Inhibitory effect of Nifedipine on aldose reductase delays cataract progression

Alaparthi Malini Devi; Venu Sankeshi; Arugonda Ravali; Srinivas Bandaru; Vinay Kumar Theendra; Someswar Rao Sagurthi

doi:10.1007/s00210-023-02588-1

Inhibitory effect of Nifedipine on aldose reductase delays cataract progression

Naunyn Schmiedebergs Arch Pharmacol. 2024 Jan;397(1):161-171. doi: 10.1007/s00210-023-02588-1. Epub 2023 Jul 3.

Authors

Alaparthi Malini Devi¹, Venu Sankeshi¹, Arugonda Ravali¹, Srinivas Bandaru², Vinay Kumar Theendra³, Someswar Rao Sagurthi⁴

Affiliations

¹ Drug Design & Molecular Medicine Laboratory, Department of Genetics & Biotechnology, Osmania University, Hyderabad, 500007, India.
² Department of Biotechnology, Koneru Lakshmaiah Education Foundation (Deemed to be University), Guntur, 522302, India.
³ Department of Pharmacology, Nirmala College of Pharmacy, Guntur, 522503, India.
⁴ Drug Design & Molecular Medicine Laboratory, Department of Genetics & Biotechnology, Osmania University, Hyderabad, 500007, India. drsomeswar@osmania.ac.in.

PMID: 37395794
DOI: 10.1007/s00210-023-02588-1

Abstract

Aldose reductase (ALR2) is a rate-limiting component of the polyol pathway, which is essential for the NADPH-mediated conversion from glucose to sorbitol. ALR2 dysregulation has been linked to α-crystallin aggregation, increased oxidative stress, and calcium inflow, all of which contribute to a diabetic cataract. Given its crucial role in occular pathologies, ALR2 has emerged as a promising target to treat oxidative stress and hyperglycaemic condition which form the underlying cause of diabetic cataracts. However, several of them had issues with sensitivity and specificity to ALR2, despite being screened as effective ALR2 inhibitors from a wide range of structurally varied molecules. The current study investigates the inhibitory potential of Nifedipine, an analog of the dihydro nicotinamide class of compounds against ALR2 activity. The enzyme inhibition studies were supported by in vitro biomolecular interactions, molecular modeling approaches, and in vivo validation in diabetic rat models. Nifedipine demonstrated appreciable inhibitory potential with the purified recombinant hAR (human aldose reductase; with an IC50 value of 2.5 µM), which was further supported by Nifedipine-hAR binding affinity (Kd = 2.91 ± 1.87 × 10^-4 M) by ITC and fluorescence quenching assays. In the in vivo models of STZ-induced diabetic rats, Nifedipine delayed the onset progression of cataracts by preserving the antioxidant enzyme activity (SOD, CAT, and GPX GSH, TBARS, and protein carbonyls) and was shown to retain the α-crystallin chaperone activity by reducing the calcium levels in the diabetic rat lens. In conclusion, our results demonstrate effective inhibition of ALR2 by Nifedipine, resulting in amelioration of diabetic cataract conditions by lowering oxidative and osmotic stress while retaining the chaperone activity of α-crystallins. The present study could be envisaged to improve the eye condition in older adults upon Nifedipine treatment.

Keywords: Aldose reductase (ALR2); Cataract; Nifedipine; α-Crystallins.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Aged
Aldehyde Reductase
Animals
Antioxidants / therapeutic use
Calcium
Cataract* / drug therapy
Cataract* / prevention & control
Diabetes Mellitus, Experimental* / drug therapy
Enzyme Inhibitors / pharmacology
Humans
Nifedipine / pharmacology
Nifedipine / therapeutic use
Rats
alpha-Crystallins* / metabolism

Substances

Nifedipine
Aldehyde Reductase
Calcium
Antioxidants
Enzyme Inhibitors
alpha-Crystallins

Grants and funding

C-DST-PURSE-II/26/2017/DST-PURSE, INDIA