an immunomodulatory effect leading to their chemopreventive actions. Various foods exhibit better efficacy as complete extracts than their individual phytochemicals, indicating an orchestrated effect of the food components. Combining bioactive agents with available chemotherapies helps synergize the anticancer action of both to overcome drug resistance. Novel techniques to deliver bioactive agents enhance their therapeutic response. Such combinations and novel approaches are also discussed in this review. Notably, most of the food components that have been studied for cancer have shown their efficacy in vivo. This bolsters the claims of these studies and, thus, provides us with hope of discovering anticancer agents in the food that we eat. [ABSTRACT FROM AUTHOR]

Published

2022

3. Palliative radiotherapy: a one-week course in advanced head and neck cancer - quality of life outcomes.

Author

Prakash, Sadanand, Chakrabarti, Deep, Kumar, Rajendra, Agrawal, Manas Mani, Verma, Mrinalini, Singh, Sudhir, Gupta, Seema, Srivastava, Kirti, Gupta, Rajeev, and Brahma Bhatt, Madan Lal

Published

2024

4. Interferon stimulated gene 15 (ISG15) in cancer: An update.

Author

Nguyen, Hong-My, Gaikwad, Shreyas, Oladejo, Mariam, Agrawal, Manas Yogendra, Srivastava, Sanjay K., and Wood, Laurence M.

Subjects

*TYPE I interferons, *INTERFERONS, *CANCER vaccines, *GENES, *TUMOR microenvironment

Abstract

Among the plethora of defense mechanisms which a host elicits after pathogen invasion, type 1 interferons play a central role in regulating the immune system's response. They induce several interferon-stimulated genes (ISGs) which play a diverse role once activated. Over the past few decades, there have been several studies exploring the role of ISGs in cancer and ISG15 is among the most studied for its pro and anti-tumorigenic role. In this review, we aim to provide an update on the recent observations and findings related to ISG15 in cancer. We provide a brief overview about the initial observations and important historical findings which helped scientists understand structure and function of ISG15. We aim to provide an overview of ISG15 in cancer with an emphasis on studies which delve into the molecular mechanism of ISG15 in modulating the tumor microenvironment. Further, the dysregulation of ISG15 in cancer and the molecular mechanisms associated with its pro and anti-tumor roles are discussed in respective cancer types. Finally, we discuss multiple therapeutic applications of ISG15 in current cancer therapy. • ISG15 is emerging as an important proto-oncoprotein, a potential prognostic biomarker and therapeutic target for cancer. • ISG15 plays a contradictory role in cancers and is currently studied for its pro and anti-tumorigenic role. • Therapeutic administered recombinant ISG15 could be beneficial. • Overexpression of ISG15 is an avenue that can be exploited for immunotherapeutic targeting by cancer vaccines. [ABSTRACT FROM AUTHOR]

Published

2023

5. Development of Dual ARV-825 and Nintedanib-Loaded PEGylated Nano-Liposomes for Synergistic Efficacy in Vemurafnib-Resistant Melanoma.

Author

Fu, Yige, Saraswat, Aishwarya, Wei, Zenghui, Agrawal, Manas Yogendra, Dukhande, Vikas V., Reznik, Sandra E., and Patel, Ketan

Subjects

*THERAPEUTICS, *VASCULOGENIC mimicry, *LIPOSOMES, *MELANOMA, *CITRIC acid, *TUMOR growth

Abstract

A novel treatment strategy by co-targeting c-Myc and tumor stroma was explored in vemurafenib-resistant melanoma. BRD4 proteolysis targeting chimera (ARV-825) and nintedanib co-loaded PEGylated nanoliposomes (ARNIPL) were developed to incorporate a synergistic cytotoxic ratio. Both the molecules have extremely poor aqueous solubility. A modified hydration method with citric acid was used to improve the loading of both the molecules in liposomes. ARNIPL with mean particle size 111.1 ± 6.55 nm exhibited more than 90% encapsulation efficiency for both the drugs and was found to be physically stable for a month at 4 °C. Both the molecules and ARNIPL showed significantly higher cytotoxicity, apoptosis and down-regulation of target proteins BRD4 and c-Myc in vemurafenib-resistant cell line (A375R). Vasculogenic mimicry and clonogenic potential of A375R were significantly inhibited by ARNIPL. Tumor growth inhibition in 3D spheroids with reduction of TGF-β1 was observed with ARNIPL treatment. Therefore, ARNIPL could be a promising therapeutic approach for the treatment of vemurafenib-resistant melanoma. [ABSTRACT FROM AUTHOR]

Published

2021

6. Repurposing an Antiepileptic Drug for the Treatment of Glioblastoma.

Author

Yadav, Anjali, Alnakhli, Ali, Vemana, Hari Priya, Barot, Shrikant, Agrawal, Manas, Bhutkar, Shraddha, and Dukhande, Vikas V.

