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人类结肠黏膜中的异常隐窝:推定的癌前病变。

Aberrant crypts in human colonic mucosa: putative preneoplastic lesions.

作者信息

Pretlow T P, O'Riordan M A, Pretlow T G, Stellato T A

机构信息

Department of Pathology, Case Western Reserve University School of Medicine, Cleveland, Ohio 44106.

出版信息

J Cell Biochem Suppl. 1992;16G:55-62. doi: 10.1002/jcb.240501111.

Abstract

Aberrant crypts are recognized in methylene blue-stained, unsectioned, colonic mucosa by their increased size, elliptical lumenal opening, thicker epithelial layer, and increased pericryptal region. Aberrant crypt foci in rodents are observed as early as 2 weeks and for at least 9 months after a single dose of carcinogen, have a distribution that parallels that of tumors, and have an increased number of aberrant crypts per focus with time after the carcinogen dose. The ability to quantify these lesions in the entire colon of rodents in less than an hour suggests that aberrant crypts may provide a highly efficient in vivo bioassay for colon carcinogens. Since aberrant crypt foci appear to be the earliest identifiable putative precursors of colon cancer, they represent lesions that can be characterized further for the earliest genetic and biochemical alterations. In F344 rats, we have demonstrated that aberrant crypts have multiple histochemically-detectable enzyme alterations. Using similar techniques, we were the first to demonstrate aberrant crypts in unsectioned human mucosa. After embedding and sectioning, these microscopic aberrant crypts resemble rare lesions described earlier in the literature after extensive serial sectioning. In rats and humans, aberrant crypts may be histologically normal or display varying degrees of dysplasia and histochemically-detectable altered enzyme activities. These putative, preneoplastic lesions should reveal early changes that precede colon cancer and ways to alter their progression.

摘要

在亚甲蓝染色的未切片结肠黏膜中,异常隐窝可通过其增大的尺寸、椭圆形的管腔开口、更厚的上皮层以及增大的隐窝周围区域来识别。啮齿动物中的异常隐窝灶最早在单次给予致癌物后2周即可观察到,并且在至少9个月内持续存在,其分布与肿瘤相似,且每个灶中的异常隐窝数量在给予致癌物后随时间增加。在不到一小时的时间内对啮齿动物整个结肠中的这些病变进行量化的能力表明,异常隐窝可能为结肠癌致癌物提供一种高效的体内生物测定方法。由于异常隐窝灶似乎是结肠癌最早可识别的假定前体,它们代表了可以进一步表征最早的遗传和生化改变的病变。在F344大鼠中,我们已经证明异常隐窝有多种可通过组织化学检测到的酶改变。使用类似技术,我们首次在未切片的人类黏膜中证明了异常隐窝。在包埋和切片后,这些微观异常隐窝类似于文献中早期在广泛连续切片后描述的罕见病变。在大鼠和人类中,异常隐窝在组织学上可能是正常的,也可能表现出不同程度的发育异常以及可通过组织化学检测到的酶活性改变。这些假定的癌前病变应该揭示结肠癌之前的早期变化以及改变其进展的方法。

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