首页> 外文期刊>Lung cancer: Journal of the International Association for the Study of Lung Cancer >Pulmonary adenosquamous carcinoma with mucoepidermoid carcinoma-like component with characteristic p63 staining pattern: Either a novel subtype originating from bronchial epithelium or variant mucoepidermoid carcinoma
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Pulmonary adenosquamous carcinoma with mucoepidermoid carcinoma-like component with characteristic p63 staining pattern: Either a novel subtype originating from bronchial epithelium or variant mucoepidermoid carcinoma

机译:具有特征性p63染色模式的类黏液表皮样癌成分的肺腺鳞癌:源自支气管上皮的新型亚型或变异的黏液表皮样癌

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Background: Our previous study found unique adenosquamous carcinomas (ADSQs) containing a mucoepidermoid carcinoma (MEC)-like component and a characteristic p63 staining pattern. This study focused on these unique ADSQs. Methods: Thirty ADSQ cases were studied histologically and by immunohistochemistry for TTF-1 and p63. Of these 30 ADSQs, eight were selected as unique ADSQs. The clinicopathological characteristics of these ADSQs were further studied, and the gene rearrangement of mammalian mastermind-like 2 (MAML2) was investigated by fluorescence in situ hybridization (FISH) for differentiation from pulmonary MEC. Results: The clinicopathological characteristics between the eight ADSQs and the other ADSQ cases showed no statistically significant differences, except for serum CEA level. Histologically, the eight ADSQs contained varying degrees of the MEC-like component, which consisted of solid nests with mucin-filled cysts or a cribriform-like structure. Immunohistochemically, p63-positive nuclei characteristically encircled the tumor nests, although TTF-1 was completely negative. All unique ADSQs not only had a variable degree of squamous cell carcinoma component in addition to the MEC-like component, but also contained a small tubular adenocarcinoma component in three tumors. FISH analysis revealed no MAML2 gene rearrangement in the eight ADSQs. Conclusions: Of the 30 ADSQs investigated in this study, eight contained a MEC-like component with a characteristic p63 basilar staining pattern similar to that of bronchial basal cells. These unique ADSQs shared clinical characteristics with ordinary ADSQs, but clinicopathologically differed from pulmonary ordinary MEC. Therefore, these unique ADSQs may be either a novel ADSQ subtype originating from bronchial epithelium or variant-type MEC.
机译:背景:我们以前的研究发现独特的腺鳞癌(ADSQs)包含类粘液表皮样癌(MEC)样和特征性的p63染色模式。这项研究的重点是这些独特的ADSQ。方法:对30例ADSQ病例进行了组织学和免疫组化的TTF-1和p63研究。在这30个ADSQ中,有8个被选为唯一的ADSQ。进一步研究了这些ADSQs的临床病理特征,并通过荧光原位杂交(FISH)研究了哺乳动物主敏样2(MAML2)的基因重排,以区别于肺部MEC。结果:除了血清CEA水平外,八个ADSQ与其他ADSQ病例之间的临床病理特征无统计学差异。从组织学上讲,八个ADSQs包含不同程度的MEC样成分,由具有粘蛋白填充囊肿或筛状结构的固体巢组成。免疫组织化学分析显示,尽管TTF-1完全阴性,但p63阳性细胞核却以肿瘤为特​​征。除MEC样成分外,所有独特的ADSQ不仅具有可变程度的鳞状细胞癌成分,而且在三种肿瘤中还包含小的管状腺癌成分。 FISH分析显示八个ADSQ中没有MAML2基因重排。结论:在这项研究中研究的30个ADSQ中,有8个包含MEC样成分,其特征性p63基底染色模式类似于支气管基底细胞。这些独特的ADSQ与普通ADSQ具有共同的临床特征,但临床病理上与肺部普通MEC不同。因此,这些独特的ADSQ可能是源自支气管上皮的新型ADSQ亚型,也可能是变异型MEC。

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