Section on Endocrinology Genetics, Program on Developmental Endocrinology Genetics, Eunice Kennedy Shriver National Institute of Child Health & Human Development, and Pediatric Endocrinology Inter-Institute Training Program, National Institutes of Health, Bethesda, MD, USA.
Horm Metab Res. 2010 Aug;42(9):682-8. doi: 10.1055/s-0030-1252021. Epub 2010 Apr 21.
The original description of patients with Russell-Silver syndrome included precocious puberty, the mechanism of which was unclear. We describe a child with a Russell-Silver syndrome-like phenotype who presented with precocious puberty that was associated with hyperplasia of the Sertoli cells. The patient was found to have an immature cryptorchid testicle; hyperplastic Sertoli cells were also aneuploid carrying trisomy 8. This chromosomal abnormality was present in Sertoli cells only and could not be detected in peripheral lymphocytes, tunica vaginalis, or other, normal, testicular tissue. Sertoli cells in culture showed excess aromatization providing an explanation for the rapid advancement of the patient's bone age. We conclude that in a patient with a Russell-Silver syndrome-like phenotype, Sertoli cell hyperplasia was associated with somatic trisomy 8, increased aromatization, and gonadotropin-independent precocious puberty.
Russell-Silver 综合征患者的原始描述包括性早熟,但发病机制尚不清楚。我们描述了一例 Russell-Silver 综合征样表型的患儿,其性早熟与支持细胞增生有关。患者表现为隐睾,增生的支持细胞呈三体 8 号染色体非整倍体。这种染色体异常仅存在于支持细胞中,在外周血淋巴细胞、鞘膜或其他正常睾丸组织中无法检测到。培养的支持细胞表现出过度芳香化作用,这可以解释患者骨龄快速进展的原因。我们的结论是,在具有 Russell-Silver 综合征样表型的患者中,支持细胞增生与体细胞三体 8 号、芳香化作用增加以及促性腺激素非依赖性性早熟有关。