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Glial Implants in Gliomatosis Peritonei Arise from Normal Tissue, Not from the Associated Teratoma

机译:腹膜胶质瘤病的胶质植入物来自正常组织,而非相关的畸胎瘤

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摘要

Metaplasia of subcoelomic mesenchyme has been implicated, but not proven, in the pathogenesis of common gynecological diseases such as endometriosis and rarer entities such as leiomyomatosis peritonealis disseminata and gliomatosis peritonei (GP). GP is associated with ovarian teratomas and is characterized by numerous peritoneal and omental implants composed of glial tissue. Two theories to explain the origin of GP have been proposed. In one, glial implants arise from the teratoma, whereas in the other, pluripotent Müllerian stem cells in the peritoneum or subjacent mesenchyme undergo glial metaplasia. To address the origin of GP, we exploited a unique characteristic of many ovarian teratomas: they often contain a duplicated set of maternal chromosomes and are thus homozygous at polymorphic microsatellite (MS) loci. In contrast, DNA from matched normal or metaplastic tissue (containing genetic material of both maternal and paternal origin) is expected to show heterozygosity at many of these same MS loci. DNA samples extracted from paraffin-embedded normal tissue, ovarian teratoma and three individual laser-dissected glial implants were studied in two cases of GP. In one case, all three implants and normal tissue showed heterozygosity at each of three MS loci on different chromosomes, whereas the teratoma showed homozygosity at the same MS loci. Similar results were observed in the second case. Our findings indicate that glial implants in GP often arise from cells within the peritoneum, presumably pluripotent Müllerian stem cells, and not from the associated ovarian teratoma. This finding has important implications for more common gynecological entities with debatable pathogenesis, such as endometriosis, by definitively demonstrating the metaplastic potential of stem cells within the peritoneal cavity.
机译:亚结肠间质的化生与子宫内膜异位症等常见妇科疾病以及腹膜平滑肌瘤和腹膜胶质瘤病(GP)等罕见妇科疾病的发病机制有关,但尚未得到证实。 GP与卵巢畸胎瘤相关,其特征是由许多由胶质组织组成的腹膜和网膜植入物。提出了两种解释GP起源的理论。一种是胶质瘤植入物,而另一种是腹膜或下层间充质中的多能穆勒干细胞。为了解决GP的起源,我们利用了许多卵巢畸胎瘤的独特特征:它们通常包含一组重复的母体染色体,因此在多态微卫星(MS)位点是纯合的。相反,预期来自匹配的正常或化生组织(包含母体和父体来源的遗传物质)的DNA在许多这些相同的MS基因座上均表现出杂合性。在2例GP病例中,研究了从石蜡包埋的正常组织,卵巢畸胎瘤和3个单独的激光切割的神经胶质植入物中提取的DNA样品。在一种情况下,所有三个植入物和正常组织在不同染色体上的三个MS基因座中的每个处均显示杂合性,而畸胎瘤在相同MS基因座中显示出纯合性。在第二种情况下观察到类似的结果。我们的发现表明,GP中的神经胶质植入物通常来自腹膜内的细胞,可能是多能的苗勒氏干细胞,而不是来自相关的卵巢畸胎瘤。这一发现通过明确证实腹膜腔内干细胞的生化潜能,对更常见的妇科病原体(如子宫内膜异位症)具有重要意义。

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