Your search keyword '"Keri, Rangappa S"' showing total 6 results

1. Benzimidazole–Oxadiazole Hybrids—Development in Medicinal Chemistry: An Overview.

Author

Bhat, Raveendra Madhukar, Hegde, Venkatraman, Budagumpi, Srinivasa, Adimule, Vinayak, and Keri, Rangappa S.

Subjects

DRUG discovery, PHARMACEUTICAL chemistry, ANTITUBERCULAR agents, FUNCTIONAL groups, ANTIHYPERTENSIVE agents

Abstract

To increase the success rate of drug discovery, one practical strategy is to begin molecular hybridisation. The presence of two or more pharmacophores in a single unit leads to a pharmacological potency greater than the sum of each individual moiety's potency. Heterocyclic compounds are very widely distributed in nature and are essential for life activities. Benzimidazole and oxadiazole are privileged structures in medicinal chemistry and are widely used in drug discovery and development due to their vast biological properties. The drug‐like properties (like pharmacokinetics and pharmacodynamics) of the individual scaffolds can be improved by benzimidazole–oxadiazole chimeric molecules via a molecular hybridisation approach. Benzimidazole and oxadiazole cores can either be fused or incorporated using either functional groups/bonds. Over the last few decades, drug discovery scientists have predicted that these moieties could be interconnected to yield a novel or modified hybrid compound. Benzimidazole and oxadiazole hybrids were identified as the most potent anticancer, antimicrobial, anti‐inflammatory, antioxidant, anticonvulsant, antidepressant, antihypertensive and antitubercular agents. In this context, the present review describes the biological properties of benzimidazole–oxadiazole (1,3,4 and 1,2,4) hybrids, their possible structure–activity relationship and the mechanism of action studies presented. This review article is intended to stimulate fresh ideas in the search for rational designs of more active and less toxic benzimidazole–oxadiazole hybrid prospective therapeutic candidates, as well as more effective diagnostic agents and pathologic probes. [ABSTRACT FROM AUTHOR]

Published

2024

2. Synthetic and natural coumarins as potent anticonvulsant agents: A review with structure–activity relationship.

Author

Keri, Rangappa S., Budagumpi, Srinivasa, and Balappa Somappa, Sasidhar

Subjects

*ANTICONVULSANTS, *AZEPINES, *BIOLOGICAL products, *DRUG design, *BENZOPYRANS, *MOLECULAR structure, *PHARMACEUTICAL chemistry, *PHARMACODYNAMICS

Abstract

What is known and objective: The main objective of this review is to highlight the most relevant studies since 1990 (to date) in the area of medicinal chemistry aspects to provide a panoramic view to the biologists/medicinal chemists working in this area and would assist them in their efforts to design, synthesize and extract (from natural source) coumarin‐based anticonvulsant agents. Also, the structure–activity relationship (SAR) studies are also discussed for further rational design of this kind of derivatives. It is hoped that this review will be helpful for new thoughts in the quest for rational designs of more active and less toxic coumarin‐based antiepileptic agents. Methods: A literature review emphasizing the application of coumarin core as antiepileptic agents identify articles related to the topic; we performed a standardized search from 1990 to November 2021, using search engines like Scifinder, web of Science, Pubmed and Scopus. Results and discussion: This review gives an overview of attempts to shed light and compile published reports on coumarin derivatives along with some opinions on different approaches to help the medicinal chemists in designing future generation potent yet safer anticonvulsant agents. The possible structure–activity relationships (SARs) will also be discussed to indicate the direction for the rational design of more effective candidates. What is new and conclusion: The findings from this review provide new indications or directions for the discovery of new and better drugs from synthetic and naturally occurring coumarins as antiepileptic agents. In our review, we have tried to depict the recent researches which made in the design and development of novel anticonvulsant compounds with coumarin nucleus. Also, SAR of expressed derivatives indicated that the choice of a fitting substitution containing electron‐withdrawing/donating groups to coumarin or with some heterocyclic moieties joined to parent coumarin skeleton assumes an essential role in changing the anticonvulsant activity of synthesized derivatives. These findings encourage the scientific community towards the optimization of the pharmacological profile of this structural moiety as an important scaffold for the treatment of epilepsy. [ABSTRACT FROM AUTHOR]

Published

2022

3. An overview of benzo[b]thiophene-based medicinal chemistry.

Author

Keri, Rangappa S., Chand, Karam, Budagumpi, Srinivasa, Balappa Somappa, Sasidhar, Patil, Siddappa A., and Nagaraja, Bhari Mallanna

Subjects

*THIOPHENES, *PHARMACEUTICAL chemistry, *DRUG design, *HETEROCYCLIC compound derivatives, *STRUCTURE-activity relationships

