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首页> 外文期刊>Histology and histopathology >Histological complexities of pancreatic lesions from transgenic mouse models are consistent with biological and morphological heterogeneity of human pancreatic cancer.
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Histological complexities of pancreatic lesions from transgenic mouse models are consistent with biological and morphological heterogeneity of human pancreatic cancer.

机译:来自转基因小鼠模型的胰腺病变的组织学复杂性与人类胰腺癌的生物学和形态学异质性是一致的。

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摘要

Although pancreatic cancer is the fourth leading cause of cancer death, it has received much less attention compared to other malignancies. There are several transgenic animal models available for studies of pancreatic carcinogenesis, but most of them do not recapitulate, histologically, human pancreatic cancer. Here we review some detailed molecular complexity of human pancreatic cancer and their reflection in histomorphological complexities of pancreatic lesions developed in various transgenic mouse models with a special concern for studying the effects of chemotherapeutic and chemopreventive agents. These studies usually require a large number of animals that are at the same age and gender and should be either homozygote or heterozygote but not a mixture of both. Only single-transgene models can meet these special requirements, but many currently available models require a mouse to simultaneously bear several transgene alleles. Thus it is imperative to identify new gene promoters or enhancers that are specific for the ductal cells of the pancreas and are highly active in vivo so as to establish new single-transgene models that yield pancreatic ductal adenocarcinomas for chemotherapeutic and chemopreventive studies.
机译:尽管胰腺癌是癌症死亡的第四大主要原因,但与其他恶性肿瘤相比,它受到的关注要少得多。有几种可用于胰腺癌发生研究的转基因动物模型,但是从组织学角度讲,大多数它们并没有概括人类胰腺癌。在这里,我们审查了人类胰腺癌的一些详细的分子复杂性,以及它们在各种转基因小鼠模型中发展的胰腺病变的组织形态学复杂性中的反映,特别关注了研究化学疗法和化学预防剂的作用。这些研究通常需要大量具有相同年龄和性别的动物,并且应该是纯合子或杂合子,而不是两者的混合物。只有单转基因模型可以满足这些特殊要求,但是许多当前可用的模型需要鼠标同时带有多个转基因等位基因。因此,必须确定对胰腺导管细胞具有特异性并在体内具有高活性的新基因启动子或增强子,以便建立新的单转基因模型,以产生胰腺导管腺癌用于化学疗法和化学预防研究。

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