C. Stumptner et al., Sequence of events in the assembly of Mallory body components in mouse liver: clues to the pathogenesis and significance of Mallory body formation, J HEPATOL, 34(5), 2001, pp. 665-675
Background/Aims: Chronic intoxication of mice with 3,5-diethoxycarbonyl-1,4
-dihydrocollidine (DDC) or griseofulvin (GF) results in appearance of Mallo
ry bodies (MBs) and alterations of the keratin cytoskeleton, which are reve
rsible upon drug withdrawal but recur after readministration within 2-3 day
s.
Methods: DDC- or GF-treated and recovered mice were reintoxicated with the
original drugs but also colchicine and lumicolchicine. Cytoskeletal alterat
ions of hepatocytes and MB formation were monitored by immunofluorescence m
icroscopy using keratin, MB-specific antibodies, antibodies to phosphoepito
pes and to HSP70, Keratin 8/18 mRNA expression and protein levels were dete
rmined by competitive reverse transcription-polymerase chain reaction, in s
itu-hybridization and western blotting.
Results: Duration of pretreatment was important for the efficiency of MB tr
iggering. Rapid increase of keratin 8/18 mRNA and proteins was found in all
reintoxicated mice concomitant with MB formation, whereby keratin 8 prevai
led over keratin 18. Keratins and a protein with heat shock characteristics
(M(M)120-1 antigen) were the earliest detectable MB components, whereas ub
iquitination and phosphorylation followed later.
Conclusions: Overproduction of keratins is a major but not the only step re
sponsible for MB formation. Additional components (e,g, M-M 120-1 antigen)
and excess of keratin 8 over keratin 18 are essential, (C) 2001 European As
sociation for the Study of the Liver. Published by Elsevier Science B.V. Al
l rights reserved.