Your search keyword '"HEPATIC fibrosis"' showing total 11 results

1. ПОКРАЩЕННЯ ВЕРИФІКАЦІЇ ФІБРОЗУ ПЕЧІНКИ ЗА ДОПОМОГОЮ НОВИХ МАЛОІНВАЗИВНИХ МАРКЕРІВ У ХВОРИХ НА ХРОНІЧНІ ДИФУЗНІ ЗАХВОРЮВАННЯ ПЕЧІНКИ.

Author

Степанов, Ю. М., Діденко, В. І., Кленіна, І. А., Татарчук, О. М., and Петішко, О. П.

Subjects

*NON-alcoholic fatty liver disease, *LIVER disease etiology, *HEPATIC fibrosis, *CHRONIC active hepatitis, *HEPATITIS C virus

Abstract

. The aim of our research was to obtain new minimally invasive serum markers of fibrotic changes of liver in patients with chronic diffuse liver diseases of different etiology and compare them with traditional markers. 364 patients aged 30 to 66 years were examined: 221 women (60.7%) and 143 men (39.3%). Depending on the etiological factors, all patients were divided into 4 groups: group I consisted of 108 patients with non-alcoholic fatty liver disease (NAFLD), group II – 143 patients with chronic hepatitis associated with virus C (CHC), group III – 56 patients with alcoholic liver disease (ALD), group IV – 57 patients with toxic drug-induced hepatitis (TH). The control group consisted of 30 practically healthy people. Using correlation and ROC-analyzes, we obtained minimally invasive diagnostics markers that show the risk of developing liver fibrosis. For patients with NAFLD these were the levels of HOMA-IR, TNFα/IL-10 and α1-acid glycopeptide content, which are better in quality of the diagnostic model than the traditional Forns index, APRI, FIB-4, AAR. For patients with CHC, these were the protein-bound hydroxyproline (HPp/b) /HPf ratio, phospholipids content, and IL-6, CD4+ levels, which are better diagnostic models than the traditional Forns index, APRI, FIB-4, AAR. The following markers were obtained for patients with ALD – TNFα levels, HPp/b and glycosaminoglycans content, which are better diagnostic models than the traditional Forns index, APRI, FIB-4, AAR. For patients with TH, these were medium molecular weight peptides content, IL-6/IL-10 ratio and CD4+/CD8+, which are better diagnostic models than the traditional Forns index, APRI, FIB-4, AAR. Thus, new minimally invasive markers of fibrosis in patients with chronic diffuse liver diseases have been obtained. . The aim of our research was to obtain new minimally invasive serum markers of fibrotic changes of liver in patients with chronic diffuse liver diseases of different etiology and compare them with traditional markers. 364 patients aged 30 to 66 years were examined: 221 women (60.7%) and 143 men (39.3%). Depending on the etiological factors, all patients were divided into 4 groups: group I consisted of 108 patients with non-alcoholic fatty liver disease (NAFLD), group II – 143 patients with chronic hepatitis associated with virus C (CHC), group III – 56 patients with alcoholic liver disease (ALD), group IV – 57 patients with toxic drug-induced hepatitis (TH). The control group consisted of 30 practically healthy people. Using correlation and ROC-analyzes, we obtained minimally invasive diagnostics markers that show the risk of developing liver fibrosis. For patients with NAFLD these were the levels of HOMA-IR, TNFα/IL-10 and α1-acid glycopeptide content, which are better in quality of the diagnostic model than the traditional Forns index, APRI, FIB-4, AAR. For patients with CHC, these were the protein-bound hydroxyproline (HPp/b) /HPf ratio, phospholipids content, and IL-6, CD4+ levels, which are better diagnostic models than the traditional Forns index, APRI, FIB-4, AAR. The following markers were obtained for patients with ALD – TNFα levels, HPp/b and glycosaminoglycans content, which are better diagnostic models than the traditional Forns index, APRI, FIB-4, AAR. For patients with TH, these were medium molecular weight peptides content, IL-6/IL-10 ratio and CD4+/CD8+, which are better diagnostic models than the traditional Forns index, APRI, FIB-4, AAR. Thus, new minimally invasive markers of fibrosis in patients with chronic diffuse liver diseases have been obtained. [ABSTRACT FROM AUTHOR]

