The Effects of 2′- <i>O</i> -Methoxyethyl Oligonucleotides on Renal Function in Humans

Stanley T. Crooke(Ionis Pharmaceuticals (United States)), Brenda F. Baker(Ionis Pharmaceuticals (United States)), Nguyen C. Pham(Ionis Pharmaceuticals (United States)), Steven G. Hughes(Ionis Pharmaceuticals (United States)), T. Jesse Kwoh(Ionis Pharmaceuticals (United States)), Danlin Cai(Ionis Pharmaceuticals (United States)), Sotirios Tsimikas(Ionis Pharmaceuticals (United States)), Richard S. Geary(Ionis Pharmaceuticals (United States)), Sanjay Bhanot(Ionis Pharmaceuticals (United States))
Nucleic Acid Therapeutics
November 29, 2017
Cited by 67Open Access
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Abstract

Systemically administered 2'-O-methoxyethyl (2'MOE) antisense oligonucleotides (ASOs) accumulate in the kidney and metabolites are cleared in urine. The effects of eleven 2'MOE ASOs on renal function were assessed in 2,435 patients from 32 phase 2 and phase 3 trials. The principle analysis was on data from 28 randomized placebo-controlled trials. Mean levels of renal parameters remained within normal ranges over time across dose groups. Patient-level meta-analyses demonstrated a significant difference between placebo-treated and 2'MOE ASO-treated patients at doses >175 mg/week in the percentage and absolute change from baseline for serum creatinine and estimated glomerular filtration rate. However, these changes were not clinically significant or progressive. No dose-related effects were observed in the incidence of abnormal renal test results in the total population of patients, or subpopulation of diabetic patients or patients with renal dysfunction at baseline. The incidence of acute kidney injury [serum creatinine ≥0.3 mg/dL (26.5 μM) increases from baseline or ≥1.5 × baseline] in 2'MOE ASO-treated patients (2.4%) was not statistically different from placebo (1.7%, P = 0.411). In conclusion, in this database, encompassing 32 clinical trials and 11 different 2'MOE ASOs, we found no evidence of clinically significant renal dysfunction up to 52 weeks of randomized-controlled treatment.


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