scholarly journals New Therapeutic Targets for Hepatic Fibrosis in the Integrin Family, α8β1 and α11β1, Induced Specifically on Activated Stellate Cells

2021 ◽  
Author(s):  
Yasuyuki Yokosaki ◽  
Norohisa Nishimichi
Keyword(s):  
Clinical Trial ◽  
Stellate Cells ◽  
Ligand Specificity ◽  
Central Target ◽  
The Road ◽  
Rgd Sequence ◽  
Cell Matrix ◽  
Cell Type Specific ◽  
Disease Specificity ◽  
Integrin Family

Huge effort has been devoted to developing drugs targeting integrins over 30 years, because of the primary roles of integrins in the cell-matrix milieu. Five αv-containing integrins, in the 24 family members, have been a central target of fibrosis. Currently, a small molecule against αvβ1 is undergoing a clinical trial for NASH-associated fibrosis as a rare reagent aiming at fibrogenesis. Latent TGFβ activation, a distinct talent of αv-integrins, has been intriguing as therapeutic target. None of the αv-integrin inhibitors, however, has been in the clinical market. αv-integrins commonly recognize an Arg-Gly-Asp (RGD) sequence, and thus the pharmacophore of inhibitors for the 5-integrins is based on the same RGD structure. The RGD preference of the integrins, at the same time, dilutes ligand specificity, as the 5-integrins share ligands containing RGD sequence such as fibronectin. With the inherent little specificity in both drugs and targets, “disease specificity” has become less important for the inhibitors than blocking as many αv-integrins. In fact, an almighty inhibitor for αv-integrins, pan-αv, was in a clinical trial. On the contrary, approved integrin inhibitors are all specific to target integrins, which are expressed in cell-type specific manner: αIIbβ3 on platelets, α4β1, α4β7 and αLβ2 on leukocytes. Herein, “disease specific” integrins would serve as attractive targets. α8β1 and α11β1 are selectively expressed in hepatic stellate cells (HSCs) and distinctively induced upon culture activation. The exceptional specificity to activated HSCs reflects rather “pathology specific” nature of these new integrins. The monoclonal antibodies against α8β1 and α11β1 in preclinical examinations may illuminate the road to the first medical reagents.

scholarly journals New Therapeutic Targets for Hepatic Fibrosis in the Integrin Family, α8β1 and α11β1, Induced Specifically on Activated Stellate Cells

2021 ◽  
Vol 22 (23) ◽  
pp. 12794
Author(s):  
Yasuyuki Yokosaki ◽  
Norihisa Nishimichi
Keyword(s):  
Clinical Trial ◽  
Stellate Cells ◽  
Ligand Specificity ◽  
Central Target ◽  
The Road ◽  
Rgd Sequence ◽  
Cell Matrix ◽  
A Cell ◽  
Cell Type Specific ◽  
Integrin Family

A huge effort has been devoted to developing drugs targeting integrins over 30 years, because of the primary roles of integrins in the cell-matrix milieu. Five αv-containing integrins, in the 24 family members, have been a central target of fibrosis. Currently, a small molecule against αvβ1 is undergoing a clinical trial for NASH-associated fibrosis as a rare agent aiming at fibrogenesis. Latent TGFβ activation, a distinct talent of αv-integrins, has been intriguing as a therapeutic target. None of the αv-integrin inhibitors, however, has been in the clinical market. αv-integrins commonly recognize an Arg-Gly-Asp (RGD) sequence, and thus the pharmacophore of inhibitors for the 5-integrins is based on the same RGD structure. The RGD preference of the integrins, at the same time, dilutes ligand specificity, as the 5-integrins share ligands containing RGD sequence such as fibronectin. With the inherent little specificity in both drugs and targets, “disease specificity” has become less important for the inhibitors than blocking as many αv-integrins. In fact, an almighty inhibitor for αv-integrins, pan-αv, was in a clinical trial. On the contrary, approved integrin inhibitors are all specific to target integrins, which are expressed in a cell-type specific manner: αIIbβ3 on platelets, α4β1, α4β7 and αLβ2 on leukocytes. Herein, “disease specific” integrins would serve as attractive targets. α8β1 and α11β1 are selectively expressed in hepatic stellate cells (HSCs) and distinctively induced upon culture activation. The exceptional specificity to activated HSCs reflects a rather “pathology specific” nature of these new integrins. The monoclonal antibodies against α8β1 and α11β1 in preclinical examinations may illuminate the road to the first medical agents.

Bumps and bridges on the road to responsible sharing of clinical trial data

2014 ◽  
Vol 11 (1) ◽  
pp. 7-12 ◽  
Author(s):  
Jesse A Berlin ◽  
Sandra Morris ◽  
Frank Rockhold ◽  
Lisa Askie ◽  
Davina Ghersi ◽  
...  
Keyword(s):  
Clinical Trial ◽  
Clinical Trial Data ◽  
Trial Data ◽  
The Road ◽  
On The Road

scholarly journals Fibronectin receptors of phagocytes. Characterization of the Arg-Gly-Asp binding proteins of human monocytes and polymorphonuclear leukocytes.

