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1. Immunosuppressive drugs affect interferon (IFN)-γ and programmed cell death 1 (PD-1) kinetics in patients with newly diagnosed autoimmune hepatitis.

Author

Grant, C. R., Holder, B. S., Liberal, R., Heneghan, M. A., Ma, Y., Mieli‐Vergani, G., Vergani, D., and Longhi, M. S.

Subjects
CHRONIC active hepatitis, IMMUNOSUPPRESSIVE agents, TUMOR necrosis factors, INTERFERON gamma, INTERLEUKIN-17, APOPTOSIS, CYTOKINES, DIAGNOSIS
Abstract

Autoimmune hepatitis (AIH) is characterized by overwhelming effector immune responses associated with defective regulatory T cells (Tregs). Several lines of evidence indicate CD4 as the main effectors involved in autoimmune liver damage. Herein we investigate the in-vitro effects of prednisolone, 6-mercaptopurine, cyclosporin, tacrolimus, mycophenolic acid (MPA) and rapamycin, immunosuppressive drugs (ISDs) used in AIH treatment, on the expression of proinflammatory cytokines, co-inhibitory molecules and ability to proliferate of CD4+CD25- cells, isolated from the peripheral blood of treatment-naive patients with AIH. We note that in healthy subjects (HS) following polyclonal stimulation and in the absence of ISDs, the expression of interferon (IFN)-γ, interleukin (IL)-17 and tumour necrosis factor (TNF)-α by CD4 effectors peaks at 48 h and decreases at 96 h to reach baseline levels. In contrast, in AIH the expression of all these proinflammatory cytokines continue rising between 48 and 96 h. Levels of programmed cell death-1 (PD-1), T cell immunoglobulin and mucin domain-containing molecule-3 (TIM-3) and cytotoxic T lymphocyte antigen-4 (CTLA-4) increase over 96-h culture both in HS and AIH, although with faster kinetics in the latter. Exposure to ISDs contains IFN-γ and PD-1 expression in AIH, where control over CD4+CD25- cell proliferation is also noted upon exposure to MPA. Treatment with tacrolimus and cyclosporin render CD4+CD25- cells more susceptible to Treg control. Collectively, our data indicate that in treatment-naive patients with AIH, all ISDs restrain T helper type 1 (Th1) cells and modulate PD-1 expression. Furthermore, they suggest that tacrolimus and cyclosporin may ameliorate effector cell responsiveness to Tregs. [ABSTRACT FROM AUTHOR]

Published
2017
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3. HBs Ag plasma level kinetics: a new role for an old marker as a therapy response predictor in vertically infected children on combination therapy.

Author

Carey, I., Bruce, M., Horner, M., Zen, Y., D'Antiga, L., Bansal, S., Vergani, D., and Mieli‐Vergani, G.

Subjects
VIRAL diseases in children, CHRONIC diseases in children, HEPATITIS associated antigen, CELLULAR therapy, BIOMARKERS, CHRONIC hepatitis B, LAMIVUDINE, THERAPEUTICS
Abstract

We aimed to investigate the ability of HBsAg plasma level kinetics to predict therapy response by studying 23 children with infancy-acquired chronic hepatitis B ( CHB) during combination sequential therapy with lead-in lamivudine ( LAM) and add-on interferon-α ( IFN-α) [5 responders ( R = anti- HBs seroconversion) and 18 nonresponders ( NR)] and to assess their relationship with pretreatment intrahepatic HBV- DNA and ccc DNA and HBs Ag and HBc Ag liver expression. Plasma HBs Ag levels were measured in samples before (treatment week 0 = TW0), during ( TW9, TW28, TW52) and after (follow-up week = FUW24) therapy by Abbott ARCHITECT® assay [log10 IU/ mL]. Baseline liver HBV- DNA and ccc DNA were quantified by real-time Taq Man PCR [log10copies/ng genomic DNA]. HBs Ag and HBc Ag liver expression was evaluated by immunostaining of formalin-fixed, paraffin-embedded specimens [number of positive cells/1000 hepatocytes]. All results are presented as medians. Plasma: at baseline, on-treatment and during follow-up, HBsAg levels were lower in R than NR ( TW0: 4.36 vs 4.75; TW28: 2.44 vs 4.35; TW52: 0 vs 4.08 and FUW24: 0.17 vs 4.35, all P < 0.05). Liver: baseline HBV- DNA (3.82 vs 4.71, P = 0.16) and ccc DNA (1.98 vs 2.26, P = 0.18) tended to be lower in R than NR, HBs Ag expression was lower in R than NR (0.5 vs 4.7, P = 0.03), and HBc Ag expression was similar between R and NR. There were positive correlations between plasma HBs Ag levels and liver HBV- DNA ( r = 0.44, P = 0.04), ccc DNA ( r = 0.41, P = 0.04) and HBs Ag liver expression ( r = 0.38, P = 0.05). Lower baseline HBs Ag plasma levels, lower HBs Ag expression in liver and on-treatment decline of plasma HBs Ag levels heralds HBs Ag clearance and response to treatment in tolerant children with CHB. [ABSTRACT FROM AUTHOR]

Published
2015
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4. Treatment of chronic viral hepatitis C in children and adolescents: UK experience.

Author

Abdel-Hady, M., Bansal, S., Davison, S. M., Brown, M., Tizzard, S. A., Mulla, S., Barnes, E., Davies, P., Mieli-Vergani, G., and Kelly, D. A.

