L. Posobiec, J. Vidal, Angela Hughes-Earle, Susan B Laffan, T. Hart
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引用次数: 7
摘要
Dabrafenib (DAB)是一种BRAF激酶活性抑制剂,被批准用于BRAF V600E突变的转移性黑色素瘤。为了支持儿童癌症的发展,进行了一项非临床幼年大鼠毒性研究,其中雌性早期阴道开口(VO)。据推测,早期的VO不是性成熟的标志,而是阴道局部作用的结果。一项模拟最终研究设计的调查研究进行了,从出生后第7天(PND)到35岁,大鼠口服DAB或载药,并在VO之前,在第一次和第二次发情,以及年龄匹配的对照组进行尸检。对生殖组织进行组织病理学检查,包括免疫组化检测BRAF表达。女性DAB患者比对照组更早发生VO (PND 27.2 vs. 31.5);然而,第一次发情的时间不受影响(PND 34.0 vs. 33.0)。在VO (PND 22.0)之前接受dada治疗的女性生殖道大多不成熟,没有排卵的证据,与年龄匹配的对照组相似;然而,接受dada治疗的女性阴道角化,组织学上开放。此外,泌尿生殖区周围有凸起的皮肤,这与外阴皮肤增生/角化病和阴道远端角化有关。BRAF表达(在对照组中评估)局限于这些组织。因此,给予DAB的大鼠早期VO可能代表了局部效应,加速阴道角化变得开放,而不是加速性成熟。
Early Vaginal Opening in Juvenile Female Rats Given BRAF-Inhibitor Dabrafenib Is Not Associated with Early Physiologic Sexual Maturation.
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.
期刊介绍:
The purpose of this journal is to publish original contributions describing the toxicity of chemicals to developing organisms and the process of reproduction. The scope of the journal will inlcude: • toxicity of new chemical entities and biotechnology derived products to developing organismal systems; • toxicity of these and other xenobiotic agents to reproductive function; • multi-generation studies; • endocrine-mediated toxicity, particularly for endpoints that are relevant to development and reproduction; • novel protocols for evaluating developmental and reproductive toxicity; Part B: Developmental and Reproductive Toxicology , formerly published as Teratogenesis, Carcinogenesis and Mutagenesis