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Identification of Mallory bodies with rhodamine B fluorescence and other stains for keratin.

作者信息

Wessely Z, Shapiro S H, Klavins J V, Tinberg H M

出版信息

Stain Technol. 1981 May;56(3):169-76. doi: 10.3109/10520298109067305.

DOI:10.3109/10520298109067305
PMID:6168037
Abstract

Rhodamine B staining in conjunction with fluorescence microscopy is shown to demonstrate Mallory bodies. Mallory body morphology, localization, and distribution in hepatocytes from griseofulvin-fed mice, human hepatoma, and human alcoholics were similar to those observed in the same tissues after conventional staining methods for Mallory bodies. The presence of these inclusions was further confirmed by specific cytochemical localization with indirect immunoperoxidase labeling, horseradish peroxidase labeling, and electron microscopy. Other tinctorial or histochemical procedures previously used for keratin or prekeratin (modified Mallory stain, Kreyberg method, Pauly method for histidine) also stained Mallory bodies for study with white light microscopy but with decreasing sensitivity respectively. Mallory bodies from mouse and human liver both appear to contain a keratin-like moiety. This entity may be simply, rapidly, and permanently stained with rhodamine B, and selectively and reproducibly demonstrated with fluorescence microscopy.

摘要

相似文献

1
Identification of Mallory bodies with rhodamine B fluorescence and other stains for keratin.
Stain Technol. 1981 May;56(3):169-76. doi: 10.3109/10520298109067305.
2
Changes in the cytokeratin intermediate filament cytoskeleton associated with Mallory body formation in mouse and human liver.
Hepatology. 1987 Nov-Dec;7(6):1215-23. doi: 10.1002/hep.1840070608.
3
Formation and involution of Mallory bodies ("alcoholic hyalin") in murine and human liver revealed by immunofluorescence microscopy with antibodies to prekeratin.用抗前角蛋白抗体通过免疫荧光显微镜观察小鼠和人肝脏中马洛里小体(“酒精性透明小体”)的形成与消退。
Proc Natl Acad Sci U S A. 1979 Aug;76(8):4112-6. doi: 10.1073/pnas.76.8.4112.
4
Ultrastructural, biochemical, and immunologic characterization of Mallory bodies in livers of griseofulvin-treated mice. Fimbriated rods of filaments containing prekeratin-like polypeptides.灰黄霉素处理小鼠肝脏中马洛里小体的超微结构、生化及免疫学特征。含前角蛋白样多肽的丝状菌毛棒。
Lab Invest. 1979 Feb;40(2):207-20.
5
Mallory bodies: lesions of hepatocytes containing proteins of the keratin-myosin-epidermin group.马洛里小体:肝细胞的病变,含有角蛋白-肌球蛋白-表皮素族蛋白。
Histochemistry. 1982;75(4):445-60. doi: 10.1007/BF00640597.
6
Immunological and biochemical characterization of the keratin-related component of Mallory bodies: a pathological pattern of hepatocytic cytokeratins.
Liver. 1982 Sep;2(3):165-75. doi: 10.1111/j.1600-0676.1982.tb00194.x.
7
Fate of Mallory body-containing hepatocytes: disappearance of Mallory bodies and restoration of the hepatocytic intermediate filament cytoskeleton after drug withdrawal in the griseofulvin-treated mouse.
Hepatology. 1990 Apr;11(4):652-61. doi: 10.1002/hep.1840110419.
8
Experimental induction of hepatocellular hyalin (Mallory bodies) in mice by griseofulvin treatment. 1. Light microscopic observation.用灰黄霉素处理小鼠实验诱导肝细胞透明变性(马洛里小体)。1. 光学显微镜观察。
Lab Invest. 1976 Oct;35(4):377-82.
9
Disturbance of keratin homeostasis in griseofulvin-intoxicated mouse liver.灰黄霉素中毒小鼠肝脏中角蛋白稳态的紊乱
Lab Invest. 1993 Nov;69(5):576-82.
10
Relationship of Mallory bodies to the cytoskeleton of hepatocytes in griseofulvin-treated mice.灰黄霉素处理小鼠中马洛里小体与肝细胞细胞骨架的关系。
Lab Invest. 1982 Oct;47(4):336-45.

引用本文的文献

1
A study on the interaction of rhodamine B with methylthioadenosine phosphorylase protein sourced from an Antarctic soil metagenomic library.来自南极土壤宏基因组文库的硫代腺苷甲硫氨酸磷酸化酶蛋白与罗丹明 B 的相互作用研究。
PLoS One. 2013;8(1):e55697. doi: 10.1371/journal.pone.0055697. Epub 2013 Jan 31.
2
Formation of Mallory body-like inclusions and cell death induced by deregulated expression of keratin 18.角蛋白18表达失调诱导马洛里小体样包涵体的形成及细胞死亡。
Mol Biol Cell. 2002 Oct;13(10):3441-51. doi: 10.1091/mbc.01-10-0510.
3
Mallory bodies: lesions of hepatocytes containing proteins of the keratin-myosin-epidermin group.
马洛里小体:肝细胞的病变,含有角蛋白-肌球蛋白-表皮素族蛋白。
Histochemistry. 1982;75(4):445-60. doi: 10.1007/BF00640597.