Cardiovasculaire bijwerkingen van doelgerichte behandelingen, deel II*

Bronnen:

1. Maurea N, Coppola C, Piscopo G et al. Pathophysiology of cardiotoxicity from target therapy and angiogenesis inhibitors. Cardiovasc Med. 2016;17 (suppl 1):e19-e26,Rupert CE, and Coulombe KLK. The Roles of Neuregulin-1 in Cardiac Development, Homeostasis, and Disease. Biomarker Insights. 2015:10(S1) 1-9. ,Sandoo A, Kitas GD, Carmichael AR. Breast cancer therapy and cardiovascular risk: focus on trastuzumab Vascular Health and Risk Management. 2015;11:223-8.,Herrmann J, Eric H. Yang EH Iliescu C, et al. Vascular Toxicities of Cancer Therapies: The Old and The New – An Evolving Avenue. Circulation. 2016;133: 1272-89.,LI W, Croce K, Steensma DP, et al. Vascular and metabolic implications of novel targeted cancer therapies: focus on kinase inhibitors. J Am Coll Cardiol 2015;66:1160-78.,Lankhorst S, Saleh L, Danser AJ, et al. Ethiology of angiogenesis inhibition-related hypertension. Curr Opin Pharmacol. 2015;21:7-13.,Grandin EW, Ky B, Cornell RF, et al. Patterns of Cardiac Toxicity Associated With Irreversible Proteasome Inhibition in the Treatment of Multiple Myeloma. J Cardiac Fail. 2015;21:138-44.,McMullen JR, Boey EJH, Ooy JYY, et al. Ibrutinib increases the risk of atrial fibrillation, potentially through inhibition of cardiac PI3K-Akt signaling. Blood. 2014;124: 3829-30.,Moslehi JJ. Cardiovascular toxic effects of targeted cancer therapies. N Engl J Med. 2016;375:1457-67.,Escalante CP, Chang YC, Liao K, et al. Meta-analysis of cardiovascular toxicity risks in cancer patients on selected targeted agents. Support Care Cancer. 2016;24:4057-74.,Aghel N, Delgado DH, Lipton JH. Cardiovascular toxicities of BCR-ABL tyrosine kinase inhibitors in chronic myeloid leukemia: preventive strategies and cardiovascular surveillance. Vasc Health Risk Manag. 2017;13:293-303.,Murakami N, Riella LV, Funakoshi T. Risk of Metabolic Complications in Kidney Transplantation After Conversion to mTOR Inhibitor: A Systematic Review and Meta‐Analysis. Am J Transplantation. 2014;14:2317-27. ,Glass CK, Mitchell RN. Winning the battle, but losing the war: mechanisms and morphology of cancer-therapy-associated cardiovascular toxicity. Cardiovasc Pathol. 2017;30:55-63.,Krönke J, Udeshi N, Narla A, et al. Lenalidomide causes selective degradation of IKZF1 and IKZF3 in multiple myeloma cells. Science. 2014:343:301-5.,Giuliani M, Janji B, Berchem G. Activation of NK cells and disruption of PD-L1/PD-1 axis: two different ways for lenalidomide to block myeloma progression. Oncotarget. 2017;8:24031-44.,Holstein SA, McCarthy PL. Immunomodulatory Drugs in Multiple Myeloma: mechanisms of Action and Clinical Experience. Drugs. 2017;77:505-20.,Postow MA, Sidlow R, Hellmann MD. Immune-related adverse events associated with immune checkpoint blockade. N Engl J Med. 2018;378:158-68.,Maurea N, Spallarossa P, Cadeddu C, et al. A recommended practical approach to the management of target therapy and angiogenesis inhibitors cardiotoxicity: an opinion paper of the working group on drug cardiotoxicity and cardioprotection, Italian Society of Cardiology. J Cardiovasc Med. 2016;17 (suppl 1):e93-e104.,Maas AHEM, Ottevanger N, Atsma F, et al. Cardiovascular surveillance in breast cancer treatment: A more individualized approach is needed. Maturitas. 2016; 89:58-62.