Growth hormone and targeted oncological agents: Are we stopping children with brain tumours from reaching their true height potential?

Abstract

Children with low-grade gliomas have excellent long-term survival outcomes. The development of therapies targeted to the driver mutations along the Mitogen Activated Protein (MAP) kinase signalling pathway are providing long-term stability for many patients with these tumours. Given the frequency of these tumours residing within or near the suprasellar region, our patients commonly suffer from hormone deficiencies. In Australia, the Pharmaceutical Benefits Scheme currently restricts growth hormone therapy to patients who are not being actively treated for cancer, including those receiving targeted therapies. This viewpoint hopes to facilitate an important discussion amongst our colleagues as to whether this should be changed to allow growth hormone to become available to children on chronic tumour suppressive therapy.

Related Papers

• → The 5′-Deiodinases Are Not Essential for the Fasting-Induced Decrease in Circulating Thyroid Hormone Levels in Male Mice: Possible Roles for the Type 3 Deiodinase and Tissue Sequestration of Hormone(2014)31 cited
• → The interrelationships of thyroid and growth hormones: effect of growth hormone releasing hormone in hypo- and hyperthyroid male rats(1986)25 cited
• → Changes in plasma thyroid hormones following administration of exogenous pituitary hormones and steroid hormones to rainbow trout (Salmo gairdneri)(1980)63 cited
• → Developmental changes of plasma inhibin, gonadotropins, steroid hormones, and thyroid hormones in male and female Shao ducks(2005)19 cited
• → Epidermal Growth Factor: Effect on Circulating Thyroid Hormone Levels in Sheep*(1986)30 cited