Published

2022

2. Prognostic model of rapid hepatic fibrosis progression in men with chronic hepatitis C

Author

T. I. Koval, L. M. Syzova, H. M. Dubynska, N. O. Pryimenko, and S. S. Rudenko

Subjects

chronic hepatitis C, hepatic fibrosis, men, prognosis, TLR7 gene, Pathology, RB1-214

Abstract

The aim of the research was to determine clinical and genetic predictors and to create a prognostic model for the rapid hepatic fibrosis progression in men with chronic hepatitis C. Materials and methods. А cross-sectional study which included 111 male patients with chronic hepatitis C was conducted. The patient examination program included: assessment of complaints and anamnestic data, physical examination, complete blood count, biochemical test, the stages of hepatic fibrosis according to METAVIR аnd genetic studies (detecting carriers alleles 11Gln or 11Leu of TLR7 gene in the genome of the examined men). Results. It was determined that informative predictors of rapid hepatic fibrosis progression in men with chronic hepatitis C are: ethanol use in a dose of more than 40 g/day (ОR = 2.40, P = 0.042), presence of chronic cholecystitis in past history (ОR = 2.94, P = 0.013), ALT level above 3 upper limit of normal (ОR = 2.49, P = 0.031), the levels of AST, GGT exceeding upper limit of normal (ОR = 6.94, P < 0.001 and ОR = 4.02, P = 0.001 respectively), hyperbilirubinemia (ОR = 3.13, P = 0.010) and carrier state of allele 11Gln of TLR7 gene in the genome (ОR = 3.62, P = 0.036). In order to optimize the prognosis of rapid hepatic fibrosis progression in men with chronic hepatitis C a model that demonstrated statistical significance (χ² = 44.73, P < 0.001) and high operational characteristics (sensitivity – 76.8 %, specificity – 74.5 %, the total number of correct predictions – 75.7 %, AUC of the ROC-curve – 0.828), which indicates the feasibility of its practical use, was proposed. Conclusions. An effective clinical and genetic prognostic model has been created and allows us to predict the probability of rapid hepatic fibrosis progression in men with chronic hepatitis C with high accuracy and to form a group of patients who need high priority antiviral therapy.

Published

2019

3. Патогенез фіброзу печінки та можливості його корекції = Pathogenesis of the hepatic fibrosis and possibilities of its correction = Патогенез фиброза печени и возможности его коррекции

Author

D. M. Gorchag, O. L. Kholodkova, and M. M. Perepeliuk

Subjects

патогенез, фіброз печінки, регенерація, збагачена тромбоцитами плазма, корекція, pathogenesis, hepatic fibrosis, regeneration, platelet-rich plasma, correction, Education, Sports, GV557-1198.995, Medicine

