Search

Your search keyword '"Khetan, Riya"' showing total 4 results
Start Over Author "Khetan, Riya" Search Limiters Available in Library Collection
4 results on '"Khetan, Riya"'

1. Unveiling G-protein coupled receptors as potential targets for ovarian cancer nanomedicines: from RNA sequencing data analysis to in vitro validation.

Author

Khetan, Riya, Eldi, Preethi, Lokman, Noor A., Ricciardelli, Carmela, Oehler, Martin K., Blencowe, Anton, Garg, Sanjay, Pillman, Katherine, and Albrecht, Hugo

Subjects
*RNA sequencing, *OVARIAN cancer, *G protein coupled receptors, *NANOMEDICINE, *GENE expression
Abstract

Genetic heterogeneity in ovarian cancer indicates the need for personalised treatment approaches. Currently, very few G-protein coupled receptors (GPCRs) have been investigated for active targeting with nanomedicines such as antibody-conjugated drugs and drug-loaded nanoparticles, highlighting a neglected potential to develop personalised treatment. To address the genetic heterogeneity of ovarian cancer, a future personalised approach could include the identification of unique GPCRs expressed in cancer biopsies, matched with personalised GPCR-targeted nanomedicines, for the delivery of lethal drugs to tumour tissue before, during and after surgery. Here we report on the systematic analysis of public ribonucleic acid-sequencing (RNA-seq) gene expression data, which led to prioritisation of 13 GPCRs as candidates with frequent overexpression in ovarian cancer tissues. Subsequently, primary ovarian cancer cells derived from ascites and ovarian cancer cell lines were used to confirm frequent gene expression for the selected GPCRs. However, the expression levels showed high variability within our selection of samples, therefore, supporting and emphasising the need for the future development of case-to-case personalised targeting approaches. [ABSTRACT FROM AUTHOR]

Published
2024
Full Text
View/download PDF

4. Using GPCRs as molecular beacons to target ovarian cancer with nanomedicines

Author

Riya Khetan, Cintya Dharmayanti, Todd A. Gillam, Eric Kübler, Manuela Klingler-Hoffmann, Carmela Ricciardelli, Martin K. Oehler, Anton Blencowe, Sanjay Garg, Hugo Albrecht, Khetan, Riya, Dharmayanti, Cintya, Gillam, Todd A, Kübler, Eric, Klingler-Hoffmann, Manuela, Ricciardelli, Carmela, Oehler, Martin K, Blencowe, Anton, Garg, Sanjay, and Albrecht, Hugo

Subjects
active targeting, internalization, Cancer Research, GPCR, ovarian cancer, Oncology, nanoparticle, receptor, drug delivery, G protein-coupled receptor, ligand
Abstract

Refereed/Peer-reviewed The five-year survival rate for women with ovarian cancer is very poor despite radical cytoreductive surgery and chemotherapy. Although most patients initially respond to platinum-based chemotherapy, the majority experience recurrence and ultimately develop chemoresistance, resulting in fatal outcomes. The current administration of cytotoxic compounds is hampered by dose-limiting severe adverse effects. There is an unmet clinical need for targeted drug delivery systems that transport chemotherapeutics selectively to tumor cells while minimizing off-target toxicity. G protein-coupled receptors (GPCRs) are the largest family of membrane receptors, and many are overexpressed in solid tumors, including ovarian cancer. This review summarizes the progress in engineered nanoparticle research for drug delivery for ovarian cancer and discusses the potential use of GPCRs as molecular entry points to deliver anti-cancer compounds into ovarian cancer cells. A newly emerging treatment paradigm could be the personalized design of nanomedicines on a case-by-case basis.

Published
2022

Catalog

Books, media, physical & digital resources
See catalog results