1988 ◽  
Vol 167 (3) ◽  
pp. 777-793 ◽  
Author(s):  
E J Brown ◽  
J L Goodwin
Keyword(s):  
Surface Molecule ◽  
Human Monocytes ◽  
Ligand Specificity ◽  
Cell Binding ◽  
Antigenic Analysis ◽  
Vitronectin Receptor ◽  
Surface Molecules ◽  
Rgd Sequence ◽  
Single Receptor

We have defined the cell surface molecules of human monocytes and PMN that bind to the chymotryptic cell binding domain of Fn and to a synthetic peptide, KYAVTGRGDS, based on the sequence of Fn, by affinity chromatography. Monocytes express two receptors that differ in their affinity for CBD-Sepharose and peptide-Sepharose, but that both recognize the RGD sequence. Only a single receptor is purified from PMN, which resembles the monocyte surface molecule that binds to peptide-Sepharose. These receptors are not part of the Mac-1, LFA-1, p(150,95) family, but do have homology to the platelet Fn receptor, gpIIb/IIIa. Interestingly, the antigenic crossreactivity between gpIIb/IIIa and the phagocyte receptors purified on peptide-Sepharose is largely in the beta chain of the receptors. The alpha chains appear to be distinct, based on molecular weight, antigenic analysis, and ligand specificity. This receptor also seems to be the surface molecule on monocytes that is critical for phagocytosis enhancement by Fn. Thus, we have defined the phagocyte Fn receptor that transduces the signal for increased phagocytosis by monocytes; it may be a third member of a family of adhesion molecules that includes the gpIIb/IIIa of platelets and the vitronectin receptor of fibroblasts.

Clinical trial end points: On the road to nowhere?

Neurology ◽  
2002 ◽  
Vol 58 (5) ◽  
pp. 679-686 ◽  
Author(s):  
R. G. Holloway ◽  
A. W. Dick
Keyword(s):  
Clinical Trial ◽  
End Points ◽  
The Road ◽  
On The Road

scholarly journals Activation of the alpha 4 beta 1 integrin through the beta 1 subunit induces recognition of the RGDS sequence in fibronectin.

1994 ◽  
Vol 126 (1) ◽  
pp. 271-279 ◽  
Author(s):  
P Sánchez-Aparicio ◽  
C Dominguez-Jiménez ◽  
A Garcia-Pardo
Keyword(s):  
Cell Adhesion ◽  
B Cell ◽  
High Avidity ◽  
Ligand Specificity ◽  
Lymphocyte Migration ◽  
Rgd Peptides ◽  
Constitutive Function ◽  
Rgd Sequence ◽  
Beta 1 Integrin ◽  
And Function

Lymphocyte attachment to fibronectin is mainly mediated by the interaction of alpha 5 beta 1 and alpha 4 beta 1 integrins with the RGD and CS-1/Hep II sites, respectively. We have recently shown that the anti-beta 1 mAb TS2/16 can convert the partly active alpha 4 beta 1 present on certain hemopoietic cells that recognizes CS-1 but not Hep II, to a high avidity form that binds both ligands. In this report we have studied whether mAb TS2/16 also affects alpha 4 beta 1 ligand specificity. Incubation of the B cell lines Ramos and Daudi (which lack alpha 5 beta 1) with mAb TS2/16 induced specific attachment to an 80-kD fragment which lacks CS-1 and Hep II and contains the RGD sequence. mAbs anti-alpha 4 and the synthetic peptides CS-1 and IDAPS inhibited adhesion to the 80-kD fragment thus implying alpha 4 beta 1 as the receptor for this fragment. Interestingly, the synthetic peptide GRGDSPC and a 15-kD peptic fibronectin fragment containing the RGD sequence also inhibited B cell adhesion to the 80-kD fragment. Because we have previously shown that RGD peptides do not affect the constitutive function of alpha 4 beta 1, we tested whether TS2/16-activated alpha 4 beta 1 acquired the capacity to recognize RGD. Indeed RGD peptides inhibited TS2/16-treated B cell adhesion to a 38-kD fragment containing CS-1 and Hep II but did not affect binding of untreated cells to this fragment. An anti-fibronectin mAb reactive with an epitope on or near the RGD sequence also efficiently inhibited cell adhesion to the 80-kD fragment, indicating that the RGD sequence is a novel adhesive ligand for activated alpha 4 beta 1. These results emphasize the role of alpha 4 beta 1 as a receptor with different ligand specificities according to the activation state, a fact that may be important for lymphocyte migration, localization, and function.

scholarly journals Regulation and dynamics of force transmission at individual cell-matrix adhesion bonds

2019 ◽  
Author(s):  
Steven J. Tan ◽  
Alice C. Chang ◽  
Cayla M. Miller ◽  
Sarah M. Anderson ◽  
Louis S. Prahl ◽  
...  
Keyword(s):  
Biological Function ◽  
Molecular Level ◽  
Individual Cell ◽  
Ligand Specificity ◽  
Force Transmission ◽  
Animal Tissues ◽  
Cell Matrix ◽  
Mechanical Homeostasis ◽  
Cell Matrix Adhesion ◽  
Adhesion Complex

AbstractIntegrin-based adhesion complexes link the cytoskeleton to the extracellular matrix (ECM) and are central to the construction of multicellular animal tissues. How biological function emerges from the 10s-1000s of proteins present within a single adhesion complex has remained unclear. We used fluorescent molecular tension sensors to visualize force transmission by individual integrins in living cells. These measurements revealed an underlying functional modularity in which integrin class controlled adhesion size and ECM ligand specificity, while the number and type of connections between integrins and F-actin determined the force per individual integrin. In addition, we found that most integrins existed in a state of near-mechanical equilibrium, a result not predicted by existing models of cytoskeletal force transduction. A revised model that includes reversible crosslinks within the F-actin network accounts for this result, and suggests how cellular mechanical homeostasis can arise at the molecular level.

scholarly journals Desktop software to identify patients eligible for recruitment into a clinical trial: using SARMA to recruit to the ROAD feasibility trial

2010 ◽  
Vol 18 (1) ◽  
pp. 51-58 ◽  
Author(s):  
Shaun Treweek ◽  
Ewan Pearson ◽  
Natalie Smith ◽  
Ron Neville ◽  
Paul Sargeant ◽  
...  
Keyword(s):  
Clinical Trial ◽  
Feasibility Trial ◽  
The Road
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