Abstract

Gorchag D. M., Kholodkova O. L., Perepeliuk M. M. Патогенез фіброзу печінки та можливості його корекції = Pathogenesis of the hepatic fibrosis and possibilities of its correction = Патогенез фиброза печени и возможности его коррекции Journal of Education, Health and Sport. 2016;6(10):586-600. eISSN 2391-8306. DOI http://dx.doi.org/10.5281/zenodo.179432 http://ojs.ukw.edu.pl/index.php/johs/article/view/4023 The journal has had 7 points in Ministry of Science and Higher Education parametric evaluation. Part B item 755 (23.12.2015). 755 Journal of Education, Health and Sport eISSN 2391-8306 7 © The Author (s) 2016; This article is published with open access at Licensee Open Journal Systems of Kazimierz Wielki University in Bydgoszcz, Poland Open Access. This article is distributed under the terms of the Creative Commons Attribution Noncommercial License which permits any noncommercial use, distribution, and reproduction in any medium, provided the original author(s) and source are credited. This is an open access article licensed under the terms of the Creative Commons Attribution Non Commercial License (http://creativecommons.org/licenses/by-nc/4.0/) which permits unrestricted, non commercial use, distribution and reproduction in any medium, provided the work is properly cited. This is an open access article licensed under the terms of the Creative Commons Attribution Non Commercial License (http://creativecommons.org/licenses/by-nc/4.0/) which permits unrestricted, non commercial use, distribution and reproduction in any medium, provided the work is properly cited. The authors declare that there is no conflict of interests regarding the publication of this paper. Received: 02.09.2016. Revised 24.09.2016. Accepted: 30.10.2016. УДК 616.36-018.22-092-08 ПАТОГЕНЕЗ ФІБРОЗУ ПЕЧІНКИ ТА МОЖЛИВОСТІ ЙОГО КОРЕКЦІЇ Д. М. Горчаг, О. Л. Холодкова, М. М. Перепелюк Одеський національний медичний університет, м. Одеса Резюме В статті розглянуті основні ланки патогенезу фіброзних змін у печінці за умов негативного впливу та можливі шляхи їх корекції. Обговорені можливості спрямованої індукції зворотного розвитку фіброзу печінки (ФП). Також наведені результати власних досліджень щодо ефективності застосування збагаченої тромбоцитами плазми при ФП. Ключові слова: патогенез; фіброз печінки; регенерація; збагачена тромбоцитами плазма; корекція. PATHOGENESIS OF THE HEPATIC FIBROSIS AND POSSIBILITIES OF ITS CORRECTION D. M. Gorchag, O. L. Kholodkova, M. M. Perepeliuk Odessa National Medical University, Odessa Summary The main links of the hepatic fibrosis pathogenesis under the negative condition are looked out in the article. Possibilities of the directed induction of reverse development of hepatic fibrosis are discussed. The data of own researches of the effectiveness of platelet-rich plasma also shown. Key words: pathogenesis; hepatic fibrosis; regeneration; platelet-rich plasma; correction. ПАТОГЕНЕЗ ФИБРОЗА ПЕЧЕНИ И ВОЗМОЖНОСТИ ЕГО КОРРЕКЦИИ Д. М. Горчаг, О. Л. Холодкова, М. М. Перепелюк Одесский национальный медицинский университет, г. Одесса Резюме В статье рассмотрены основные звенья патогенеза фиброзных изменений в печени в условиях негативного воздействия. Обсуждены возможности направленной индукции обратного развития фиброза печени (ФП). Также приведены результаты собственных исследований об эффективности использования обогащенной тромбоцитами плазмы при ФП. Ключевые слова: патогенез; фиброз печени; регенерация; обогащенная тромбоцитами плазма; коррекция.

Published

2016

4. IMPACT OF ANTIVIRAL THERAPY FOR CHRONIC HEPATITIS C ON CYTOKINE SYNTHESIS AND HEPATIC FIBROSING PROCESSES

Author

V. V. Shchekotov, I. A. Bulatova, A. P. Shchekotova, N. I. Nasibullina, G. G. Larionova, and A. I. Pavlov

Subjects

chronic hepatitis c, cytokine, tumor necrosis factor-α, interleukin-4, interleukin-6, hyaluronic acid, hepatic fibrosis, elastography, liver elasticity index, viremia, antiviral therapy, ribavirin, interferon alpha-2b, Medicine

Published

2015

5. The problem of viral hepatitis C in the Russian Federation

Author

N D Iushchuk, O O Znoĭko, K R Dudina, and P A Belyĭ

Subjects

chronic hepatitis c, antiviral therapy, disease burden, liver cirrhosis, hepatic fibrosis, hcv protease and polymerase inhibitors, pegylated interferon-α, ribavirin, Medicine

