Identification of <scp>benzothiazole‐rhodanine</scp> derivatives as <scp>α‐amylase</scp> and <scp>α‐glucosidase</scp> inhibitors: Design, synthesis, in silico, and in vitro analysis

Srinivasa, Mahendra Gowdru; Aggarwal, Natasha Naval; Gatpoh, Banylla Felicity Dkhar; Shankar, Madan Kumar; Ravindranath, Kannika Byadarahalli; Veeranna, Pujar Gurubasavaraj; Dixit, Sheshagiri R.; Mandal, Subhankar P.; Ravanappa, Prashantha Kumar Bommenahally; Khanal, Pukar; Chandrashekarappa, Revanasiddappa Bistuvalli

doi:10.1002/jmr.2959

Cited by 8 publications

(4 citation statements)

References 34 publications

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“…determined that compounds containing rhodanine benzothiazole are α‐amylase and α‐glucosidase inhibitors. Due to the electron‐donating group (OH) positioned at position‐4, compound 45 has strong inhibitory effects on α‐glucosidase and α‐amylase activity with IC 50 : 24.61±1.76 μM and 24.64±2.10 μM respectively [53] …”

Section: Discussionmentioning

confidence: 99%

“…Due to the electron-donating group (OH) positioned at position-4, compound 45 has strong inhibitory effects on α-glucosidase and α-amylase activity with IC 50 : 24.61 � 1.76 μM and 24.64 � 2.10 μM respectively. [53] Patil Ser497, and Ser505. [54] RB C et al identified rhodanine benzothiazole compounds as α-amylase and α-glucosidase inhibitors.…”

Section: Pharmacological Characteristics Of Benzothiazole Analoguesmentioning

confidence: 98%

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Recent Studies of Nitrogen and Sulfur Containing Heterocyclic Analogues as Novel Antidiabetic Agents: A Review

Gharge,

Alegaon

2024

Chemistry & Biodiversity

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The prevalence of diabetes mellitus is on the rise, which demands for the identification of novel antidiabetic drugs. There is a need for safer and more effective alternatives because the therapy methods now available to manage diabetes have limits. Due to their diverse pharmacological characteristics, heterocyclic molecules with nitrogen and Sulfur atoms have become intriguing candidates in medicinal chemistry. These substances have a wide variety of structures that can be customized to target different pathways associated with diabetes and can affect important biological targets involved in glucose homeostasis. This review provides a thorough summary of the most recent studies on heterocyclic analogues of nitrogen and Sulfur as prospective antidiabetic agents. This review examines the variety of their structural forms, their methods of action, and assesses the results of preclinical and clinical investigations on their effectiveness and safety. Additionally, further optimization and development of innovative antidiabetic medications are highlighted, as well as the difficulties and prospects for the future in utilizing the therapeutic potential of these analogues. This study seeks to stimulate additional investigation and cooperation between researchers and medicinal chemists, promoting improvements in the creation of efficient and secure antidiabetic medicines to fulfil the needs in the management of diabetes.

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Section: Discussionmentioning

confidence: 99%

Section: Pharmacological Characteristics Of Benzothiazole Analoguesmentioning

confidence: 98%

Recent Studies of Nitrogen and Sulfur Containing Heterocyclic Analogues as Novel Antidiabetic Agents: A Review

Gharge,

Alegaon

2024

Chemistry & Biodiversity

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“…Benzothiazole clubbed derivatives of rhodanine 25 a – j were synthesized by Srinivasa and coauthors [82] and evaluated for their antidiabetic potential against α‐amylase and α‐glucosidase enzymes. Compounds 25 e and 25 i displayed comparable inhibitory potential with IC 50 =24.22 and 24.64 μM, respectively, against α‐amylase enzyme with standard Acarbose (IC 50 =24.35 μM), whereas with α‐glucosidase, compounds 25 g and 25 i displayed significant inhibition with IC 50 =24.74 and 24.61 μM, respectively.…”

Section: Thiazolidinone Based α‐Amylase Inhibitorsmentioning

confidence: 99%

α‐Amylase Inhibitors Based on Thiazolidinone Skeleton: A Promising Approach in Diabetes Management

