[HTML][HTML] Myofibroblastic cell activation and neovascularization predict native liver survival and development of esophageal varices in biliary atresia

JS Suominen, H Lampela, P Heikkilä… - World Journal of …, 2014 - ncbi.nlm.nih.gov
JS Suominen, H Lampela, P Heikkilä, J Lohi, H Jalanko, MP Pakarinen
World Journal of Gastroenterology: WJG, 2014ncbi.nlm.nih.gov
AIM: To study the relation between collagen 1, α-smooth muscle actin (α-SMA) and CD34
expression and the most essential portoenterostomy (PE) outcomes. METHODS: Liver
specimens were obtained at PE from 33 biliary atresia (BA) patients for
immunohistochemical analysis of collagen 1, α-SMA and CD34. Liver biopsies from 35
organ donors were used as controls. Expression patterns were related to clinical data
including age at PE, serum total and conjugated bilirubin concentration at the time of PE and …
Abstract
AIM: To study the relation between collagen 1, α-smooth muscle actin (α-SMA) and CD34 expression and the most essential portoenterostomy (PE) outcomes.
METHODS: Liver specimens were obtained at PE from 33 biliary atresia (BA) patients for immunohistochemical analysis of collagen 1, α-SMA and CD34. Liver biopsies from 35 organ donors were used as controls. Expression patterns were related to clinical data including age at PE, serum total and conjugated bilirubin concentration at the time of PE and during follow-up, incidence of esophageal varices in follow-up upper gastrointestinal endoscopies, and native liver survival as well as to detailed histopathological findings.
RESULTS: Collagen 1 (16.4% vs 4.5%, P< 0.0001), α-SMA (17.9% vs 4.6%, P< 0.0001) and CD34 (4.9% vs 3.8%, P= 0.017) were markedly overexpressed in BA patients compared with controls. Patients who underwent liver transplantation by age of two years had significantly higher expression of collagen 1 (18.6% vs 13.7%, P= 0.024), α-SMA (20.4% vs 15.4%, P= 0.009) and CD34 (5.9% vs 4.0%, P= 0.029) at PE compared with native liver survivors. CD34-positive microvessels were identified in the centrizonal region close to central vein in every BA patient. In majority of BA cases (56%) neovascularization was frequent as CD34-positive microvessels were observed in over half of the hepatic lobules. In controls, the CD34-positive microvessels were rare as they were completely absent in 40% and were found in less than 5% of the hepatic lobules in the rest. The difference between BA patients and controls was significant (P< 0.0001). Patients who developed esophageal varices by two years had significantly higher expression of CD34 at PE compared with patients without varices (5.6% vs 4.0%, P= 0.019). Expression of α-SMA (r= 0.758, P< 0.0001) and collagen 1 (r= 0.474, P= 0.016), and the amount of CD34-positive microvessels (r= 0.356, P= 0.047) were related to patient age at PE.
CONCLUSION: Hepatic myofibroblastic cell activation, fibrogenesis and neovascularization are enhanced in BA, progress with increasing PE age and relate to native liver survival and development of esophageal varices.
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