Abstract

The incidence of chronic viral hepatitides (CVH) has increased 2.2-fold in the Russian Federation over the past decade. This increase is mainly determined by an almost threefold rise in the incidence of chronic hepatitis C (CHC): from 12.9 in 1999 to 39.1 per 100,000 population in 2012. The calculated data of hepatitis C burden in the Russian Federation show that in 2010 the total medical and social losses and expenses associated with hepatitis C and its implications were 48.47 billion rubles or 0.108% of the gross domestic product, the direct medical costs were 17.1 billion (35.28%) rubles, GDP losses were 26.05 billion (53.75%) rubles, and the disability payments were 5.32 billion (10.97%) rubles. The patients (mean age 45 years) with liver cirrhosis (LC) were 15.2% in the structure of the CHC patients (mean age 37 years) admitted to Moscow infectious diseases hospitals in 2010. Analysis of the regional registers of the Russian Federation, the proportion of patients with LC among those with CHC was 18%. The existing forms for recording morbidity and mortality from poor CHC outcomes cannot significantly estimate the true disease stage distribution of patients and hepatitis C-associated disability and mortality rates. In this connection, it is necessary to introduce a federal register and to change recording forms for patients with viral hepatitides. Standard interferon, pegylated interferon alpha 2a and pegylated alpha 2b, and the HCV protease inhibitors telaprevir, boceprevir, and simeprevir have been registered for the treatment of hepatitis C in the Russian Federation.

Published

2014

6. Hepatitis C virus Genotype 3: that 'simple', yet that 'complex'

Author

S N Batskikh, S V Morozov, V P Chulanov, and V I Pokrovskiĭ

Subjects

hepatitis c virus, genotype, chronic hepatitis c, viral load, hepatic fibrosis, hepatic steatosis, il-28b, antiviral treatment, interferon-α, ribavirin, Medicine

Abstract

The data on natural course of chronic viral hepatitis C infection (HCV) and the efficacy of antiviral treatment depending on virus genotype are summarized in the article. The significance of virus genotype in progression of liver febrosis and liver steatosis is discussed. It is pointed out that chronic HCV infection caused by genotype 3 is characterized by a more aggressive clinical course of disease and less favorable prognosis. Optimal approaches to the management of patients with genotype 3 of chronic HCV infection as well as perspectives of antiviral therapy in this group of patients are discussed in the article.

Published

2012

7. REAL-TIME ELASTOGRAPHY AND ITS CLINICAL APPLICATION COMPARED WITH OTHER METHODS FOR EVALUATION OF THE LIVER FIBROSIS DEGREE IN PATIENTS WITH CHRONIC HEPATITIS C

Author

E. V. Lichnaya, A. V. Dmitriev, M. A. Belopolskaya, O. D. Denisova, V. Yu. Avrutin, Alexey Yakovlev, E. Yu. Yushina, and S. I. Gurina

Subjects

0301 basic medicine, medicine.medical_specialty, Liver fibrosis, Infectious and parasitic diseases, RC109-216, Gastroenterology, apri-index, 03 medical and health sciences, 0302 clinical medicine, Fibrosis, Internal medicine, medicine, In patient, сompression elastography, Real time elastography, medicine.diagnostic_test, business.industry, medicine.disease, transient elastography, 030104 developmental biology, Infectious Diseases, Liver biopsy, chronic hepatitis c, 030211 gastroenterology & hepatology, Elastography, business, Hepatic fibrosis, Transient elastography

