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  2. Early Vaginal Opening in Juvenile Female Rats Given BRAF-Inhibitor Dabrafenib Is Not Associated with Early Physiologic Sexual Maturation

Early Vaginal Opening in Juvenile Female Rats Given BRAF-Inhibitor Dabrafenib Is Not Associated with Early Physiologic Sexual Maturation

  • Birth Defects Res B Dev Reprod Toxicol. 2015 Dec;104(6):244-52. doi: 10.1002/bdrb.21165.
Lorraine M Posobiec 1 Justin D Vidal 2 Angela Hughes-Earle 1 Susan B Laffan 1 Timothy Hart 1
Affiliations

Affiliations

  • 1 Safety Assessment, GlaxoSmithKline, King of Prussia, Pennsylvania.
  • 2 Vet Path Services, Inc, Mason, Ohio.
Abstract

Dabrafenib (DAB), an inhibitor of BRaf kinase activity, is approved for metastatic melanoma with a BRaf V600E mutation. In support of pediatric Cancer development, a nonclinical juvenile rat toxicity study was conducted in which females had early vaginal opening (VO). It was hypothesized that the early VO was not indicative of sexual maturation, but a result of a local effect on the vagina. An investigative study was conducted that mimicked the definitive study design, with rats given DAB or vehicle orally from Postnatal Day (PND) 7 to 35 and with necropsy subsets just before VO, at the first and second estrus, along with age-matched controls. Histopathology was performed on reproductive tissues, including immunohistochemistry for BRaf expression. VO occurred earlier in DAB females than in controls (PND 27.2 vs. 31.5); however, the timing of the first estrus was unaffected (PND 34.0 vs. 33.0). DAB-treated females evaluated just before VO (PND 22.0) had mostly immature reproductive tracts with no evidence of ovulation, similar to age-matched controls; however, DAB-treated females had keratinized and histologically open vaginas. Also, there was raised skin around the urogenital area, which correlated with hyperplasia/keratosis of the vulvar skin and keratinization of the distal vagina. BRaf expression (evaluated in controls) was localized to these tissues. Thus, early VO in rats given DAB likely represents a local effect accelerating vaginal keratinization to become open and not accelerated sexual maturation.

Keywords

postnatal evaluation; risk assessment; safety assessment; vagina.

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