Role of PARP and TRPM2 in VEGF Inhibitor‐Induced Vascular Dysfunction

Neves, Karla B; Alves-Lopes, Rhéure; Montezano, Augusto C; Touyz, Rhian M.

doi:10.1161/jaha.122.027769

Cited by 5 publications

(1 citation statement)

References 37 publications

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“…63 In contrast to niraparib, olaparib exhibits a low risk of hypertension than placebo and was mainly driven by PAOLA-1 RCT who assessed monoclonal antibody bevacizumab (a vascular endothelial growth factor A inhibitor, VEGF-Ai) in combination with olaparib or placebo in patients with EOC. To elucidate this observation, Neves et al 64 studied the druginduced vascular dysfunction in human vascular smooth muscle cells and aortic endothelial cells as well as in wild-type mouse mesenteric arteries. To mimic vascular dysfunction, cells and arteries were exposed to axitinib, a VEGF inhibitor, alone or in combination with olaparib.…”

Section: Discussionmentioning

confidence: 99%

Arterial hypertension associated with PARPi: A meta‐analysis of 41 placebo randomized controlled trials combined with a World Health Organization's pharmacovigilance study

Blaize,

Surtouque,

Font

et al. 2024

Fundamemntal Clinical Pharma

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BackgroundArterial hypertension has been recently reported from randomized controlled trials (RCTs) assessing poly (ADP‐ribose) polymerase inhibitor (PARPi).ObjectiveIn a context of increasing use of PARPi, it is crucial to properly assess risk and incidence of this adverse event for clinical practice.MethodsWe performed a systematic review and meta‐analysis in MEDLINE, Cochrane CENTRAL and ClinicalTrials.gov up to January 4, 2023 with an ongoing surveillance up to June 7, 2023. RCTs comparing PARPi to placebo in adult patients with solid tumors were included if hypertension was reported. The primary outcome was the summary risk ratio (RR, with 95% CIs) of any hypertension of PARPi class in placebo RCTs. Secondary outcomes were the summary risk and incidence of hypertension of each individual PARPi. To provide clinical features of PARPi‐associated hypertension, we independently queried the WHO's pharmacovigilance database, up to September 1, 2022.ResultsIn total, 41 placebo RCTs (n = 15 264 adult patients) were included. PARPi class was not associated with an increased risk of hypertension compared with placebo. In individual analyses, the risk of hypertension was lower with olaparib than placebo (RR 0.77 [95% CI: 0.68–0.86], P < 0.01; I2 = 19%, χ2 P = 0.26). Niraparib monotherapy increased the risk of any (RR 2.84 [95% CI: 1.76–4.57], P < 0.01; I2 = 66%, χ2 P = 0.01) hypertension with a summary incidence of 19.87% (95% CI: 15.23–25.50). In real‐life setting, niraparib‐associated hypertension occurs within 20 days and was serious in 66%. Co‐prescription of at least one antihypertensive or therapy‐induced hypertension was reported in 20.5% or 14.4% of cases, respectively.ConclusionsIn a context of extensive assessment of niraparib in combination, these data reinforce the need of a close monitoring of this adverse event to preserve its clinical benefit on patients' survival.

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Section: Discussionmentioning

confidence: 99%