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(American Journal of Pathology. 1999;154:1701-1710.)
© 1999 American Society for Investigative Pathology

Regular Articles

Analysis of Intracytoplasmic Hyaline Bodies in a Hepatocellular Carcinoma

Demonstration of p62 as Major Constituent

Cornelia Stumptner^*, Hans Heid, Andrea Fuchsbichler^*, Hubert Hauser, Hans-Jörg Mischinger, Kurt Zatloukal^* and Helmut Denk^*

From the Departments of Pathology^*
and Surgery,
University of Graz School of Medicine, Graz, Austria, and the Division of Cell Biology,
German Cancer Research Center, Heidelberg, Germany

Intracytoplasmic hyaline bodies (IHBs) resemble inclusions in hepatocellular carcinoma cells, which so far have escaped further characterization. A relationship to Mallory bodies was suggested on the basis of light microscopy and filamentous ultrastructure. A hepatocellular carcinoma containing numerous IHBs was studied. Our studies revealed immunoreactivity of IHBs with the monoclonal antibodies SMI 31 and MPM-2, which recognize hyperphosphorylated epitopes present on paired helical filaments in Alzheimer's disease brains (SMI 31) or on diverse proteins hyperphosphorylated by mitotic kinases in the M-phase of the cell cycle (MPM-2). One- and two-dimensional gel electrophoresis of tumor extracts followed by immunoblotting with SMI 31 and MPM-2 antibodies revealed a major immunoreactive protein with an apparent molecular weight between 62 and 65 kd, which was resolved into several highly acidic (pH 4.5) protein components in two-dimensional gels. This protein was undetectable in non-neoplastic liver tissue. Sequence analysis identified the SMI 31 and MPM-2 immunoreactive material as p62, indicating that p62 is a major constituent of IHBs. p62 is an only recently discovered protein that is a phosphotyrosine-independent ligand of the SH2 domain of p56^lck, a member of the c-src family of cytoplasmic kinases. Moreover, p62 binds ubiquitin and may act as an adapter linking ubiquitinated species to other proteins. These features suggest a role of p62 in signal transduction and possibly also carcinogenesis. IHBs observed in the hepatocellular carcinoma cells presented are the first indications of a role of p62 in disease.

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