Improved detection of hepatocyte proliferation using antibody to the pre-replication complex: An association with hepatic fibrosis and viral replication in chronic hepatitis C virus infection

A. Freeman; S. Hamid; L. Morris; S. Vowler; S. Rushbrook; D. G.D. Wight; N. Coleman; G. J.M. Alexander

doi:10.1046/j.1365-2893.2003.00454.x

Improved detection of hepatocyte proliferation using antibody to the pre-replication complex: An association with hepatic fibrosis and viral replication in chronic hepatitis C virus infection

A. Freeman
, S. Hamid
, L. Morris
, S. Vowler
, S. Rushbrook
, D. G.D. Wight
, N. Coleman
, G. J.M. Alexander

Research output: Contribution to journal › Article › peer-review

30 Citations (Scopus)

Abstract

To test the hypothesis that hepatitis C virus (HCV) might induce hepatocyte proliferation directly, thereby pre-disposing HCV carriers to cirrhosis and hepatocellular carcinoma, we have used a new method to identify proliferating hepatocytes, employing a novel monoclonal antibody to minichromosome maintenance (Mcm) proteins, essential components of the pre-replication complex. Antibody to Ki-67, a conventional marker of cell division, was also studied. Eighty-seven patients with chronic HCV infection and a broad spectrum of histological change were studied. Proliferation was observed rarely in hepatocytes from normal liver from healthy controls (always less than 0.01%). However, proliferating hepatocytes were detected in all HCV-infected patients and the proportion of hepatocytes expressing Mcm-2 (3-40%) always exceeded that expressing Ki-67 (1-14%) and correlated positively with increasing stage of fibrosis (P = 0.0001) and viral replication (P = 0.0004). There were weaker but significant associations between the proportion of hepatocytes expressing Mcm-2 and inflammatory indices including interface hepatitis, portal tract inflammation, lobular inflammation and steatosis. There was no association between the proportion of hepatocytes expressing Mcm-2 and age, gender or past alcohol consumption, but there was a weak association with current consumption of alcohol (P = 0.0067). The proportion of Ki-67 hepatocytes did not correlate with any clinical, laboratory or histological parameter. Mcm-2 was also detected in bile duct cells, sinusoidal lining cells and infiltrating lymphocytes, but at low frequency. These data indicate first, that Mcm-2 is a more sensitive marker of hepatocyte proliferation than Ki-67, second that many hepatocytes in chronic HCV infection have entered the cell cycle and third, suggest that interference with the hepatocyte cell cycle might be an alternative approach to therapy.

Original language	English (UK)
Pages (from-to)	345-350
Number of pages	6
Journal	Journal of Viral Hepatitis
Volume	10
Issue number	5
DOIs	https://doi.org/10.1046/j.1365-2893.2003.00454.x
Publication status	Published - Sept 2003
Externally published	Yes

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

Keywords

Cell cycle
DNA proliferation
Disease progression
Hepatitis C
Natural history

Access to Document

10.1046/j.1365-2893.2003.00454.x

Cite this

Freeman, A., Hamid, S., Morris, L., Vowler, S., Rushbrook, S., Wight, D. G. D., Coleman, N., & Alexander, G. J. M. (2003). Improved detection of hepatocyte proliferation using antibody to the pre-replication complex: An association with hepatic fibrosis and viral replication in chronic hepatitis C virus infection. Journal of Viral Hepatitis, 10(5), 345-350. https://doi.org/10.1046/j.1365-2893.2003.00454.x

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title = "Improved detection of hepatocyte proliferation using antibody to the pre-replication complex: An association with hepatic fibrosis and viral replication in chronic hepatitis C virus infection",

abstract = "To test the hypothesis that hepatitis C virus (HCV) might induce hepatocyte proliferation directly, thereby pre-disposing HCV carriers to cirrhosis and hepatocellular carcinoma, we have used a new method to identify proliferating hepatocytes, employing a novel monoclonal antibody to minichromosome maintenance (Mcm) proteins, essential components of the pre-replication complex. Antibody to Ki-67, a conventional marker of cell division, was also studied. Eighty-seven patients with chronic HCV infection and a broad spectrum of histological change were studied. Proliferation was observed rarely in hepatocytes from normal liver from healthy controls (always less than 0.01\%). However, proliferating hepatocytes were detected in all HCV-infected patients and the proportion of hepatocytes expressing Mcm-2 (3-40\%) always exceeded that expressing Ki-67 (1-14\%) and correlated positively with increasing stage of fibrosis (P = 0.0001) and viral replication (P = 0.0004). There were weaker but significant associations between the proportion of hepatocytes expressing Mcm-2 and inflammatory indices including interface hepatitis, portal tract inflammation, lobular inflammation and steatosis. There was no association between the proportion of hepatocytes expressing Mcm-2 and age, gender or past alcohol consumption, but there was a weak association with current consumption of alcohol (P = 0.0067). The proportion of Ki-67 hepatocytes did not correlate with any clinical, laboratory or histological parameter. Mcm-2 was also detected in bile duct cells, sinusoidal lining cells and infiltrating lymphocytes, but at low frequency. These data indicate first, that Mcm-2 is a more sensitive marker of hepatocyte proliferation than Ki-67, second that many hepatocytes in chronic HCV infection have entered the cell cycle and third, suggest that interference with the hepatocyte cell cycle might be an alternative approach to therapy.",

keywords = "Cell cycle, DNA proliferation, Disease progression, Hepatitis C, Natural history",

author = "A. Freeman and S. Hamid and L. Morris and S. Vowler and S. Rushbrook and Wight, \{D. G.D.\} and N. Coleman and Alexander, \{G. J.M.\}",

year = "2003",

month = sep,

doi = "10.1046/j.1365-2893.2003.00454.x",

language = "English (UK)",

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Freeman, A, Hamid, S, Morris, L, Vowler, S, Rushbrook, S, Wight, DGD, Coleman, N & Alexander, GJM 2003, 'Improved detection of hepatocyte proliferation using antibody to the pre-replication complex: An association with hepatic fibrosis and viral replication in chronic hepatitis C virus infection', Journal of Viral Hepatitis, vol. 10, no. 5, pp. 345-350. https://doi.org/10.1046/j.1365-2893.2003.00454.x

