Discover @ Loyola University Chicago Health Sciences Division - Utility of the ACE Inhibitor Captopril in Mitigating Radiation-associated Pulmonary Toxicity in Lung Cancer: Results From NRG Oncology RTOG 0123.

Utility of the ACE Inhibitor Captopril in Mitigating Radiation-associated Pulmonary Toxicity in Lung Cancer: Results From NRG Oncology RTOG 0123. Journal Article

Local Library Link: Find It @ Loyola

Authors:	Small, W; James, JL; Moore, TD; Fintel, DJ; Lutz, ST; Movsas, B; Suntharalingam, M; Garces, YI; Ivker, R; Moulder, J; Pugh, S; Berk, LB
Article Title:	Utility of the ACE Inhibitor Captopril in Mitigating Radiation-associated Pulmonary Toxicity in Lung Cancer: Results From NRG Oncology RTOG 0123.
Abstract:	OBJECTIVES: The primary objective of NRG Oncology Radiation Therapy Oncology Group 0123 was to test the ability of the angiotensin-converting enzyme inhibitor captopril to alter the incidence of pulmonary damage after radiation therapy for lung cancer; secondary objectives included analyzing pulmonary cytokine expression, quality of life, and the long-term effects of captopril. MATERIALS AND METHODS: Eligible patients included stage II-IIIB non-small cell lung cancer, stage I central non-small cell lung cancer, or limited-stage small cell. Patients who met eligibility for randomization at the end of radiotherapy received either captopril or standard care for 1 year. The captopril was to be escalated to 50 mg three times a day. Primary endpoint was incidence of grade 2+ radiation-induced pulmonary toxicity in the first year. RESULTS: Eighty-one patients were accrued between June 2003 and August 2007. Given the low accrual rate, the study was closed early. No significant safety issues were encountered. Eight patients were ineligible for registration or withdrew consent before randomization and 40 patients were not randomized postradiation. Major reasons for nonrandomization included patients' refusal and physician preference. Of the 33 randomized patients, 20 were analyzable (13 observation, 7 captopril). The incidence of grade 2+ pulmonary toxicity attributable to radiation therapy was 23% (3/13) in the observation arm and 14% (1/7) in the captopril arm. CONCLUSIONS: Despite significant resources and multiple amendments, NRG Oncology Radiation Therapy Oncology Group 0123 was unable to test the hypothesis that captopril mitigates radiation-induced pulmonary toxicity. It did show the safety of such an approach and the use of newer angiotensin-converting enzyme inhibitors started during radiotherapy may solve the accrual problems.
Journal Title:	American journal of clinical oncology
ISSN:	1537-453X; 0277-3732
Publisher:	Unknown
Date Published:	2018

LUC Authors

181 Small

Related LUC Article

Decreased Risk Of Radiation Pneumonitis With Coincident Concurrent Use Of Angiotensin Converting Enzyme Inhibitors In Patients Receiving Lung Stereotactic Body Radiation Therapy

American journal of clinical oncology 2016
Treatment Of Life Threatening Ace Inhibitor Induced Angioedema.

Advanced emergency nursing journal
A Review Of Concurrent Chemo/Radiation, Immunotherapy, Radiation Planning, And Biomarkers For Locally Advanced Non Small Cell Lung Cancer And Their Role In The Development Of Ecog Acrin Ea5181.

Clinical lung cancer 2022
Quality Of Life Analysis Of A Radiation Dose Escalation Study Of Patients With Non Small Cell Lung Cancer: A Secondary Analysis Of The Radiation Therapy Oncology Group 0617 Randomized Clinical Trial.

JAMA oncology 2016
Rtog 9804: A Prospective Randomized Trial For Good Risk Ductal Carcinoma In Situ Comparing Radiotherapy With Observation.

Journal of Clinical Oncology 2015