Abstract

R4625 --> Glioblastoma multiforme (GBM) is a grade IV malignant glioma. It is a highly proliferative brain tumor with the 5‐year survival rate close to 5% indicating a high mortality rate. Current treatment strategies include surgery, radiation, and chemotherapy. Development of resistance against the current treatment options and the blood brain barrier (BBB) pose major challenges in GBM management. Therefore, we studied an FDA‐approved drug stiripentol which is used for Dravet's syndrome (a rare form of epilepsy) for its efficacy in GBM. Stiripentol decreased the cytotoxicity in U87 and U138 astrocytoma cells. Cell proliferation and clonogenic survival of U87 cells was also adversely affected by stiripentol. Cellular anticancer activity was studied by cell cycle assay, apoptosis assay by flow cytometry, and by measuring the expression of apoptotic markers by Western blotting. In addition, effect of stiripentol on key cell signaling proteins was determined using Western blotting. Stiripentol treatment induced apoptosis and resulted in cell cycle arrest in GBM cells. 3D spheroid assay was performed to replicate the tumor environment and analyze the multidirectional metastatic growth of the cancer cells in presence of stiripentol and the standard GBM therapeutic Temozolomide (TMZ). Fluorescence imaging of spheroids demonstrated anticancer effects of stiripentol and TMZ. Further in vivo studies will be performed on xenograft models of astrocytoma cells. Our results indicate that stiripentol can be an effective GBM therapeutic and merits further investigation. [ABSTRACT FROM AUTHOR]

Published

2021

7. Systemic Immuno-metabolic alterations in chronic obstructive pulmonary disease (COPD).

Author

Agarwal, Amit R, Kadam, Smita, Brahme, Ankita, Agrawal, Manas, Apte, Komalkirti, Narke, Govinda, Kekan, Kushal, Madas, Sapna, and Salvi, Sundeep

Subjects

*OBSTRUCTIVE lung diseases, *INFLUENZA, *MANN Whitney U Test, *CIGARETTE smoke, *CELL physiology, *SMOKING

Abstract

Background: Metabolic adaptation in immune cells is necessary to modulate immune cell function as it is intricately coupled with intracellular metabolism. We aimed to characterize the metabolic state of human peripheral blood mononuclear cells (PBMCs) after long-term exposure to tobacco smoke in smokers with preserved lung function and COPD subjects.Methods: PBMCs were isolated from healthy non-smokers (HNS), healthy smokers (HS) and COPD subjects, cultured and the mitochondrial respiration while utilizing glucose (glycolysis), fatty acids (β-oxidation) or pyruvate (direct Krebs' cycle substrate) was measured using the XFp Extracellular Flux Analyzer. Plasma levels of inflammatory cytokines IFN-γ, IL-17, TNF-α, IL-5, IL-9 and IFN-α were measured using flow cytometry. RAW264.7 cells were exposed to cigarette smoke condensate (CSC) for 1 h and its effect on cell viability, cellular metabolism and phagocytosis ability were also studied. Patient's data was analyzed using the Mann Whitney U test, whereas Student's t test was performed to analyze the in-vitro data.Results: PBMCs from COPD subjects showed a significant decrease in extracellular acidification rate (ECAR) while utilizing glucose as compared to HNS (151.9 Vs 215%). Mitochondrial oxygen consumption rate (OCR) on palmitate or pyruvate was also found to be significantly lower in COPD subjects as compared to HS and a strong positive correlation between palmitate OCR in PBMCs and FEV1 (r = 0.74, p < 0.05) and FVC (r = 0.79, p < 0.05) values in HS was observed. The metabolic shift towards fatty acid metabolism in healthy smokers promoted an inflammatory cytokine response with a greater increase in the levels of IL-5, IL-9 and IFN-α as compared to IFN-γ, IL-17 and TNF-α. In-vitro experiments with RAW 264.7 cells showed similar metabolic alterations and a reduced ability to phagocytose Streptococcus pneumonia and Haemophilus influenza after cigarette smoke exposure in the presence of glucose or palmitate.Conclusions: These findings indicate a metabolic basis for the inflammatory response in COPD and could suggest a new therapeutic target for controlling the immune response and delaying the onset of disease.Trial Registration: This observational study was retrospectively registered in the Clinical Trails Registry - India (ICMR - NIMS) on 19th January 2018 with the registration number CTRI/2018/01/011441 . [ABSTRACT FROM AUTHOR]

Published

2019