Subjects
HEPATITIS C treatment, JUVENILE diseases, DISEASES in teenagers, THERAPEUTIC use of interferons, RIBAVIRIN, DRUG efficacy
Abstract

Aim: To review the efficacy and tolerability of pegylated interferon-a and ribavirin for treatment of chronic hepatitis C (CHC) in children in the UK. Methods: Retrospective review of children treated for CHC in 3 UK paediatric specialist liver centres between 2005 and 2010. Data on viral response to treatment, demographic and clinical details were collected. Treatment outcome was assessed by the absence of detectable viral RNA in blood 24 weeks after treatment --sustained viral response (SVR). Results: 75 children were included; 34 genotype 1; 39 genotypes 2 and 3; 2 genotype 4. Overall SVR was achieved in 54/71 (76%); 65% genotype 1; 89% genotypes 2 and 3; 100% genotype 4. Early response at 12 weeks was achieved in 53 and sustained in 47 (89%). Data on rapid response after 4 weeks of treatment were available in 25; 17/25 (68%) responded and 16 of these (94%) achieved SVR. IL28 T/T genotype was associated with higher SVR. There were no significant changes in weight and height z scores from baseline compared with 24 weeks post-treatment followup. No child discontinued treatment due to side effects, although 43 required dose modification. Treatment affected quality of life (QoL) in the initial 12 weeks of treatment, which improved by the end of treatment. Conclusions: Children respond well to therapy for CHC. Treatment was tolerated with minimal impact on QoL and no significant effect on growth. Knowledge of viral and IL28 genotypes and early viral response is useful to plan treatment in children and provide appropriate counselling. [ABSTRACT FROM AUTHOR]

Published
2014
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11. Chronic hepatitis.

Author

Murray KF, Shah U, Mohan N, Heller S, González-Peralta RP, Kelly D, Chang MH, Mieli-Vergani G, Jara P, Fujisawa T, and Chronic Hepatitis Working Group

Published
2008

12. Living related liver transplantation in children.

Author

Heaton, N., Faraj, W., Vilca Melendez, H., Jassem, W., Muiesan, P., Mieli-Vergani, G., Dhawan, A., and Rela, M.

Subjects
LIVING related donor transplantation, LIVER transplantation, LIVER surgery, ORGAN donors, PEDIATRIC surgery
Abstract

The article examines a single-center experience of left lateral segment liver transplants from living donors in children. Fifty left lateral segment living related liver transplantation (LRLT) procedures have been performed since 1993. There were no donor mortality and low morbidity at a median follow-up of 86 months. The study suggests that LRLT has good long-term results in children.

Published
2008
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13. Perinatal hepatitis C virus infection: diagnosis and management.

Author

Davison, S. M., Mieli-Vergani, G., Sira, J., and Kelly, D. A.

Subjects
NEONATAL hepatitis, VIRAL hepatitis, HEPATITIS C virus, LIVER diseases, COMORBIDITY, DRUG therapy, CHILDREN'S health, HEPATITIS in children
Abstract

Hepatitis C virus (HCV) infection in children is becoming an increasing challenge to health professionals. As our understanding of the disease evolves, so must our diagnostic and management strategies. In the 1990s, when HCY testing became available, children identified with HCV infection in the UK were mostly those who had required blood products, particularly those with haematological disorders. Acquiring knowledge of the natural history of HCV infection was confounded by the comorbidity of iron overload, viral co-infection, and chemotherapy. [ABSTRACT FROM AUTHOR]

Published
2006
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16. Mimicry between the hepatitis C virus polyprotein and antigenic targets of nuclear and smooth muscle antibodies in chronic hepatitis C virus infection.

Author

Gregorio, G.V., Choudhuri, K., Ma, Y., Pensati, P., Iorio, R., Grant, P., Garson, J., Bogdanos, D.P., Vegnente, A., Mieli-Vergani, G., and Vergani, D.

Subjects
HEPATITIS C virus, ANTIGENS, PEPTIDES, SMOOTH muscle
Abstract

SUMMARY Autoantibodies to smooth muscle (SMA) and nuclear components (ANA) arise in the natural course of chronic infection with hepatitis C virus. In view of the growing evidence for ‘molecular mimicry’ as a mechanism of autoimmunity we investigated whether cross-reactive immune reactions between host smooth muscle/nuclear components and HCV antigens may contribute to the formation of SMA and ANA in chronic HCV infection. Computer-assisted protein database search methods were used to identify three smooth muscle (smoothelin[sub 698-717] , myosin[sub 1035-1054] , vimentin[sub 69-88] ) and three nuclear (matrin[sub 722-741] , histone H2A[sub 11-30] , replication protein A[sub 133-152] ) host antigens with the highest local sequence similarity to the HCV polyprotein and 20-mer peptides corresponding to these regions were constructed. Sera from 51 children with chronic HCV infection [median age: 8 (2–16); 27 boys], 26 SMA positive and five ANA positive, were tested for reactivity to the synthesized HCV peptides and their human homologues by enzyme linked immunosorbent assay (ELISA). Sera from patients with HBV infection and chronic liver disease of different aetiologies were used as controls. ‘Double reactivity’ to HCV peptides and smooth muscle/nuclear homologues was associated strongly with HCV infection (P < 0·001 for both). Humoral cross-reactivity was established as the basis for double recognition by competition ELISA. Double-reactivity to smooth muscle and HCV peptide antigens correlated with SMA positivity by indirect immunofluouresence (P = 0·05). Of 15 patients double-reactive to myosin[sub 1035-1054] and its HCV homologue, 13 recognized whole myosin by immunoblot. These results suggest that ANA and SMA in chronic HCV infection may arise, at least in part, as a consequence of cross-reactive immune responses to HCV and host smooth muscle/nuclear antigens. [ABSTRACT FROM AUTHOR]

Published
2003
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18. Intestinal absorption of mixed micellar phylloquinone (vitamin K[sub 1]) is unreliable in infants with conjugated hyperbilirubinaemia: Implications for oral prophylaxis of vitamin K deficiency bleeding.

Author

Pereira, S.P., Shearer, M.J., Williams, R., and Mieli-Vergani, G.

