Recent Trends in Rationally Designed Molecules as Kinase Inhibitors

Parteek Prasher; Mousmee Sharma; Yinghan Chan; Sachin Kumar Singh; Krishnan Anand; Harish Dureja; Niraj Kumar Jha; Gaurav Gupta; Flavia Zacconi; Dinesh K. Chellappan; Kamal Dua

doi:10.2174/0929867328666211111161811

Recent Trends in Rationally Designed Molecules as Kinase Inhibitors

Parteek Prasher
, Mousmee Sharma
, Yinghan Chan
, Sachin Kumar Singh
, Krishnan Anand
, Harish Dureja
, Niraj Kumar Jha
, Gaurav Gupta
, Flavia Zacconi
, Dinesh K. Chellappan
, Kamal Dua

University of Petroleum and Energy Studies
Uttaranchal University
International Medical University
Lovely Professional University
University of The Free State
Maharshi Dayanand University
Sharda University
Suresh Gyan Vihar University
Pontificia Universidad Católica de Chile
University of Technology Sydney

Research output: Contribution to journal › Review article › peer-review

4 Scopus citations

Abstract

Protein kinases modulate the structure and function of proteins by adding phosphate groups to threonine, tyrosine, and serine residues. The phosphorylation process mediated by the kinases regulates several physiological processes, while their overexpression results in the development of chronic diseases, including cancer. Targeting of receptor tyro-sine kinase pathways results in the inhibition of angiogenesis and cell proliferation that vali-dates kinases as a key target in the management of aggressive cancers. As such, the identification of protein kinase inhibitors revolutionized the contemporary anticancer therapy by inducing a paradigm shift in the management of disease pathogenesis. Contemporary drug design programs focus on a broad range of kinase targets for the development of novel pharmacophores to manage the overexpression of kinases and their pathophysiology in cancer pathogenesis. In this review, we present the emerging trends in the development of rationally designed molecular inhibitors of kinases over the last five years (2016-2021) and their incipient role in the development of impending anticancer pharmaceuticals.

Original language	English
Pages (from-to)	1529-1567
Number of pages	39
Journal	Current Medicinal Chemistry
Volume	30
Issue number	13
DOIs	https://doi.org/10.2174/0929867328666211111161811
State	Published - 2023
Externally published	Yes

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

Keywords

GPCR kinase
Kinases
MAP kinase
RAF-kinase
VEGFR-2
cancer
cyclic dependent kinase
inhibitors
pharmacophore

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10.2174/0929867328666211111161811

Cite this

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title = "Recent Trends in Rationally Designed Molecules as Kinase Inhibitors",

abstract = "Protein kinases modulate the structure and function of proteins by adding phosphate groups to threonine, tyrosine, and serine residues. The phosphorylation process mediated by the kinases regulates several physiological processes, while their overexpression results in the development of chronic diseases, including cancer. Targeting of receptor tyro-sine kinase pathways results in the inhibition of angiogenesis and cell proliferation that vali-dates kinases as a key target in the management of aggressive cancers. As such, the identification of protein kinase inhibitors revolutionized the contemporary anticancer therapy by inducing a paradigm shift in the management of disease pathogenesis. Contemporary drug design programs focus on a broad range of kinase targets for the development of novel pharmacophores to manage the overexpression of kinases and their pathophysiology in cancer pathogenesis. In this review, we present the emerging trends in the development of rationally designed molecular inhibitors of kinases over the last five years (2016-2021) and their incipient role in the development of impending anticancer pharmaceuticals.",

keywords = "GPCR kinase, Kinases, MAP kinase, RAF-kinase, VEGFR-2, cancer, cyclic dependent kinase, inhibitors, pharmacophore",

author = "Parteek Prasher and Mousmee Sharma and Yinghan Chan and Singh, \{Sachin Kumar\} and Krishnan Anand and Harish Dureja and Jha, \{Niraj Kumar\} and Gaurav Gupta and Flavia Zacconi and Chellappan, \{Dinesh K.\} and Kamal Dua",

note = "Publisher Copyright: {\textcopyright} 2023 Bentham Science Publishers.",

year = "2023",

doi = "10.2174/0929867328666211111161811",

language = "English",

volume = "30",

pages = "1529--1567",

journal = "Current Medicinal Chemistry",

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T1 - Recent Trends in Rationally Designed Molecules as Kinase Inhibitors

AU - Prasher, Parteek

AU - Sharma, Mousmee

AU - Chan, Yinghan

AU - Singh, Sachin Kumar

AU - Anand, Krishnan

AU - Dureja, Harish

AU - Jha, Niraj Kumar

AU - Gupta, Gaurav

AU - Zacconi, Flavia

AU - Chellappan, Dinesh K.

AU - Dua, Kamal

PY - 2023

Y1 - 2023

N2 - Protein kinases modulate the structure and function of proteins by adding phosphate groups to threonine, tyrosine, and serine residues. The phosphorylation process mediated by the kinases regulates several physiological processes, while their overexpression results in the development of chronic diseases, including cancer. Targeting of receptor tyro-sine kinase pathways results in the inhibition of angiogenesis and cell proliferation that vali-dates kinases as a key target in the management of aggressive cancers. As such, the identification of protein kinase inhibitors revolutionized the contemporary anticancer therapy by inducing a paradigm shift in the management of disease pathogenesis. Contemporary drug design programs focus on a broad range of kinase targets for the development of novel pharmacophores to manage the overexpression of kinases and their pathophysiology in cancer pathogenesis. In this review, we present the emerging trends in the development of rationally designed molecular inhibitors of kinases over the last five years (2016-2021) and their incipient role in the development of impending anticancer pharmaceuticals.

AB - Protein kinases modulate the structure and function of proteins by adding phosphate groups to threonine, tyrosine, and serine residues. The phosphorylation process mediated by the kinases regulates several physiological processes, while their overexpression results in the development of chronic diseases, including cancer. Targeting of receptor tyro-sine kinase pathways results in the inhibition of angiogenesis and cell proliferation that vali-dates kinases as a key target in the management of aggressive cancers. As such, the identification of protein kinase inhibitors revolutionized the contemporary anticancer therapy by inducing a paradigm shift in the management of disease pathogenesis. Contemporary drug design programs focus on a broad range of kinase targets for the development of novel pharmacophores to manage the overexpression of kinases and their pathophysiology in cancer pathogenesis. In this review, we present the emerging trends in the development of rationally designed molecular inhibitors of kinases over the last five years (2016-2021) and their incipient role in the development of impending anticancer pharmaceuticals.

KW - GPCR kinase

KW - Kinases

KW - MAP kinase

KW - RAF-kinase

KW - VEGFR-2

KW - cancer

KW - cyclic dependent kinase

KW - inhibitors

KW - pharmacophore

UR - https://www.scopus.com/pages/publications/85147526721

U2 - 10.2174/0929867328666211111161811

DO - 10.2174/0929867328666211111161811

M3 - Review article

C2 - 34766883

AN - SCOPUS:85147526721

SN - 0929-8673

VL - 30

SP - 1529

EP - 1567

JO - Current Medicinal Chemistry

JF - Current Medicinal Chemistry

IS - 13

ER -

Recent Trends in Rationally Designed Molecules as Kinase Inhibitors

Abstract

UN SDGs

Keywords

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