Dinne Naresh Kumar Reddy scite author profile

Dinne Naresh Kumar Reddy

4Publications

19Citation Statements Received

75Citation Statements Given

How they've been cited

How they cite others

126

Affiliations

Dr. Reddy's Laboratories (India), Jawaharlal Nehru Technological University Anantapur

Publications

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Development of a Chemoenzymatic Process for Dehydroepiandrosterone Acetate Synthesis

Fryszkowska

Peterson

Davies

et al. 2016

Org. Process Res. Dev.

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Dehydroepiandrosterone (DHEA, 2) is an important endogenous steroid hormone in mammals used in the treatment of a variety of dysfunctions in female and male health, 1 as well as an intermediate in the synthesis of steroidal drugs, such as abiraterone acetate which is used for the treatment of prostate cancer. 2−4 In this manuscript we describe a novel, concise, and cost-efficient route toward DHEA (2) and DHEA acetate (3) from 4-androstene-3,17-dione (4-AD, 1). Crucial to success was the identification of a ketoreductase from Sphingomonas wittichii for the highly regio-and stereoselective reduction of the C3carbonyl group of 5-androstene-3,17-dione (5) to the required 3β-alcohol (2, >99% de). The enzyme displayed excellent robustness and solvent stability under high substrate concentrations (up to 150 g/L).

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SnCl2·2H2O as a precatalyst in MCR: synthesis of pyridine derivatives via a 4-component reaction in water

Reddy

Chandrasekhar

Ganesh

et al. 2015

Tetrahedron Letters

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Catalysis by zeolite leading to the construction of thiazole ring: an improved synthesis of 4-alkynyl substituted thiazoles

Arunkumar¹,

Reddy²,

Chandrasekhar³

et al. 2012

Tetrahedron Letters

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Characterization of Five Oxidative Degradation Impurities and One Process Impurity of Suvorexant Drug Substance by LC-MS/MS, HR-MS and 1D, 2D NMR: Validation of Suvorexant Drug Substance and Process Impurities by HPLC and UPLC

Rajana

Devi

Reddy

et al. 2020

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During the oxidative (10% H2O2) degradation of suvorexant drug substance, around 1.0% of one impurity and less than 1.0% four impurities were found by a new high-performance liquid chromatography (HPLC) assay and related substance method. The mass numbers of 1.0% impurity was 469 [M + H]+, remaining four impurities were 172 [M + H]+, 467 [M + H]+, 483 [M + H]+ and 485 [M + H]+. The 469 [M + H]+, 485[M + H] and 172 [M + H]+ impurities were characterized by using the LC-MS/MS, HR-MS and 1D, 2D NMR spectroscopic data. The 172 [M + H]+ impurity was prepared synthetically and co-injected in HPLC. The retention time of synthesized 172 [M + H]+ impurity was matching with the unknown degradation impurity in HPLC. The developed mass compatible HPLC and ultra performance liquid chromatography methods were validated for drug substance and process impurities by following ICH Q2 (R1) guidelines.

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