Abstract

In this work we investigated to which extent the evaluation results of the degree of hepatic fibrosis obtained by realtime elastography (RTE) method are compatible with the results of the transient elastography (TE) and with the APRI indexes. We also analyzed the factors which can influence the reliability of the fibrosis degree evaluation obtained by different methods.Materials and methods. The study included 99 patients (60 women and 39 men) with HCV, examined in the polyclinic department of the Saint-Petersburg Botkin clinical infectious hospital in 2017. In 83 patients, the fibrosis degree in the liver tissue has been evaluated by the RTE method using HI VISION Preirus (Hitachi, Japan) with a linear sensor. In 67 patients, the evaluation has been performed by the TE method using Fibroscan (Echosens, France). Both methods have been applied to 51 patients.Conclusions. The aplication results of the RTE and TE methods do not differ significantly for patients with a severe fibrosis. Usually, the degree of fibrosis in patients with CHC obtained by the RTE is higher than the one obtained by the TE in the same patient. Due to the possibility to visualize a larger area under study, the RTE method has clear advantages in evaluating the degree of fibrosis in liver tissue in patients with focal changes in the liver. If the results obtained by the RTE and TE methods differ significantly, alternative methods must be used, such as a liver biopsy and biochemical methods.

Published

2018

8. Dna damage in lymphocytes in chronic viral hepatitis B, C

Author

N. S Ivanova, A.F. Popov, A. O Mikhailov, and A.I. Simakova

Subjects

Hepatitis, medicine.medical_specialty, business.industry, DNA damage, Infectious and parasitic diseases, RC109-216, Hepatitis B, medicine.disease, Gastroenterology, digestive system diseases, Comet assay, Infectious Diseases, Blood serum, Fibrosis, comet assay, Internal medicine, medicine, DNA fragmentation, oxidative stress, hepatitis, dna damage, business, Hepatic fibrosis, chirrosis

Abstract

Objective: determine grade of DNA damage in lymphocytes and the levels of 8-hydroxy-2-deoxyguanosine (8- OHdG) and 8-nitroguanine (8-NO2G), total antioxidant activity (TAA) in the blood serum of patients with chronic viral hepatitis C (HCV), B (HBV). Materials and methods. The study included 100 people with HCV, 50 with HBV and 43 volunteers. DNA damage was evaluated by comet assay. Level 8-NO2G and 8-OHdG were determined in serum samples using ELISA kits. TAA determined according to the standard ABTS method. All statisticalcalculations were performed and the graphs were plotted using STATISTICA 10.0 software. Results. There was a tendency to increase the level of DNA damage with progression of the liver fibrosis stage in HCV and HBV. Significant differences from the norm of 8-NO2G in the F1, F2, F3 groups with HCV and in the groups F2, F3, F4 (ρ

Published

2017

9. A histological response to antiviral therapy for chronic hepatitis C in patients who failed to achieve a sustained virological response

Author

A M Riumin and O V Korochkina

Subjects

chronic hepatitis c, antiviral therapy, histological response, sustained virological response, hepatic fibrosis, Medicine

Abstract

The paper presents the results of combination antiviral therapy (AVT) in 2 patients with chronic hepatitis C (CHC) unresponsive to AVT. Both patients are classified as difficult to treat (genotype 1b, a high viral load, overweight). 1.5 years after the termination of a course of AVT, histological examination of biopsy specimens revealed a histological response in one patient and significant histological worsening in the other. The specific features of the development of a histological response to AVT and possible reasons for its lack are discussed by the example of the described patients.

Published

2012

10. Патоморфологія фіброзу печінки в трепанобіоптатах хворих на стеатогепатит: основні типи, джерела розвитку, особливості прогресування

Author

V. A. Tumanskiy and S. V. Fen

Subjects

0301 basic medicine, Pathology, medicine.medical_specialty, Cirrhosis, liver cirrhosis, steatohepatitis, 03 medical and health sciences, 0302 clinical medicine, Immunophenotyping, hepatic stellate cells, fibroblasts, biopsy, Fibrosis, стеатогепатит, звёздчатые клетки, фибробласты, цирроз печени, биопсия, medicine, lcsh:Pathology, business.industry, medicine.disease, 030104 developmental biology, medicine.anatomical_structure, Hepatocyte, Hepatic stellate cell, 030211 gastroenterology & hepatology, Steatosis, Hepatic fibrosis, business, зірчасті клітини, фібробласти, цироз печінки, біопсія, Myofibroblast, lcsh:RB1-214

