A mosaic karyotype of 45,X/46,X,psu idic(Y)(q12) in a ten-year-old boy: integrating high-throughput sequencing with cytogenetic technique for precise diagnosis and genetic counselling

The Y chromosome is one of the smallest chromosomes in human male, consisting of a short (Yp) arm and a long (Yq) one. The genes on the Y chromosome such as sex-determining gene SRY and spermatogenesis genes (azoospermia factor, AZF) are important for male sex determination and spermatogenesis [1]. Isodicentric Y chromosome (idic(Y)) is the most common Y chromosome aberration, and it consists of two identical arms with an axis of symmetry lying between two centromeres [2]. The unstable genomic structures of Y chromosome also occur in different cell lines, and consequently, most reported patients have alternate cell lines, including 45,X cell line [3]. The resulting phenotypes of the affected cases vary from healthy infertile males, females with or without Turner syndrome to individuals with ambiguous genitalia or with mixed gonadal dysgenesis, depending on the proportion of mosaics as well as the location of the breakpoints [4].

Here, we detailedly described a patient with short stature, hypospadias, micropenis and unilateral cryptorchidism without normal structure of testicular seminiferous tubules. We finished the accurate genetic diagnosis of the mosaic karyotype 45,X[8]/46,X,psu idic(Y)(q12)[32], combining high-throughput sequencing and cytogenetic tests.

A 10-year-old boy was referred to Affiliated Children’s Hospital of Capital Institute of Pediatrics due to complaints of short stature and micropenis. His mother and father had normal karyotypes. No family history of sterility or abortion was reported. The mother's and the father's height were 171 cm and 175 cm, respectively.

The patient underwent a C-section at 37 weeks because of fetal distress. His birth weight and height were 2960 g and 49 cm respectively. He was diagnosed as hypoxic ischemic encephalopathy (HIE) at birth, and showed borderline developmental delay since he was six months old. He suffered from epilepsy at age of 11 months. He was diagnosed as hypospadias, unilateral cryptorchidism and underwent left radical orchiectomy and urethroplasty when he was 13 months old. The biopsy of the left testicular didn’t show normal structure of seminiferous tubules. Instead, a number of fibrous connective tissue and new blood vessel presented (Fig. 1A). In addition, no mature structure of epididymal duct was seen in the left epididymidis with the full of immature mesenchymal cells (Fig. 1B).

The growth velocity was 3-4 cm per year since he was 5 years old. Physical examination at age of 10 showed a height of 129 cm (-2 SDS) and weight of 12 kg (-1.5 SDS) with proportional short stature. Genitourinary checkup revealed Prader class 5 genitalia, with approximately 4 cm-size penis. No palpable gonad was detected bilaterally in the scrotum. Ultrasound of the gonads showed right testis in the groin area, with a size of 1.39 × 0.63 cm. The baseline level of anti-mullerian hormone and inhibin B indicated dysfunction of sertoli cells (Table 1). Also, the level of testosterone concentration was relatively low. Further examination of these hormones after HCG and GnRHa stimulation demonstrated normal pituitary reaction and poor function of leydig cell, respectively (Table 1).

Due to the instability of isodicentric Y chromosome during cell division, it is likely to generate different cell lines. Several types of cell lines are found in reported patients with idic(Y), most commonly including 45,X cell line (95% of cases) [3]. Cases with mosaic 45,X/46,X,idic(Y) usually have very wide and variable phenotypes [6, 7]. Among these symptoms, ambiguous genitalia and short stature were most common.

We reported a new case presenting multiple phenotypes including short stature, hypospadias, micropenis and unilateral cryptorchidism. The karyotype of this patient showed two different cell lines: 45,X and 46,X,idic(Y), with the breakpoint was determined in Yq12. As we known, the phenotypes resulting from isodicentric Y chromosomes depends on the proportion of mosaics as well as the location of the breakpoints [4]. In order to explore the influence of mosaics with 45,X/46,X,dic(Y)(q12), we reviewed their phenotypes previously published and found that were variable (Table 2). In our case, in addition to the common phenotypes (ambiguous sexual development and short stature), testicular biopsy of the boy was proven to be immature tissues without normal seminiferous tubules structure. For his testicular function, the results of laboratory examination such as anti-mullerian hormone and inhibin B indicated poor function of his sertoli cells. This means that he is likely to be sterile in adulthood, as reported in previous literatures [8‐10]. Moreover, compared with the low level of testosterone, the levels of LH and FSH after GnRH stimulating test are relatively high. This means that his leydig cells are not functioning well, suggesting that he may have hypergonadotropic hypogonadism and the possibility of delayed puberty in the near future. One previous literature has reported a 14-year-old boy presenting delayed puberty, so further follow-up is needed for our patient [11].

The arrangement mechanism was studied before. An isodicentric Y chromosome is formed due to an aberrant homologous crossing over between opposite arms of a palindrome during spermatogenesis [16]. A duplication of the short arm and proximal long arm and a deletion of a part of the long arm is referred to as idic(Y)(q). The heterochromatin Yq12 region are unstable and fragile sites for breaking, that confer susceptibility to the formation of idic(Y)(q), possibly for the HSAT I/Alu/AT-rich tripartite repeat on human Yq12 is dramatic [17].

High-throughput sequencing technologies including WES, whole genome sequencing (WGS), CNV-Seq have been widely used in genetic diagnosis of rare diseases. In our study, whole Y chromosome mosaic duplication was firstly detected from CNV-Seq. However, the proportion of mosaics as well as the location of the breakpoints, which affect the clinical sex phenotype and disease severity, can not be determined, then cytogenetic tests was used to confirm the genetic diagnosis. Our case proved that the cytogenetic tests is still necessary technique for the patients detected as Y abnormality from sequencing because cytogenic tests can illuminate mosaics proportion and breakpoint location visually.

In conclusion, the present study reported the patient of a 10-year-old boy with mosaic 45,X/46,X,psu idic(Y)(q12). In addition to the common phenotypes, testicular biopsy of the boy showed no seminiferous tubules structure increasing a risk of delayed puberty and infertility. Our study proved that it would be beneficial to integrate high-throughput sequencing with cytogenetic technique for precise diagnosis, treatment and genetic counselling.