Improved detection of hepatocyte proliferation using antibody to the pre-replication complex: An association with hepatic fibrosis and viral replication in chronic hepatitis C virus infection. / Freeman, A.; Hamid, S.; Morris, L. et al.
In: Journal of Viral Hepatitis, Vol. 10, No. 5, 09.2003, p. 345-350.

Research output: Contribution to journal › Article › peer-review

TY - JOUR

T1 - Improved detection of hepatocyte proliferation using antibody to the pre-replication complex

T2 - An association with hepatic fibrosis and viral replication in chronic hepatitis C virus infection

AU - Freeman, A.

AU - Hamid, S.

AU - Morris, L.

AU - Vowler, S.

AU - Rushbrook, S.

AU - Wight, D. G.D.

AU - Coleman, N.

AU - Alexander, G. J.M.

PY - 2003/9

Y1 - 2003/9

N2 - To test the hypothesis that hepatitis C virus (HCV) might induce hepatocyte proliferation directly, thereby pre-disposing HCV carriers to cirrhosis and hepatocellular carcinoma, we have used a new method to identify proliferating hepatocytes, employing a novel monoclonal antibody to minichromosome maintenance (Mcm) proteins, essential components of the pre-replication complex. Antibody to Ki-67, a conventional marker of cell division, was also studied. Eighty-seven patients with chronic HCV infection and a broad spectrum of histological change were studied. Proliferation was observed rarely in hepatocytes from normal liver from healthy controls (always less than 0.01%). However, proliferating hepatocytes were detected in all HCV-infected patients and the proportion of hepatocytes expressing Mcm-2 (3-40%) always exceeded that expressing Ki-67 (1-14%) and correlated positively with increasing stage of fibrosis (P = 0.0001) and viral replication (P = 0.0004). There were weaker but significant associations between the proportion of hepatocytes expressing Mcm-2 and inflammatory indices including interface hepatitis, portal tract inflammation, lobular inflammation and steatosis. There was no association between the proportion of hepatocytes expressing Mcm-2 and age, gender or past alcohol consumption, but there was a weak association with current consumption of alcohol (P = 0.0067). The proportion of Ki-67 hepatocytes did not correlate with any clinical, laboratory or histological parameter. Mcm-2 was also detected in bile duct cells, sinusoidal lining cells and infiltrating lymphocytes, but at low frequency. These data indicate first, that Mcm-2 is a more sensitive marker of hepatocyte proliferation than Ki-67, second that many hepatocytes in chronic HCV infection have entered the cell cycle and third, suggest that interference with the hepatocyte cell cycle might be an alternative approach to therapy.

AB - To test the hypothesis that hepatitis C virus (HCV) might induce hepatocyte proliferation directly, thereby pre-disposing HCV carriers to cirrhosis and hepatocellular carcinoma, we have used a new method to identify proliferating hepatocytes, employing a novel monoclonal antibody to minichromosome maintenance (Mcm) proteins, essential components of the pre-replication complex. Antibody to Ki-67, a conventional marker of cell division, was also studied. Eighty-seven patients with chronic HCV infection and a broad spectrum of histological change were studied. Proliferation was observed rarely in hepatocytes from normal liver from healthy controls (always less than 0.01%). However, proliferating hepatocytes were detected in all HCV-infected patients and the proportion of hepatocytes expressing Mcm-2 (3-40%) always exceeded that expressing Ki-67 (1-14%) and correlated positively with increasing stage of fibrosis (P = 0.0001) and viral replication (P = 0.0004). There were weaker but significant associations between the proportion of hepatocytes expressing Mcm-2 and inflammatory indices including interface hepatitis, portal tract inflammation, lobular inflammation and steatosis. There was no association between the proportion of hepatocytes expressing Mcm-2 and age, gender or past alcohol consumption, but there was a weak association with current consumption of alcohol (P = 0.0067). The proportion of Ki-67 hepatocytes did not correlate with any clinical, laboratory or histological parameter. Mcm-2 was also detected in bile duct cells, sinusoidal lining cells and infiltrating lymphocytes, but at low frequency. These data indicate first, that Mcm-2 is a more sensitive marker of hepatocyte proliferation than Ki-67, second that many hepatocytes in chronic HCV infection have entered the cell cycle and third, suggest that interference with the hepatocyte cell cycle might be an alternative approach to therapy.

KW - Cell cycle

KW - DNA proliferation

KW - Disease progression

KW - Hepatitis C

KW - Natural history

UR - https://www.scopus.com/pages/publications/0141427994

U2 - 10.1046/j.1365-2893.2003.00454.x

DO - 10.1046/j.1365-2893.2003.00454.x

M3 - Article

C2 - 12969185

AN - SCOPUS:0141427994

SN - 1352-0504

VL - 10

SP - 345

EP - 350

JO - Journal of Viral Hepatitis

JF - Journal of Viral Hepatitis

IS - 5

ER -

Improved detection of hepatocyte proliferation using antibody to the pre-replication complex: An association with hepatic fibrosis and viral replication in chronic hepatitis C virus infection

Abstract

UN SDGs

Keywords

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