2015
DOI: 10.1002/prp2.175
|View full text |Cite
|
Sign up to set email alerts
|

In vitro pharmacological profiling of R406 identifies molecular targets underlying the clinical effects of fostamatinib

Abstract: Off-target pharmacology may contribute to both adverse and beneficial effects of a new drug. In vitro pharmacological profiling is often applied early in drug discovery; there are fewer reports addressing the relevance of broad profiles to clinical adverse effects. Here, we have characterized the pharmacological profile of the active metabolite of fostamatinib, R406, linking an understanding of drug selectivity to the increase in blood pressure observed in clinical studies. R406 was profiled in a broad range o… Show more

Help me understand this report

Search citation statements

Order By: Relevance

Paper Sections

Select...
4
1

Citation Types

3
73
1

Year Published

2016
2016
2024
2024

Publication Types

Select...
6
1

Relationship

0
7

Authors

Journals

citations
Cited by 87 publications
(77 citation statements)
references
References 45 publications
3
73
1
Order By: Relevance
“…Off-target inhibition of VEGFR2 was found to increase vascular resistance and reduced VEGF-induced nitric oxide release in animal models [50], where effects were dose-dependent, but effectively managed by drug withdrawal or concomitant treatment with antihypertensive agents [51]. R406 also inhibited VEGF-dependent human endothelial cell tube formation and tube outgrowth, further supporting a possible role for VEGF signaling in blood pressure effects of fostamatinib [48].…”
Section: Spleen Tyrosine Kinase Inhibitionmentioning
confidence: 91%
See 3 more Smart Citations
“…Off-target inhibition of VEGFR2 was found to increase vascular resistance and reduced VEGF-induced nitric oxide release in animal models [50], where effects were dose-dependent, but effectively managed by drug withdrawal or concomitant treatment with antihypertensive agents [51]. R406 also inhibited VEGF-dependent human endothelial cell tube formation and tube outgrowth, further supporting a possible role for VEGF signaling in blood pressure effects of fostamatinib [48].…”
Section: Spleen Tyrosine Kinase Inhibitionmentioning
confidence: 91%
“…R406 is a potent and selective inhibitor of Syk; it inhibits Syk kinase activity by binding the catalytic domain (K i = 30 nM) and acts as an ATP-competitive inhibitor (IC 50 = 41 nM) [37]. As with other kinase inhibitors, additional molecular targets of fostamatinib have been explored to investigate potential off-target effects that may contribute to its pharmacological effects [47,48]. Selectivity of R406 has been demonstrated in panels of in vitro and cell-based assays.…”
Section: Spleen Tyrosine Kinase Inhibitionmentioning
confidence: 99%
See 2 more Smart Citations
“…The significance of this change is unknown, as ovarian follicles, unlike corpora lutea, are avascular and therefore not expected to be affected by angiogenic inhibition. R406 also has significant off-target inhibitor activity for the VEGF and FGF family of receptors, with in vitro isolated enzyme IC 50 values similar to the SYK potency (IC 50 4-60 nM; Rolf et al 2015). In vivo potency, however, is likely to be much lower since elevation of blood pressure (a recognized biomarker of VEGFR activity [Curwen et al 2008]) is much less compared to other more potent VEGFR inhibitors (fostamatinib < 5 mmHg vs. 25 mmHg for sunitinb; Rolf et al 2015).…”
Section: Discussionmentioning
confidence: 97%