Subjects
VITAMIN K, VITAMIN deficiency, PEDIATRICS
Abstract

Objective: To compare the pharmacokinetics and efficacy of oral versus intravenous mixed micellar vitamin K prophylaxis in infants with cholestatic liver disease, a known risk factor for vitamin K deficiency bleeding. Design: Prospective randomised controlled study. Setting: Paediatric Liver Unit. Patients: Forty four infants less than 6 months of age with conjugated hyperbilirubinaemia. Main outcome measures: Serum concentrations of vitamin K, and undercarboxylated prothrombin (PIVKA-II; a sensitive functional indicator of vitamin K status) before and for up to four days after a single dose of mixed micellar K[sub 1] 1 mg intravenously or 2 mg orally. Comparison of K[sub 1] levels 24 hours after oral K[sub 1] with those from 14 healthy newborns given the same dose. Results: At admission, 18 infants (41%) had elevated levels of serum PIVKA-II and eight (18%) had Iow K, concentrations, indicative of subclinical vitamin K deficiency. Median serum K[sub 1] concentrations were similar in the oral and intravenous groups at baseline (0.92 v 1.15 ng/ml), rising to 139 ng/ml six hours after intravenous K[sub 1] but to only 1.4 ng/ml after oral administration. In the latter group, the Iow median value (0.95 ng/ml) and wide range (< 0.15-111 ng/ml) of serum K[sub 1] compared unfavourably with the much higher levels (median 77, range 11-263 ng/ml) observed in healthy infants given the same oral dose, and suggested impaired and erratic intestinal absorption in cholestatic infants. The severity of malabsorption was such that only 4/24 (17%) achieved an incremental rise in serum K[sub 1] > 10 ng/ml. Conclusions: The intestinal absorption of mixed micellar K[sub 1] is unreliable in infants with conjugated hyperbilirubinaemia. Given the strong association between cholestasis and late vitamin K deficiency bleeding, these data provide an explanation for the failure of some oral vitamin K[sub 1] prophylaxis regimens in infants with latent cholestasis. [ABSTRACT FROM AUTHOR]

Published
2003
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19. Detection of liver kidney microsomal type 1 antibody using moleclarly based immunoassays.

Author

Kerkar, N., Ma, Y., Davies, E.T., Cheeseman, P., Mieli-Vergani, G., and Vergani, D.

Subjects
LIVER diseases, KIDNEY diseases, IMMUNOGLOBULINS
Abstract

Aims: To assess the diagnostic value of two commercial molecularly based immunoassays detecting liver kidney microsomal type 1 antibody (LKM1). Methods: The performance of Varelisa and LKM1 enzyme linked immunosorbent assay (ELISA) was compared with immunofluorescence, and two validated research techniques-an in house ELISA and a radioligand assay measuring antibodies to P4502D6. Thirty serum samples from three patients with autoimmune hepatitis type 2 covering immunofluorescence titres of 1/10 to 1/10 240 and 55 LKM1 negative controls were tested. Results: All 30 sera that were LKM1 positive by immunofluorescence were positive by the in house ELISA, the radioligand assay, and LKM1-ELISA, and 29 were also positive by Varelisa. None of the 55 sera negative for LKM1 by immunofluorescence was positive by the in house ELISA and radioligand assay, but one was positive by Varelisa and 14 were positive using the LKM1-ELISA. Agreement between immunofluorescence, the in house ELISA, the radioligand assay, and Varelisa was high (κ > 0.8), and agreement between immunofluorescence and LKM1-ELISA was moderate (κ = 0.63). Conclusion: The assay kit marketed as Varelisa allows accurate detection of LKM1. [ABSTRACT FROM AUTHOR]

Published
2002
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20. Mutations in the sterol 27-hydoxylase gene ( CYP27A) cause hepatitis of infancy as well as cerebrotendinous xanthomatosis.

Author

Clayton, P., Verrips, A., Sistermans, E., Mann, A., Mieli-Vergani, G., and Wevers, R.

Abstract

Follow-up investigations were undertaken on a previously reported patient who had severe familial giant cell hepatitis in infancy associated with substantially increased urinary excretion of bile alcohol glucuronides. By the age of 11 years, he had developed a profile of cholanoids in plasma and urine that closely resembled the pattern seen in cerebrotendinous xanthomatosis (CTX). Sequencing of the sterol 27-hydroxylase gene ( CYP27A) showed that he was homozygous for a deletion (525/526delG) that causes a frameshift and a premature stop codon. This genotype has previously been described in an adult female with classical symptoms of CTX (tendon xanthomata, cataracts and deteriorating cognitive function). A review of past medical histories of a group of patients with CTX revealed that prolonged neonatal cholestatic jaundice was common. The family histories also revealed fetal and neonatal deaths among siblings of patients with CTX. We conclude that defective activity of cholesterol 27-hydroxylase can lead to neonatal cholestatic jaundice ('hepatitis of infancy'), which may be self-limiting. After a latent period, however, progressive accumulation of cholesterol and cholestanol can lead to the xanthomata, neurodegeneration, cataracts and atherosclerosis that are typical of CTX. [ABSTRACT FROM AUTHOR]

Published
2002
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21. Intestinal Permeability and Absorptive Capacity in Children with Portal Hypertension.

Author

Taylor, R. M., Bjarnason, I., Cheeseman, P., Davenport, M., Baker, A. J., Mieli-Vergani, G., and Dhawan, A.

Subjects
PORTAL hypertension, LIVER diseases, MALNUTRITION in children
Abstract

Background: Portal hypertension may affect intestinal function leading to malnutrition in children with liver disease. The aim was to determine whether children with portal hypertension with or without liver disease had impaired absorptive capacity and intestinal barrier function (intestinal permeability) and to ascertain whether these abnormalities related to changes in body composition. Methods: Twenty-six children with portal hypertension were divided according to aetiology into: Group 1 intrahepatic (n = 15) and Group 2 prehepatic (n = 11). Thirty-five children acted as controls. Carbohydrate absorption and intestinal permeability were assessed using a sugar absorption/permeability test and a variety of anthropometric measurements were obtained. Results: 3-O-methyl-D-glucose, D-xylose and L-rhamnose excretion were significantly reduced in both patient groups compared to controls (P ≤ 0.008) and the differential urinary excretion of melibiose/rhamnose (intestinal permeability) was significantly increased in Group 1 only (P < 0.05). Anthropometric measurements showed low Z scores in both groups, but there was no significant (P > 0.05) difference between them. There was no significant correlation between urinary excretion of sugars, anthropometric measurements and energy intake. Conclusions: Increased portal pressure reduces the absorptive capacity of the small intestine, while liver disease itself leads to increased intestinal permeability. [ABSTRACT FROM AUTHOR]

Published
2002
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22. Serum hyaluronic acid concentrations are increased in cystic fibrosis patients with liver disease.

