Cardiotoxicity and myocardial hypoperfusion associated with anti‐vascular endothelial growth factor therapies: prospective cardiac magnetic resonance imaging in patients with cancer

myocardial blood flow at rest and ( E ) stress, and ( F ) vascular permeability at rest with 4–6weeks of vascular endothelial growth factor signalling pathway inhibitor therapy.

By interrupting tumour angiogenesis, vascular endothelial growth factor signalling pathway inhibitors (VSPIs) represent a major advance in the treatment of a wide variety of cancers. 1 However, their oncological benefits have been accompanied by considerable cardiovascular toxicity, including hypertension, left ventricular systolic dysfunction (LVSD) and heart failure. 2 These may be severe and can limit the dose and duration of anti-cancer treatment.
The timing, frequency, and pathophysiological basis of VSPI-associated myocardial toxicity is incompletely defined. In addition to the detrimental effect of an abrupt rise in left ventricular afterload as a result of VSPI-associated hypertension, inhibition of vascular endothelial growth factor may have direct myocardial toxic effects. This may be the consequence of inhibition of tyrosine kinases required both for tumour growth and normal cardiac function. Furthermore, VSPIs are associated with peripheral microvascular rarefaction 3 and it remains unclear whether myocardial micro-arterial constriction or vessel loss is implicated in the pathogenesis of VSPI-associated LVSD. The only prior study to evaluate prospectively the effects of VSPIs upon cardiac function used echocardiography and demonstrated a 9.7% incidence of cardiotoxicity, defined as ≥10% reduction in left ventricular ejection fraction (LVEF) to a value less than 50%. 4 There are inherent limitations of echocardiography for the reproducible detection of changes in myocardial function and it does not allow assessment of myocardial perfusion, vascular permeability, or myocardial tissue characterisation. We therefore used multi-parametric cardiac magnetic resonance imaging, including adenosine stress-perfusion to measure myocardial blood flow and vascular permeability in patients before and during VSPI treatment. 5 All patients over the age of 18 years at the Beatson West of Scotland Cancer Centre in Glasgow, Scotland, who were planned to commence VSPI therapy were considered for participation. Enrolment took place between December 2018 and March 2019. Exclusion criteria included an estimated glomerular filtration rate < 30 mL/min/1.73 m 2 of body surface area, persistent or permanent atrial fibrillation, second-or third-degree atrioventricular block, and a history of allergy to adenosine or gadolinium contrast.
Patients underwent stress-perfusion cardiac magnetic resonance imaging (3.0T Siemens MAGNETOM Prisma; Siemens Healthcare, Erlangen, Germany) at baseline and after 4 to 6 weeks of treatment. Biventricular mass and function, myocardial feature-tracking strain, and tissue characterisation by T1 mapping and perfusion imaging were assessed. Myocardial T1 mapping measures the myocardial longitudinal magnetic relaxation time (also known as spin-lattice relaxation time) of different molecules found within the myocardium. Intravenous adenosine infusion was used to induce hyperaemia to simulate myocardial stress.
In this hypothesis-generating study, VSPI therapy was associated with a reduction in LVEF and it is possible that the incidence of a more substantial drop in LVEF decline may be greater than previously appreciated. Although systemic hypertension may contribute to these phenomena, alterations in myocardial tissue characteristics, including reduced T1 relaxation time, may reflect direct myocardial toxic effects. The observed rise in vascular permeability supports a role for microvascular endothelial dysfunction in the development of VSPI-associated LVSD. Furthermore, reduced resting myocardial blood flow is consistent with VSPI-induced microvascular constriction and consequent myocardial hypoperfusion. The normalisation of myocardial blood flow with adenosineinduced stress suggests that VSPI-induced microvascular vasoconstriction may be reversible and that vasodilator agents might be a potential strategy to prevent or treat the early cardiotoxic effects of VSPI. It remains to be established whether such microvascular changes remain reversible in patients exposed to VSPI therapies and indeed, whether any of the potential cardiotoxic effects or injury sustained or progressed in the longer term.
Further prospective evaluation of larger groups of patients is necessary to provide robust data relating to the incidence and pathophysiology of VSPI-induced cardiotoxicity. This is required urgently to allow balanced decision-making before prescribing these effective anti-cancer therapies whilst minimising cardiovascular risk. Optimised cardiovascular surveillance strategies and mechanistically-targeted strategies to reduce VSPI-induced cardiovascular toxicity are both overdue.