Abstract

До последнего времени среди патологов, гепатологов и гастроэнтерологов продолжается дискуссия по морфогенезу и градации фиброза печени у больных неалкогольным (НАСГ) и алкогольным стеатогепатитом (АСГ).Цель работы – изучить основные типы и источники фиброза печени у больных неалкогольным и алкогольным стеатогепатитом, обосновать градацию степени его тяжести с учетом количественной динамики фиброгенных клеток-продуцентов, относительной площади фиброза и депонирования коллагена I, III и IV типа в печени.Материалы и методы. Гистологическое и гистохимическое исследование фиброза печени проведено у 198 больных НАСГ 18–79 лет и у 79 больных АСГ 47–63 лет. Иммуногистохимическое исследование с измерением площади экспрессии активированных αSMA+ перисинусоидальных звёздчатых клеток и αSMA+ портальных миофибробластов при F1 (легком), F2 (умеренном), F3 (тяжелом) фиброзе и F4 фиброзе/циррозе печени проведено в 80 трепанобиоптатах больных НАСГ (по 20 случаев в каждой группе), электронно-микроскопическое исследование печени – у 10 умерших больных, страдавших НАСГ.Результаты. У больных НАСГ и АСГ прогрессируют два основных типа фиброза печени: перисинусоидально-перицеллюлярный и портально-Z3 перисинусоидальный фиброз, источником развития которых являются новые поколения αSMA+ звездчатых клеток и αSMA+ портальных миофибробластов фиброгенного иммунофенотипа, с коэкспрессией ними фасцина, виментина и отсутствием экспрессии десмина. По мере прогрессирования перисинусоидально-перицеллюлярного фиброза от легкой F1 степени к тяжелому F3 фиброзу и к крайне тяжелому F4 фиброзу/циррозу перицеллюлярного типа в печени достоверно возрастает площадь Массон-позитивного внеклеточного молекулярно-волокнистого матрикса (Н = 88,70 р = 0,05) и площадь αSMA+ коллаген-продуцирующих звездчатых клеток перисинусоидально-перицеллюлярной локализации (Н = 45,12; р = 0,05). По данным фотоцифровой морфометрии, при возрастании степени тяжести портально-Z3перисинусоидального фиброза печени от F1 к F4 в зонах фиброза достоверно возрастает площадь Массон-позитивного внеклеточного молекулярно-волокнистого матрикса (Н = 76,56 р = 0,05), а также площадь активированных αSMA+ коллаген-продуцирующих портальных миофибробластов и перисинусоидальных звездчатых клеток Z3 зон печеночных долек (Н = 43,18; р = 0,05). Активация и увеличения числа CD-68+ макрофагов в очагах интенсивного стеатоза гепатоцитов, а также появление S100 (А4)+ макрофагов, которые активируют звездчатые клетки, дает основание предполагать, что феномен перицеллюлярности фиброза печени при НАСГ и АСГ обусловлен экзосомальным привлечением макрофагов в зоны баллонного стеатонекроза и некроптоза гепатоцитов, а также локальной экзосомально-цитокиновой активацией перисинусоидальных звездчатых клеток фиброгенного типа.Выводы. По мере прогрессии фиброза от F1 до F4 степени в печени достоверно увеличивается площадь активированных αSMA+ фибробластов, а также площадь депонирования коллагена I, III и IV типа перисинусоидально-перицеллюлярной или портально-Z3перисинусоидальной локализации., Until recently, among the pathologists, hepatologists and gastroenterologists, a discussion continues on the morphogenesis and gradation of liver fibrosis in non-alcoholic patients (NASH) and alcoholic steatohepatitis (ASH).Purpose of the study. Studying the main types and sources of liver fibrosis in patients with nonalcoholic and alcoholic steatohepatitis, justifying the gradation of its severity, taking into account the quantitative dynamics of fibrogenic producer cells, the relative area of fibrosis and the deposition of type I, III and IV collagen in the liver.Material and methods. Histological and histochemical examination of liver fibrosis was performed in 198 patients with NASH of 18-79 years and in 79 patients with ASH of 47-63 years. Immunohistochemical study with measurement of the area of expression of activated αSMA + perisinusoidal stellate cells and αSMA + portal myofibroblasts with F1 (mild), F2 (moderate), F3 (severe) fibrosis and F4 fibrosis / cirrhosis was performed in 80 trepanobioptates of patients with NASH (20 cases in each group), electron microscopic examination of the liver – in 10 deceased patients suffering from NASH.Results. In patients with NASH and ASH, there are two major types of liver fibrosis progress: the perisinusoidal pericellular and portal-Z3 perisinusoidal fibrosis, the development of which is the new generation of αSMA + star cells and αSMA + portal myofibroblasts of the fibrogenic immunophenotype, with co-expression of fascin and vimentin and absence of