Author

Wyatt, H. A., Dhawan, A., Cheeseman, P., Mieli-Vergani, G., and Price, J. F.

Subjects
CYSTIC fibrosis, HYALURONIC acid, LIVER diseases, SERUM, PULMONARY function tests, PATIENTS
Abstract

Aim: To determine whether serum hyaluronic acid (HA) concentrations are abnormal in patients with cystic fibrosis (CF) liver disease, and if so, whether the abnormality is associated with disease severity. Methods: A total of 74 patients with CF were assessed for evidence of liver involvement as indicated by clinical, ultrasound, and biochemical findings. Serum hyaluronic acid concentrations were measured and compared with concentrations in 293 normal controls. Lung function in the CF patients was also recorded. Results: Thirty four CF patients had no evidence of liver disease; in these, serum HA concentrations were similar to those in healthy controls (median (range): 16.1 (9.4-75.1) v 15(1-77) μg/I). Nineteen CF patients had established liver disease detected by clinical and ultrasound examination, with significantly increased HA concentrations (56.1 (26-355) μg/I). Serum HA concentrations were also significantly increased, although to a lesser extent, in 21 CF patients with an abnormal liver ultrasound scan alone (22.4 (9.5-43.4) μg/I). There was no correlation between serum HA concentration and lung function. Conclusion: Serum HA concentrations were significantly increased in children with clinical or ultrasound evidence of liver disease, being higher in those with more advanced hepatic damage. Despite the inflammation and fibrosis present in CF lungs there was no correlation between HA concentration and lung function, suggesting that high concentrations were a failure of hepatic clearance rather than overproduction in the lung. Longitudinal measurement of HA concentrations may prove a useful marker for the development of significant liver damage in CF patients. [ABSTRACT FROM AUTHOR]

Published
2002
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24. Autoantibodies to human cytosol: a marker of sporadic porphyria cutanea tarda.

Author

Ma, Y., Fracanzani, A. L., Sampietro, M., Mattioli, M., Cheeseman, P., Williams, R., Mieli-Vergani, G., Vergani, D., and Fargion, S.

Subjects
IMMUNOGLOBULINS, CYTOSOL
Abstract

The enzymes potentially involved in the pathogenesis of sporadic porphyria cutanea tarda (PCT) reside in liver cytosoles and microsomes. PCT is frequently associated with hepatitis C virus (HCV) infection, which is in turn associated with autoimmune manifestations. To investigate whether autoimmune reactions, possibly triggered by HCV, are involved in the pathogenesis of PCT, we measured by immunoblot autoantibodies to human cytosolic and microsomal liver fractions in 82 patients with PCT (77% with HCV infection), 105 with other liver disorders and 40 healthy subjects. Anti-liver cytosolic antibodies were more frequent in PCT patients (38/82, 46%) than in pathological controls (P < 0·05–P < 0·001) or in healthy subjects (3/40, 8%, P < 0·001). Among PCT patients, anticytosolic antibodies were more frequent in HCV positive (36/63, 57%) than in HCV negative (2/19, 11%, P < 0·05) cases. Reactivity to a 40-kDa cytosolic polypeptide was present in 20 PCT patients (19 HCV positive), being more frequent than in all pathological controls (P < 0·01–P < 0·0001). Histological activity index (P = 0·04) and antibodies to HCV (P = 0·027) – but not HCV RNA – were associated independently with anticytosolic antibodies as assessed by multivariate analysis. In contrast, frequency of antiliver microsomal antibodies was similar in PCT patients (24/82, 29%) and pathological controls (8–26%), being higher in the autoimmune hepatitis control group (23/23, 100%, P < 0·0001). In conclusion, anticytosolic antibodies, particularly to a 40-kDa polypeptide, are frequent in PCT and associated with HCV infection and severity of liver damage. [ABSTRACT FROM AUTHOR]

Published
2001
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25. Bone marrow failure in children with acute liver failure.

Author

Tung, John, Hadzic, Nedim, Layton, Mark, Baker, Alastair J., Dhawan, Anil, Rela, Mohamed, Heaton, Nigel D., Mieli-Vergani, Giorgina, Tung, J, Hadzic, N, Layton, M, Baker, A J, Dhawan, A, Rela, M, Heaton, N D, and Mieli-Vergani, G

Published
2000

26. Active surveillance of hepatitis C infection in the UK and Ireland.

Author

Gibb, D. M., Neave, P. E., Tookey, P. A., Ramsay, M., Harris, H., Balogun, K., Goldberg, D., Mieli-Vergani, G., and Kelly, D.

Abstract

Aim: To investigate the prevalence, distribution, and clinical details of paediatric hepatitis C virus (HCV) infection in the UK and Ireland.Methods: Active monthly surveillance questionnaire study coordinated through the British Paediatric Surveillance Unit, to all consultant paediatricians in 1997 and 1998.Results: A total of 182 HCV infected children were reported from 54 centres and by paediatricians from eight different specialties. In 40 children HCV was acquired through mother to child transmission (MTC children); 142 were infected by contaminated blood products (n = 134), organ transplantation (n = 2), needles (n = 4), or unknown risk factor (n = 2). Intravenous drug use was the risk factor for 35 mothers of MTC children. Twelve children were coinfected with HIV and four with HBV. Recent serum aspartate aminotransferase or alanine aminotransferase values were at least twofold greater than the upper limit of normal in 24 of 152 children; this occurred in five of 11 HIV coinfected children. Liver histology, available in 53 children, showed normal (7%), mild (74%), moderate (17%), or severe (2%) hepatitis. Twenty eight children had received therapy with interferon alfa.Conclusion: Most current paediatric HCV infection in UK and Ireland has been acquired from contaminated blood products, and most children are asymptomatic. There is a need for multicentre trials to inform clinical practice and development of good practice guidelines in this area. Long term follow up of this cohort of HCV infected children is planned to help determine the natural history over the long term of HCV acquired during infancy and childhood. [ABSTRACT FROM AUTHOR]

Published
2000
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27. Retrospective review of cystic fibrosis presenting as infantile liver disease.