Abstract

Among sulfur containing heterocycles, benzothiophene and its derivatives are at the focus as these candidates have structural similarities with active compounds to develop new potent lead molecules in drug design. Benzo [b] thiophene scaffold is one of the privileged structures in drug discovery as this core exhibits various biological activities allowing them to act as anti-microbial, anti-cancer, anti-inflammatory, anti-oxidant, anti-tubercular, anti-diabetic, anti-convulsant agents and many more. Further, numerous benzothiophene-based compounds as clinical drugs have been extensively used to treat various types of diseases with high therapeutic potency, which has led to their extensive developments. Due to the wide range of biological activities of benzothiophene, their structure activity relationships (SAR) have generated interest among medicinal chemists, and this has culminated in the discovery of several lead molecules against numerous diseases. The present review is endeavoring to highlight the progress in the various pharmacological activities of benzo [b] thiophene derivatives. It is hoped that this review will be helpful for new thoughts in the quest for rational designs of more active and less toxic benzothiophene-based medicinal drugs, as well as more effective diagnostic agents and pathologic probes. Also, SAR studies that highlight the chemical groups responsible for evoking the potential activities of benzothiophene derivatives are studied and compared. [ABSTRACT FROM AUTHOR]

Published

2017

4. Triazole: A Promising Antitubercular Agent.

Author

Keri, Rangappa S., Patil, Siddappa A., Budagumpi, Srinivasa, and Nagaraja, Bhari Mallanna

Subjects

*ANTITUBERCULAR agents, *TRIAZOLES, *TUBERCULOSIS treatment, *MICROBIOLOGISTS, *PHARMACEUTICAL chemistry

Abstract

Tuberculosis is a contagious disease with comparatively high mortality worldwide. The statistics shows that around three million people throughout the world die annually from tuberculosis and there are around eight million new cases each year, of which developing countries showed major share. Therefore, the discovery and development of effective antituberculosis drugs with novel mechanism of action have become an insistent task for infectious diseases research programs. The literature reveals that, heterocyclic moieties have drawn attention of the chemists, pharmacologists, microbiologists, and other researchers owing to its indomitable biological potential as anti-infective agents. Among heterocyclic compounds, triazole (1,2,3-triazole/1,2,4-triazole) nucleus is one of the most important and well-known heterocycles, which is a common and integral feature of a variety of natural products and medicinal agents. Triazole core is considered as a privileged structure in medicinal chemistry and is widely used as 'parental' compounds to synthesize molecules with medical benefits, especially with infection-related activities. In the present review, we have collated published reports on this versatile core to provide an insight so that its complete therapeutic potential can be utilized for the treatment of tuberculosis. This review also explores triazole as a potential targeted core moiety against tuberculosis and various research ongoing worldwide. It is hoped that this review will be helpful for new thoughts in the quest for rational designs of more active and less toxic triazole-based antituberculosis drugs. [ABSTRACT FROM AUTHOR]

Published

2015

5. Comprehensive Review in Current Developments of Benzimidazole-Based Medicinal Chemistry.

Author

Keri, Rangappa S., Hiremathad, Asha, Budagumpi, Srinivasa, and Nagaraja, Bhari Mallanna

Subjects

*BENZIMIDAZOLE derivatives, *PHARMACEUTICAL chemistry, *MOLECULAR pharmacology, *ANTINEOPLASTIC agents, *SUBSTITUTION reactions

Abstract

The properties of benzimidazole and its derivatives have been studied over more than one hundred years. Benzimidazole derivatives are useful intermediates/subunits for the development of molecules of pharmaceutical or biological interest. Substituted benzimidazole derivatives have found applications in diverse therapeutic areas such as antiulcer, anticancer agents, and anthelmintic species to name just a few. This work systematically gives a comprehensive review in current developments of benzimidazole-based compounds in the whole range of medicinal chemistry as anticancer, antibacterial, antifungal, anti-inflammatory, analgesic agents, anti- HIV, antioxidant, anticonvulsant, antitubercular, antidiabetic, antileishmanial, antihistaminic, antimalarial agents, and other medicinal agents. This review will further be helpful for the researcher on the basis of substitution pattern around the nucleus with an aim to help medicinal chemists for developing an SAR on benzimidazole drugs/compounds. [ABSTRACT FROM AUTHOR]

Published

2015

6. ChemInform Abstract: A Comprehensive Review in Current Developments of Benzothiazole-Based Molecules in Medicinal Chemistry.

Author

Keri, Rangappa S., Patil, Mahadeo R., Patil, Siddappa A., and Budagumpi, Srinivasa

Subjects

*PHARMACEUTICAL chemistry, *BENZOTHIAZOLE

Abstract

Review: 294 refs. [ABSTRACT FROM AUTHOR]

Published

2015