desmine expression. As the perisinusoidal pericellular fibrosis progresses from the mild F1 degree, to the severe F3 fibrosis and to the extremely severe F4 fibrosis / cirrhosis of the pericellular type, the area of the Masson-positive extracellular molecular-fibrous matrix (H = 88,70 р = 0,05 ) and the area of αSMA + collagen-producing stellate cells of perisinusoidal-pericellular localization (H = 45,12, p = 0,05). According to the data of photometric morphometry, with increasing severity of portal-Z3 perisinusoidal hepatic fibrosis from F1 to F4, the area of the Masson-positive extracellular molecular-fibrous matrix (N = 76,56 p = 0,05) in areas fibrofacitiously increases, as well as the area of activated αSMA + collagen-producing portal myofibroblasts and perisinusoid stellate cells of Z3 zones of hepatic lobules (H = 43,18, p = 0,05). Activation and increase in the number of CD-68+ macrophages in the centers of intensive hepatocyte steatosis, as well as the appearance of S100 (A4)+ macrophages that activate stellate cells, suggests that the phenomenon of pericellularity of liver fibrosis in NASH and ASH is due to exosomal macrophage involvement in zone of balloon steatonecrosis and necroptosis of hepatocytes, as well as local exosomal-cytokine activation of perisinusoid stellate cells of fibrogenic type.Conclusion: As the progression of fibrosis from F1 to F4 degree in the liver the area of activated αSMA + fibroblasts, and the area of deposition of collagen I, III and IV type perisinusoidal pericellular or portal-Z3 perisinusoidal localization significantly increase., До останнього часу серед патологів, гепатологів і гастроентерологів триває дискусія щодо морфогенезу та градації фіброзу печінки у хворих на неалкогольний (НАСГ) та алкогольний стеатогепатит (АСГ).Мета роботи – вивчити основні типи та джерела фіброзу печінки у хворих на неалкогольний та алкогольний стеатогепатит, обґрунтувати градацію ступеня його тяжкості з урахуванням кількісної динаміки фіброгенних клітин-продуцентів, відносної площі фіброзу та депонування колагену I, III та IV типу в печінці.Матеріали та методи. Гістологічне та гістохімічне дослідження фіброзу печінки здійснили у 198 хворих на НАСГ віком 18–79 років та у 79 хворих на АСГ віком 47–63 років. Імуногістохімічне дослідження з вимірюванням площі експресії активованих αSMA+ перисинусоїдальних зірчастих клітин та αSMA+ портальних міофібробластів при F1 (легкому), F2 (помірному), F3 (важкому) фіброзі та F4 фіброзі/цирозі печінки здійснили у 80 трепанобіоптатах хворих на НАСГ (по 20 випадків у кожній групі), електронно-мікроскопічне дослідження печінки – в 10 померлих хворих, які страждали на НАСГ.Результати. У хворих на НАСГ та АСГ прогресують два основні типи фіброзу печінки: перисинусоїдально-перицелюлярний і портально-Z3перисинусоїдальний фіброз, джерелом розвитку яких є нові покоління αSMA+ зірчастих клітин та αSMA+ портальних міофібробластів фіброгенного імунофенотипу з коекспресією ними фасцина, віментина та відсутністю експресії десмину. З прогресуванням перисинусоїдально-перицелюлярного фіброзу від легкого F1 ступеня до важкого F3 фіброзу та до вкрай важкого F4 фіброзу/цирозу перицелюлярного типу в печінці вірогідно зростає площа Массон-позитивного позаклітинного молекулярно-волокнистого матриксу (Н = 88,70 р = 0,05) і площа αSMA+ колаген-продукуючих зірчастих клітин перисинусоїдально-перицелюлярної локалізації (Н = 45,12; р = 0,05). За даними фотоцифрової морфометрії, при зростанні ступеня тяжкості портально-Z3перисинусоїдального фіброзу печінки від F1 до F4 в зонах фіброзу вірогідно зростає площа Массон-позитивного позаклітинного молекулярно-волокнистого матриксу (Н = 76,56; р = 0,05), а також площа активованих αSMA+ колаген-продукуючих портальних міофібробластів і перисинусоїдальних зірчастих клітин Z3 зон печінкових дольок (Н = 43,18; р = 0,05). Активація та збільшення числа CD-68+ макрофагів у вогнищах інтенсивного стеатоза гепатоцитів, а також поява S100 (А4)+ макрофагів, що активують зірчасті клітини, дає підставу припускати: феномен перицелюлярного фіброзу печінки при НАСГ та АСГ зумовлений екзосомальним залученням макрофагів до зон балонного стеатонекрозу та некроптозу гепатоцитів, а також локальною екзосомально-цитокіновою активацією перисинусоїдальних зірчастих клітин фіброгенного типу.Висновки. З прогресією фіброзу від F1 до F4 ступеня в печінці вірогідно збільшується площа активованих αSMA+ фібробластів, а також площа депонування колагену I, III та IV типу перисинусоїдально-перицелюлярної або портально-Z3перисинусоїдальної локалізації.