Author

Shapira, Riki, Hadžić, Nedim, Francavilla, Ruggiero, Koukulis, George, Price, John F., Mieli-Vergani, Giorgina, Shapira, R, Hadzic, N, Francavilla, R, Koukulis, G, Price, J F, and Mieli-Vergani, G

Abstract

The mode of presentation, clinical course, and outcome of 12 infants with cystic fibrosis and liver disease referred over an 18 year period were investigated retrospectively. Median age at presentation was 6.5 weeks (range, 5-12). Two thirds were boys. Conjugated hyperbilirubinaemia was the presenting symptom in 11 patients, and hypoalbuminaemia in one. Jaundice was cleared over a median period of 7.36 months. Eight patients had bile duct proliferation on liver biopsy and one required cholangiography to exclude biliary atresia. Classic histological features of cystic fibrosis were only present in two children biopsied at 8 and 18 months. Three patients had meconium ileus, including one infant with concomitant alpha(1) antitrypsin deficiency, who required early liver transplantation. All other patients had no signs of significant chronic liver disease during a median follow up of 42 months (range, 10-205). Children with cystic fibrosis and infantile liver disease have a good short and medium term prognosis. [ABSTRACT FROM AUTHOR]

Published
1999
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29. Hepatitis GB virus-C/hepatitis G virus infection in liver disease.

Author

Nagata, Ikuo, Tzampouras, Nikos, Chokshi, Shilpa, Naoumov, Nikolai V., Cheeseman, Paul, Smith, Heather M., Baker, Alastair J., Williams, Roger, Mieli-Vergani, Giorgina, Nagata, I, Tzampouras, N, Chokshi, S, Naoumov, N V, Cheeseman, P, Smith, H M, Baker, A J, Williams, R, and Mieli-Vergani, G

Abstract

Hepatitis GB virus-C (HGBV-C)/hepatitis G virus (HGV) infection was investigated in 106 children with liver disease (54 boys and 52 girls, mean age 7.3 years); 12 with chronic hepatitis C virus infection, 29 with positive hepatitis B surface antigen, nine with idiopathic fulminant hepatic failure, seven with graft dysfunction after liver transplantation associated with autoimmune features, 20 with cryptogenic liver disease, and 29 with autoimmune liver disease. HGV RNA detected by reverse transcription polymerase chain reaction was found to be positive in 4/106 patients (3.8%). Risk factors were identified in three patients, including blood transfusion and/or medical treatment in Eastern Europe. The prevalence was higher than that of blood donors but lower than that of 2 adult patients with liver disease. HGV is not associated with any specific disease group and does not seem to be a major aetiological agent of liver disease in childhood in the UK. [ABSTRACT FROM AUTHOR]

Published
1997
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31. Choledochal cysts: lessons from a 20 year experience.

Author

Stringer, M. D., Dhawan, A., Davenport, M., Mieli-Vergani, G., Mowat, A. P., and Howard, E. R.

Abstract

Cystic dilatation of the biliary tree is a rare congenital anomaly. To determine mode of presentation, diagnostic pitfalls, and long term outcome after surgery, 78 children (57 girls, 21 boys) with choledochal cyst treated between 1974 and 1994 were reviewed. Anatomical types were: Ic (n = 44), If (n = 28), IVa (n = 4), and V (n = 2); a common pancreaticobiliary channel was identified in 76% patients. Age at presentation ranged from 0-16 (median 2.2) years, six patients being diagnosed by prenatal ultrasonography. Of the 72 patients diagnosed postnatally, 50 (69%) presented with jaundice, associated with abdominal pain in 25 or a palpable mass in three, 13 (18%) presented with pain alone, and two (3%) with a palpable mass. The classic triad of jaundice, pain, and a right hypochondrial mass was present in only four (6%). Four children presented acutely after spontaneous perforation of a choledochal cyst, two presented with ascites and one cyst was discovered incidentally. Plasma and/or biliary amylase values were raised in 30 of 31 patients investigated for abdominal pain; seven had evidence of pancreatitis at operation. In 35 of 67 (52%) patients referred without previous surgery, symptoms had been present for more than one month, and in 14 of them for more than one year, before diagnosis. Delayed referral was due to misdiagnosis as hepatitis (n = 12), incomplete investigation of abdominal pain (n = 6), and failure to note the significance of ultrasonographic findings (n = 10). Two patients referred late died from liver failure. Of the 76 patients with type I or IV cysts, 59 underwent radical cyst excision and hepaticojejunostomy as a primary procedure and 10 as a secondary operation after previously unsuccessful surgery. Sixteen patients have been lost to follow up but most of the remainder are well after a mean period of 4.1 (0.1-13) years. Choledochal cysts are often misdiagnosed, but prognosis is excellent if radical excision is performed. [ABSTRACT FROM AUTHOR]

Published
1995
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33. Immunohistochemical features of the portal tract mononuclear cell infiltrate in chronic aggressive hepatitis.

Author

Senaldi, Giorgio, Portmann, Bernard, Mowat, Alex P., Mieli-Vergani, Giorgina, Vergani, Diego, Senaldi, G, Portmann, B, Mowat, A P, Mieli-Vergani, G, and Vergani, D