Singh,

Sindhu,

Kumar

et al. 2023

ChemistrySelect

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Thiazolidinone scaffold has become a promising scaffold when it comes to therapeutic importance, and researchers are quite interested in it because of its wide range of applications in the different fields of chemistry. The capacity of this nucleus to interact with a variety of biological targets, including the peroxisome proliferator‐activated receptor (PPAR), protein tyrosine phosphatase 1B, aldose reductase, α‐glucosidase, and α‐amylase, has led to the observation of its antidiabetic effect. α‐Amylase (α‐1,4‐glucan‐4‐glucanohydrolase, EC 3.2.1.1) is one of the most important industrial endoamylases capable of hydrolyzing the internal α‐1,4‐glycosidic bonds in polysaccharides with net retention of α‐anomeric configuration in low molecular weight products, such as glucose, maltose, and maltotriose units. The inhibitors of α‐amylase have the ability to lower endogenous activity, which is crucial for the management of agricultural pests as well as the treatment and prevention of human disorders. In the present review, we attempted to compile the most recent studies on thiazolidinone‐based α‐amylase inhibitors, investigate their therapeutic potential in treating diabetes, comprehend the relationships between structure and activity, offer suggestions for future research and translation of these findings into clinical applications. This comprehensive review strives to be a valuable resource for researchers, medicinal chemists, and healthcare professionals involved in developing and applying novel therapeutics for treating metabolic disorders.

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“…In case of analog 5 and 6, interactions were found such as vander Waals, conventional hydrogen bond, Pi-anion, Pi-Sigma, alkyl, Pi-alkyl, salt bridge, halogen, Pi-sulphur, etc. The further detail of docking study were summarized as in our previous articles [ 30 , 31 , 32 , 33 , 34 , 35 ] and the assay protocols of both the activities have been added in Supplementary file [ 36 , 37 ].…”

Section: Biological Profilementioning

confidence: 99%

Synthesis, In Vitro Anti-Microbial Analysis and Molecular Docking Study of Aliphatic Hydrazide-Based Benzene Sulphonamide Derivatives as Potent Inhibitors of α-Glucosidase and Urease

et al. 2022

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A unique series of sulphonamide derivatives was attempted to be synthesized in this study using a new and effective method. All of the synthesized compounds were verified using several spectroscopic methods, including FTIR, 1H-NMR, 13C-NMR, and HREI-MS, and their binding interactions were studied using molecular docking. The enzymes urease and α-glucosidase were evaluated against each derivative (1–15). When compared to their respective standard drug such as acarbose and thiourea, almost all compounds were shown to have excellent activity. Among the screened series, analogs 5 (IC50 = 3.20 ± 0.40 and 2.10 ± 0.10 µM) and 6 (IC50 = 2.50 ± 0.40 and 5.30 ± 0.20 µM), emerged as potent molecules when compared to the standard drugs acarbose (IC50 = 8.24 ± 0.08 µM) and urease (IC50 = 7.80 ± 0.30). Moreover, an anti-microbial study also demonstrated that analogs 5 and 6 were found with minimum inhibitory concentrations (MICs) in the presence of standard drugs streptomycin and terinafine.

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Identification of benzothiazole‐rhodanine derivatives as α‐amylase and α‐glucosidase inhibitors: Design, synthesis, in silico, and in vitro analysis

Cited by 8 publications

References 34 publications

Recent Studies of Nitrogen and Sulfur Containing Heterocyclic Analogues as Novel Antidiabetic Agents: A Review

Recent Studies of Nitrogen and Sulfur Containing Heterocyclic Analogues as Novel Antidiabetic Agents: A Review

α‐Amylase Inhibitors Based on Thiazolidinone Skeleton: A Promising Approach in Diabetes Management

Synthesis, In Vitro Anti-Microbial Analysis and Molecular Docking Study of Aliphatic Hydrazide-Based Benzene Sulphonamide Derivatives as Potent Inhibitors of α-Glucosidase and Urease

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