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Emerging therapeutic opportunities for integrin inhibitors
by
Jenkins, R G
, Roper, J A
, Macdonald S J F
, Slack, R J
, Hatley R J D
in
Antibodies
/ Binding sites
/ Cancer therapies
/ Clinical trials
/ Drugs
/ Eye diseases
/ Gene expression
/ Glycoproteins
/ Inflammatory bowel disease
/ Ligands
/ Multiple sclerosis
/ Peptides
/ Proteins
/ Pulmonary fibrosis
2022
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Emerging therapeutic opportunities for integrin inhibitors
by
Jenkins, R G
, Roper, J A
, Macdonald S J F
, Slack, R J
, Hatley R J D
in
Antibodies
/ Binding sites
/ Cancer therapies
/ Clinical trials
/ Drugs
/ Eye diseases
/ Gene expression
/ Glycoproteins
/ Inflammatory bowel disease
/ Ligands
/ Multiple sclerosis
/ Peptides
/ Proteins
/ Pulmonary fibrosis
2022
Oops! Something went wrong.
While trying to remove the title from your shelf something went wrong :( Kindly try again later!
Do you wish to request the book?
Emerging therapeutic opportunities for integrin inhibitors
by
Jenkins, R G
, Roper, J A
, Macdonald S J F
, Slack, R J
, Hatley R J D
in
Antibodies
/ Binding sites
/ Cancer therapies
/ Clinical trials
/ Drugs
/ Eye diseases
/ Gene expression
/ Glycoproteins
/ Inflammatory bowel disease
/ Ligands
/ Multiple sclerosis
/ Peptides
/ Proteins
/ Pulmonary fibrosis
2022
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Emerging therapeutic opportunities for integrin inhibitors
Journal Article
Emerging therapeutic opportunities for integrin inhibitors
2022
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Overview
Integrins are cell adhesion and signalling proteins crucial to a wide range of biological functions. Effective marketed treatments have successfully targeted integrins αIIbβ3, α4β7/α4β1 and αLβ2 for cardiovascular diseases, inflammatory bowel disease/multiple sclerosis and dry eye disease, respectively. Yet, clinical development of others, notably within the RGD-binding subfamily of αv integrins, including αvβ3, have faced significant challenges in the fields of cancer, ophthalmology and osteoporosis. New inhibitors of the related integrins αvβ6 and αvβ1 have recently come to the fore and are being investigated clinically for the treatment of fibrotic diseases, including idiopathic pulmonary fibrosis and nonalcoholic steatohepatitis. The design of integrin drugs may now be at a turning point, with opportunities to learn from previous clinical trials, to explore new modalities and to incorporate new findings in pharmacological and structural biology. This Review intertwines research from biological, clinical and medicinal chemistry disciplines to discuss historical and current RGD-binding integrin drug discovery, with an emphasis on small-molecule inhibitors of the αv integrins.Integrins are key signalling molecules that are present on the surface of subsets of cells and are therefore good potential therapeutic targets. In this Review, Hatley and colleagues discuss the development of integrin inhibitors, particularly the challenges in developing inhibitors for integrins that contain an αv-subunit, and suggest how these challenges could be addressed.
Publisher
Nature Publishing Group
Subject
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