Abstract

The portal tract mononuclear cell infiltrate has been characterised in 28 liver biopsy samples showing features of chronic aggressive hepatitis from 12 patients with autoimmune chronic active hepatitis, 12 with primary sclerosing cholangitis, and four with other chronic liver diseases (two with alpha 1-antitrypsin deficiency, one with Wilson's disease, and one with chronic hepatitis B infection). In all patients liver disease had started in childhood. The mononuclear cell infiltrate was investigated by a two step immunoperoxidase technique using monoclonal antibodies to: total, alpha/beta T cell receptor positive, helper/inducer, suppressor/cytotoxic T lymphocytes; B lymphocytes; killer/natural killer cells; monocyte/macrophages; and to the activation markers HLA-DR antigens, interleukin 2 receptor (IL-2R), transferrin receptor, and 4F2Ag. In all samples the infiltrate consisted of mainly alpha/beta T cell receptor T lymphocytes. Although T helper/inducer cells predominated in patients with autoimmune chronic active hepatitis, T suppressor/cytotoxic lymphocytes were preponderant in patients with primary sclerosing cholangitis and the other chronic liver diseases. Killer/natural killer cells accounted for up to 25% of the mononuclear cell infiltrate in patients with autoimmune chronic active hepatitis, being rare or absent in the other diseases. Monocytes/macrophages were always found, but they were more numerous in primary sclerosing cholangitis than in the other chronic liver diseases. B lymphocytes were rare or absent in all subjects. Activated mononuclear cells were present in all subjects, but although in patients with autoimmune chronic active hepatitis and primary sclerosing cholangitis most cells of the infiltrate expressed HLA-DR antigens and up to 75% IL-2R, in other forms of chronic liver diseases HLA-DR positive cells were less common and IL-2R positive cells ere rare or absent. These results show that the cells responsible for the histological characteristics of chronic aggressive hepatitis vary in their functional phenotype and state of activation according to the type of underlying liver disorder, confirming the involvement of different pathogenetic mechanisms. [ABSTRACT FROM AUTHOR]

Published
1992
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34. Orthotopic liver transplantation reverses the adverse nutritional changes of end-stage liver disease in children.

Author

Holt RIG, Broide E, Buchanan CR, Miell JP, Baker AJ, Mowat AP, and Mieli-Vergani G

Abstract

The changes in growth and body composition after orthotopic liver transplantation (OLT) were studied in 61 children [median age at OLT 3.49 y (range: 0.04-14.5 y), 26 boys and 35 girls] who had survived 1 y post-OLT. Height, weight, midarm circumference (MAC), triceps skinfold thickness (TSF), and subscapular skinfold thickness (SSF) were measured at OLT, 3 and 6 mo later, then annually up to 5 y. SD scores (SDS) were derived from population standards. Results are reported as mean SDS +/- SEM. At OLT the children were short and malnourished (height: -0.98 +/- 0.22; weight: -0.82 +/- 0.18; MAC: -1.77 +/- 0.21; TSF: -1.27 +/- 0.17; SSF: -1.49 +/- 0.17). By 3 mo post-OLT, there was a sustained improvement in MAC (-0.73 +/- 0.22), TSF (-0.47 +/- 0.18), and SSF (-0.50 +/- 0.18). Weight SDS (-0.48 +/- 0.20) improved by 6 mo without significant change in height SDS. The three children with Alagille syndrome were smaller (height, weight, and MAC) than children with other diagnoses but did show catch-up growth. Fulminant hepatic failure was not associated with growth failure before or after OLT. Infants (n = 14) were smaller and more malnourished at OLT (smaller skinfold thicknesses and lower weight SDS) than those who received transplants at an older age. By 1 y post-OLT, the only persisting difference was in TSF. Abnormal liver function at 1 y post-OLT (n = 8) and repeated episodes of steroid-treated rejection (n = 13) were associated with worsening height and weight SDS. The use of tacrolimus for graft salvage from rejection (n = 6) was not associated with growth failure. In conclusion, end-stage liver disease has a more adverse effect on MAC, TSF, and SSF than on height and weight, but a marked and rapid improvement occurred post-OLT. Children who were most severely malnourished and growth restricted at the time of OLT showed the greatest catch-up growth after OLT. (c) 1997 American Society for Clinical Nutrition [ABSTRACT FROM AUTHOR]

Published
1997
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35. Immunoglobulin on the surface of isolated hepatocytes is associated with antibody-dependent cell-mediated cytotoxicity and liver damage.

Author

Vergani, D., Mieli-Vergani, G., Mondelli, M., Portmann, B., and Eddleston, A. L. W. F.

Abstract

ABSTRACT- Hepatocytes isolated from patients with chronic liver disease are often covered by immunoglobulin. The aim of the present study was to establish whether this surface immunoglobulin (SIg) mediates liver cell damage. Freshly isolated hepatocytes from percutaneous liver biopsy of 16 patients with chronic active hepatitis (CAH) (6 HBsAg positive), 3 with HBsAg-positive chronic lobular hepatitis (CLH), 5 with HBsAg-positive chronic persistent hepatitis (CPH) and 12 with minor histological abnormalities (MHA) (5 HBsAg positive) were divided into two aliquots. One was studied for the presence of membrane-bound immunoglobulin and the third component of complement by direct immunofluorescence and the other was incubated, in an allogeneic cytotoxic assay, with peripheral blood mononuclear cells prepared from healthy volunteers as a source of effectors for antibody-dependent cell-mediated cytotoxicity (ADCC). Liver biopsies were scored for portal and parenchymal inflammatory activity. The percentage of SIg positive hepatocytes was significantly higher in patients with CAH (median 52.5%) than in patients with CLH/CPH (20.5%) or in patients with MHA (1%). Percentages of SIg-positive liver cells were significantly correlated with total liver biopsy scores and with both portal or parenchymal scores considered independently. SIg were found to belong to the IgG class in all groups of patients. When hepatocytes were cultured with normal human lymphocytes, allogeneic cytotoxicity values were significantly higher in patients with CAH (median 34%) than in patients with CLH and CPH (18%) or in those with MHA (12%). Percentage cytotoxicity was positively correlated with total biopsy scores and with portal activity but not with parenchymal activity, suggesting that ADCC might play a damaging role mainly in the portal areas. Our results show that in HBsAg-positive and in HBsAg-negative chronic liver disease IgG on the liver cell membrane is associated with increased susceptibility to in vitro cytotoxicity by killer cells and with increased severity of histological liver damage, suggesting a direct role for these antibodies in the generation of the liver injury. [ABSTRACT FROM AUTHOR]

Published
1987
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36. Immune responses to liver membrane antigens in patients with cystic fibrosis and liver disease.

