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X 染色体编码的癌症/睾丸抗原在发育中的性腺和睾丸精原细胞瘤中表现出独特的表达模式。

Chromosome X-encoded cancer/testis antigens show distinctive expression patterns in developing gonads and in testicular seminoma.

机构信息

Weill Cornell Medical College, 1300 York Avenue, New York, NY 10021, USA.

出版信息

Hum Reprod. 2011 Dec;26(12):3232-43. doi: 10.1093/humrep/der330. Epub 2011 Oct 20.

DOI:10.1093/humrep/der330
PMID:22016418
Abstract

BACKGROUND

Cancer/testis (CT) antigens are cancer antigens normally expressed in adult testicular germ cells. The expression of chromosome X-encoded CT antigens (CT-X antigens) in human fetal gonads and in testicular seminomas was examined.

METHODS

The expression of 10 CT-X antigens (MAGEA, NY-ESO-1, GAGE, CT7/MAGEC1, CT10/MAGEC2, CT45, SAGE1, SSX2, NXF2 and SPANX) was studied immunohistochemically.

RESULTS

In adult human testis, SPANX is expressed in late spermatids and spermatozoa, whereas all other CT-X antigens are predominantly expressed in spermatogonia or primary spermatocytes. All CT-X antigens except SPANX are expressed in human fetal germ cells. CT-X-positive germ cells appear as early as 13 weeks after gestation, increase with age and reach a plateau at around 22 weeks. In the fetal ovary, CT-X-positive oogonia are most abundant at around 24 weeks and sharply decrease subsequently. CT-X antigens are almost exclusively expressed in OCT3/4-negative gonocytes and their expression appears to coincide with the loss of pluripotency. Spermatocytic seminoma, a neoplasm derived from adult pre-meiotic germ cells, showed uniform expression of all CT-X antigens except SPANX. In contrast, most seminomas (>80%) express CT7, CT45, GAGE and CT10 but express MAGEA, NXF2 and NY-ESO-1 at lower frequency, and very rarely express SSX2 and SAGE1.

CONCLUSIONS

Most CT-X antigens are expressed in human fetal germ cells after they have lost stem cell characteristics, with predominant expression in pre-meiotic germ cells. Spermatocytic seminomas showed expression of all CT-X antigens except SPANX, whereas classical seminomas only express some CT-X antigens, reflecting their different origins from adult versus fetal germ cells.

摘要

背景

癌症/睾丸(CT)抗原是正常在成人睾丸生殖细胞中表达的癌症抗原。本研究检测了人胎儿生殖腺和睾丸精原细胞瘤中 X 染色体编码的 CT 抗原(CT-X 抗原)的表达情况。

方法

采用免疫组织化学方法检测 10 种 CT-X 抗原(MAGEA、NY-ESO-1、GAGE、CT7/MAGEC1、CT10/MAGEC2、CT45、SAGE1、SSX2、NXF2 和 SPANX)的表达情况。

结果

在成人睾丸中,SPANX 仅在晚期精母细胞和精子中表达,而其他所有 CT-X 抗原均主要在精原细胞或初级精母细胞中表达。除 SPANX 外,所有 CT-X 抗原均在人胎儿生殖细胞中表达。CT-X 阳性生殖细胞早在妊娠 13 周后即可出现,随着胎龄的增加而增加,并在 22 周左右达到高峰。在胎儿卵巢中,CT-X 阳性卵母细胞在 24 周左右最为丰富,随后急剧减少。CT-X 抗原几乎仅在 OCT3/4 阴性性生殖细胞中表达,其表达似乎与多能性丧失一致。精原细胞瘤是来源于成人减数分裂前生殖细胞的肿瘤,除 SPANX 外,所有 CT-X 抗原均呈均匀表达。相比之下,大多数精原细胞瘤(>80%)表达 CT7、CT45、GAGE 和 CT10,但 MAGEA、NXF2 和 NY-ESO-1 的表达频率较低,且很少表达 SSX2 和 SAGE1。

结论

大多数 CT-X 抗原在人类胎儿生殖细胞失去干细胞特征后表达,主要在减数分裂前生殖细胞中表达。精原细胞瘤除 SPANX 外,表达所有 CT-X 抗原,而经典精原细胞瘤仅表达某些 CT-X 抗原,反映了它们起源于成人还是胎儿生殖细胞的不同。

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