5-Azacytidine inhaled dry powder formulation profoundly improves pharmacokinetics and efficacy for lung cancer therapy through genome reprogramming

医学 药代动力学 肺癌 药理学 吸入 干粉吸入器 病理 内科学 麻醉 哮喘 吸入器
作者
Philip J. Kuehl,Carmen S. Tellez,Marcie J. Grimes,Thomas H. March,Mathewos Tessema,David Revelli,Larry M. Mallis,Wendy W. Dye,Tyler Sniegowski,Aaron Badenoch,Michael Burke,Devon Dubose,D. Vodak,Maria A. Picchi,Steven A. Belinsky
出处
期刊:British Journal of Cancer [Springer Nature]
卷期号:122 (8): 1194-1204 被引量:19
标识
DOI:10.1038/s41416-020-0765-2
摘要

Abstract Background Epigenetic therapy through demethylation of 5-methylcytosine has been largely ineffective in treating lung cancer, most likely due to poor tissue distribution with oral or subcutaneous delivery of drugs such as 5-azacytidine (5AZA). An inhalable, stable dry powder formulation of 5AZA was developed. Methods Pharmacokinetics of inhaled dry powder and aqueous formulations of 5AZA were compared to an injected formulation. Efficacy studies and effect of therapy on the epigenome were conducted in an orthotopic rat lung cancer model for inhaled formulations. Results Inhaled dry powder 5AZA showed superior pharmacokinetic properties in lung, liver, brain and blood compared to the injected formulation and for all tissues except lung compared to an inhaled aqueous formulation. Only dry powder 5AZA was detected in brain (~4-h half-life). Inhaled dry powder was superior to inhaled aqueous 5AZA in reducing tumour burden 70–95%. Superiority of inhaled 5AZA dry powder was linked to effectively reprogramming the cancer genome through demethylation and gene expression changes in cancer signalling and immune pathways. Conclusions These findings could lead to widespread use of this drug as the first inhaled dry powder therapeutic for treating local and metastatic lung cancer, for adjuvant therapy, and in combination with immunotherapy to improve patient survival.
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