Author

MIELI-VERGANI, GIORGINA, PSACHAROPOULOS, HELEN T., NICHOLSON, ANDREA M., EDDLESTON, A. L. W. F., MOWAT, ALEX P., WILLIAMS, ROGER, Mieli-Vergani, G, Psacharopoulos, H T, Nicholson, A M, Eddleston, A L, Mowat, A P, and Williams, R

Abstract

Biliary obstruction by viscid mucus, although important, may not be the only factor for the development of liver disease in some patients with cystic fibrosis. In the present study the relationship between immune responses to liver antigens and the presence of liver damage was investigated using the leucocyte migration test and lymphocyte cytotoxicity to isolated rabbit hepatocytes. Inhibition of leucocyte migration by purified liver-specific lipoprotein, derived from hepatocyte plasma membrane, was found in 9 of 11 children with liver disease, but in only 5 of 14 with cystic fibrosis and no overt liver disease (P < 0.025). Lymphocyte toxicity to isolated rabbit hepatocytes was significantly increased in 10 of 13 children with liver disease, but in only 6 of 29 children without liver disease (P < 0.001). Experiments using lymphocyte subpopulations showed that the cytotoxicity was mediated by a non-T-cell population and could be blocked with liver-specific lipoprotein in 7 out of 10 cases, suggesting that the reaction in these patients was specifically directed against liver-specific lipoprotein. The study suggests that sensitisation against liver membrane antigens, whether arising primarily or secondarily in some way to other hepatic lesions, may contribute to the progression of liver damage in cystic fibrosis. [ABSTRACT FROM AUTHOR]

Published
1980
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37. Heterogeneity of liver/kidney microsomal antibody type 1 in autoimmune hepatitis and hepatitis C virus related liver disease.

Author

Muratori, L, Lenzi, M, Ma, Y, Cataleta, M, Mieli-Vergani, G, Vergani, D, and Bianchi, F B

Abstract

Liver/kidney microsomal antibody type 1 (LKM-1), the serological marker of a subset of autoimmune hepatitis, is also present in a proportion of patients with hepatitis C virus (HCV) related chronic liver disease. To characterise further this autoreactivity and to evaluate whether an autoantibody giving an identical immunofluorescence staining, and detected in two different clinical conditions, involves the same antigenic target(s), sera from autoimmune and HCV infected patients were tested with native, recombinant, and synthetic antigens. Sixty five sera were selected on the basis of the typical immunofluorescence pattern: 50 patients had serological markers of HCV infection, the remaining 15 suffered from autoimmune hepatitis. The reactivity of each serum with rat and human microsomal fractions, full length human recombinant CYP2D6, and two synthetic peptides spanning the amino acid regions 257-269 and 373-398 of CYP2D6 was systematically investigated by immunoblotting. Fourteen (93%) sera from autoimmune hepatitis patients and 39 (78%) from HCV infected patients reacted with rat and/or human microsomal polypeptides of 39 kD, 50 kD, 58 kD, and 66 kD in different associations, the 50 kD band being the most frequently observed. Reactivity to CYP2D6 and its amino acid sequence 257-269 was significantly more common in autoimmune hepatitis than in HCV infected patients (p < 0.001 and p < 0.0003, respectively). LKM-1 reactivity is directed against heterogeneous and not entirely defined autoantigens. The main target in autoimmune sera is CYP2D6 and its 257-269 amino acid region, while sera from patients with HCV infection are more likely to recognise other microsomal targets, the molecular identity of which is currently unknown. [ABSTRACT FROM PUBLISHER]

Published
1995

38. Fulminant hepatic failure resulting from coexistent Wilson's disease and hepatitis E.

Author

Sallie, R, Chiyende, J, Tan, K C, Bradley, D, Portmann, B, Williams, R, Mowat, A P, and Mieli-Vergani, G

Abstract

Fulminant hepatic failure resulting from hepatitis E and coexistent Wilson's disease was diagnosed in a six year old girl six weeks after returning from a holiday in India. Wilson's disease was diagnosed on the basis of histological evidence of hepatocellular copper deposition, confirmed by biochemical estimation of liver copper concentration. Although severely damaged, the liver was non-cirrhotic. Hepatitis E virus (HEV) was diagnosed by nested polymerase chain reaction, the specificity of which was confirmed by direct sequencing of amplified DNA. Replication of HEV within the liver at the time of diagnosis was confirmed by selective amplification of the antigenomic strand of the virus obtained from total liver RNA. The patient had an orthotopic liver transplantation without recurrence of hepatitis and remains well at 19 months. Viral excretion, recorded by serial amplification of HEV RNA extracted from stool samples, persisted for 30 days after liver grafting. Severe vitiligo, present preoperatively, dramatically improved after liver grafting and institution of immunosuppressive treatment. This case suggests that viral infection may play a part in the acute decompensation seen in some cases of Wilson's disease. [ABSTRACT FROM PUBLISHER]

Published
1994

39. Antineutrophil antibody: a test for autoimmune primary sclerosing cholangitis in childhood?

Author

Lo, S K, Chapman, R W, Cheeseman, P, Charlton, C P, Walker-Smith, J A, Mieli-Vergani, G, and Fleming, K A

Abstract

The detection of an antineutrophil antibody which is highly sensitive and specific for adult primary sclerosing cholangitis using indirect immunoalkaline phosphatase has been previously described. In this study, the diagnostic potential of this method in childhood primary sclerosing cholangitis is described. A range of 72 blinded children's sera (36 boys), aged six months to 21 years (10 primary sclerosing cholangitis, eight autoimmune chronic active hepatitis, 10 alpha-1 antitrypsin deficiency, 12 extrahepatic bile duct atresia, 11 ulcerative colitis and 21 normal subjects) was assayed. Eight of the 10 primary sclerosing cholangitis patients were correctly identified. Three patients with chronic active hepatitis also showed the characteristic primary sclerosing cholangitis pattern of staining. No ulcerative colitis patients or any other patients showed this pattern of staining. All normal subjects were negative. As in adult primary sclerosing cholangitis, there is a specific antineutrophil antibody in childhood primary sclerosing cholangitis and this provides further evidence towards an autoimmune aetiology of this condition. The test may have diagnostic potential. [ABSTRACT FROM PUBLISHER]