Published

2017

11. [Protective effects of S-adenosylmethionine against CCl4 - and ethanol-induced experimental hepatic fibrosis].

Author

Zhang F, Gu JX, Zou XP, and Zhuge YZ

Subjects

Alanine Transaminase metabolism, Animals, Carbon Tetrachloride toxicity, Disease Models, Animal, Ethanol toxicity, Gene Expression drug effects, Liver pathology, Liver Cirrhosis chemically induced, Liver Cirrhosis pathology, Rats, Liver drug effects, Liver Cirrhosis drug therapy, Protective Agents administration & dosage, S-Adenosylmethionine administration & dosage, Smad3 Protein biosynthesis

Abstract

In this study the effects of S-adenosylmethionine (SAM) on experimental hepatic fibrotic rats induced by carbon tetrachloride (CCl(4)) and ethanol and the relevant potential mechanisms were explored. Hepatic fibrotic rat models were established with CCl(4) diluted in olive oil being drunk with 10% ethanol in water. SAM was used both for prevention and treatment. Histological evaluation was carried out by hematoxylin-eosin (HE) and Masson staining of hepatic samples. Serum biochemical assays showed that alanine aminotransferase (ALT) was increased and albumin (ALB) was decreased by CCl(4) and ethanol, and both effects were suppressed by preventing and treating use of SAM. The model control rats got significantly higher scores in fatty degeneration, lobular inflammation, and hepatocyte ballooning. A significant improvement was observed in the SAM-prevented rats and SAM-treated rats, which was consistent with the change of fibrosis scoring in each group. Smad3 was induced by CCl(4) and ethanol in the model control group, which was significantly down regulated by SAM. SAM reduced both total Smad3 and phospho-Smad3 in vitro. SAM had a protective effect on hepatic fibrosis in rats induced by CCl(4) combined with ethanol and the down-regulation of activity and expression of Smad3 were involved in the potential mechanisms.

Published

2016