Journal of Clinical Medicine (Jun 2019)

Safety Evaluation of Tadalafil Treatment for Fetuses with Early-Onset Growth Restriction (TADAFER): Results from the Phase II Trial

  • Shintaro Maki,
  • Hiroaki Tanaka,
  • Makoto Tsuji,
  • Fumi Furuhashi,
  • Shoichi Magawa,
  • Michiko K. Kaneda,
  • Masafumi Nii,
  • Kayo Tanaka,
  • Eiji Kondo,
  • Satoshi Tamaru,
  • Toru Ogura,
  • Yuki Nishimura,
  • Masayuki Endoh,
  • Tadashi Kimura,
  • Tomomi Kotani,
  • Akihiko Sekizawa,
  • Tomoaki Ikeda

DOI
https://doi.org/10.3390/jcm8060856
Journal volume & issue
Vol. 8, no. 6
p. 856

Abstract

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Tadalafil is a phosphodiesterase 5 (PDE5) inhibitor with a long half-life, high selectivity, and rapid onset of action. Because the safety of using PDE5 inhibitors as therapeutic agents for fetal growth restriction (FGR) has been a problem worldwide, this paper primarily focuses on the safety assessments performed in the Tadalafil Treatment for Fetuses with Early-Onset Growth Restriction (TADAFER) II population. Neonatal and maternal adverse events were analyzed, in addition to fetal, neonatal, and infant death cases, six months after stopping the trial. Eighty-nine pregnant women with FGR were studied between September 2016 and March 2018 (45 and 44 in the tadalafil and conventional treatment groups, respectively). Seven (16%) deaths (four fetal, one neonatal, and two infant) in the control group, whereas only one neonatal death occurred in the tadalafil group. Although headache, facial flushing, and nasal hemorrhage occurred more frequently in the tadalafil group, these symptoms were Grade 1 and transient. In conclusion, this trial showed that tadalafil decreased the fetal and infant deaths associated with FGR. This is thought to be primarily due to pregnancy prolongation. Further studies are warranted to evaluate the efficacy of tadalafil in treating early-onset FGR.

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