Issue 33, 2024
From the journal:

Chemical Communications

Molecular recognition and proteoglycan mimic arrangement: modulating cisplatin toxicity

Saurabh Anand,a   Sandhya Mardhekar,a   Preeti Ravindra Bhoge,a   Sandeep Kumar Mishraa  and  Raghavendra Kikkeri ORCID logo *a  

* Corresponding authors

a Indian Institute of Science Education and Research, Dr Homi Bhabha Road, Pashan, Pune 4110008, India
E-mail: rkikkeri@iiserpune.ac.in
Fax: +91-20-25908207
Tel: +91-20-25908207

Abstract

We have demonstrated that cisplatin (CP), an anticancer drug, showed a preference for binding the sulfated-L-iduronic acid (S-L-IdoA) unit over the sulfated-D-glucuronic acid unit of heparan sulfate. The multivalency of S-L-IdoA, such as in the proteoglycan mimic, resulted in distinct modes of cell-surface engineering in normal and cancer cells, with these disparities having a significant impact on CP-mediated toxicity.

Graphical abstract: Molecular recognition and proteoglycan mimic arrangement: modulating cisplatin toxicity

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Article information

DOI
https://doi.org/10.1039/D4CC00464G
Article type
Communication
Submitted
30 Jan 2024
Accepted
21 Feb 2024
First published
21 Feb 2024

Chem. Commun., 2024,60, 4495-4498

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Molecular recognition and proteoglycan mimic arrangement: modulating cisplatin toxicity

S. Anand, S. Mardhekar, P. R. Bhoge, S. K. Mishra and R. Kikkeri, Chem. Commun., 2024, 60, 4495 DOI: 10.1039/D4CC00464G

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