Published
1993

40. Soluble interleukin 2 receptors in autoimmune chronic active hepatitis.

Author

Lobo-Yeo, A, Mieli-Vergani, G, Mowat, A P, and Vergani, D

Abstract

Children with uncontrolled autoimmune chronic active hepatitis have increased numbers of activated T lymphocytes expressing interleukin 2 receptors (IL2R). A soluble form of IL2R has recently been described whose proposed role is to downregulate T cell activation by competing for interleukin 2. We investigated whether a deficiency of soluble IL2R could account for the high concentrations of IL2R positive T lymphocytes in autoimmune chronic active hepatitis. Soluble IL2R was measured by enzyme-linked immunosorbent assay in the serum of 16 children with autoimmune chronic active hepatitis, eight with chronic liver disease due to hepatitis B virus infection, seven with Wilson's disease, nine with alpha 1 antitrypsin deficiency, and 15 healthy age matched controls. Soluble IL2R concentration was significantly higher in patients with autoimmune chronic active hepatitis than in healthy controls (mean (SEM) 475 (75) U/ml, 145 (8) U/ml respectively, p less than 0.01). Eleven patients who had active disease had significantly higher soluble IL2R concentrations (590 (89) U/ml) than the five cases with inactive disease (220 (36) U/ml, p less than 0.01). No difference was found between the controls and the patients with chronic liver disease due to hepatitis B infection, Wilson's disease, and alpha 1 antitrypsin deficiency. Percentages and absolute numbers of surface IL2R positive T cells as detected by immunofluorescence were significantly higher in the patients with autoimmune chronic active hepatitis (11.8% (1); 274/microliters (31)) than in controls (0.2% (0.1); 5/microliters (2), p less than 0.001), the highest values being found in those with uncontrolled disease. A significantly positive correlation was observed between concentrations of soluble IL2R and the percentage of T cells expressing IL2 receptors (r=0.67, p<0.001). These results indicate that the high levels of IL2R positive T lymphocytes characteristic of autoimmune chronic active hepatitis are not due to a deficiency of soluble IL2 receptors. [ABSTRACT FROM PUBLISHER]

Published
1990

41. Lymphocyte cytotoxicity to autologous hepatocytes in alpha 1-antitrypsin deficiency.

Author

Mondelli, M, Mieli-Vergani, G, Eddleston, A L, Williams, R, and Mowat, A P

Abstract

To investigate the possible role of cell mediated cytotoxicity in the pathogenesis or perpetuation of liver damage associated with alpha 1-antitrypsin (AAT) deficiency, peripheral blood lymphocytes (PBL) from 13 children with PiZZ phenotype who had had liver disease in infancy were incubated with autologous hepatocytes in a microcytotoxicity assay. There was a clear trend for cytotoxicity to increase with age and thus significantly increased cytotoxicity was found in four cases older than 2 years, while intermediate values were recorded in three children between 6 months and 2 years and normal values in children younger than 6 months. Fractionation of PBL into T and non-T-enriched subsets showed that both were involved in the cytotoxic reaction. A purified liver membrane lipoprotein preparation (LSP) inhibited both T and non-T-cell cytotoxicity suggesting that LSP is a major target antigen in this system. Control experiments performed in infants with neonatal hepatitis syndrome, but with normal Pi phenotype, showed consistently increased cytotoxicity values. Cell-mediated immune reactions directed against autologous hepatocytes develop late in the course of the liver disease associated with AAT deficiency. While this reaction cannot be involved in the pathogenesis of the initial liver lesion, it may contribute to perpetuation of liver damage. [ABSTRACT FROM PUBLISHER]

Published
1984

42. Lymphocyte cytotoxicity to autologous hepatocytes in HBsAg positive chronic liver disease.

Author

Mieli-Vergani, G, Vergani, D, Portmann, B, White, Y, Murray-Lyon, I, Marigold, J H, Woolf, I, Eddleston, A L, and Williams, R

Abstract

Lymphocytes from 39 patients with HBsAg positive chronic liver disease were incubated with their own hepatocytes to investigate mechanisms of lymphocyte-mediated liver damage. Cytotoxicity was significantly increased in 46% overall, and in 73% of those with chronic active hepatitis. Unlike HBsAg negative chronic active hepatitis where only non-T cells were cytotoxic, HBsAg positive patients had both cytotoxic T and non-T cells. A purified liver membrane complex (LSP) and aggregated IgG both blocked non-T cytotoxicity without affecting T cell cytotoxicity; this suggests that the former is probably an antibody-dependent cell-mediated reaction against normal membrane components. This was confirmed in preliminary studies which demonstrated that preincubation of hepatocytes with the F(ab)2' fragment of an anti-human IgG reduced non-T lymphocyte cytotoxicity. T-cell cytotoxicity was restricted to HBeAg-positive patients, suggesting a relationship between T-cell cytotoxicity and viral replication. Purified HBsAg, however, blocked cytotoxicity in only three of 11 cases. Non-T lymphocytes reacting with normal membrane components may contribute to liver damage in both 'autoimmune' and virus-associated chronic liver disease, whereas cytotoxic T-cells, probably reacting with viral determinants, are exclusive to those with viral replication. [ABSTRACT FROM PUBLISHER]

Published
1982

44. Association between HLA and extrahepatic biliary atresia.

Author

Silveira, Themis R., Salzano, Francisco M., Donaldson, Peter T., Mieli-Vergani, Georgina, Howard, Edward R., Mowat, Alex P., Silveira, T R, Salzano, F M, Donaldson, P T, Mieli-Vergani, G, Howard, E R, and Mowat, A P

Published
1993

46. Complement activation in uveitis.

Author

Vergani, S., Di Mauro, E., Davies, E. T., Spinelli, D., Mieli-Vergani, G., and Vergani, D.

Abstract

To determine whether complement is activated in uveitis we have measured plasma levels of C3d, a sensitive indicator of complement activation. Increased levels of C3d were found in 11 of 15 patients with idiopathic uveitis, 13 of whom had circulating immune complexes containing complement components. Since during complement activation potent mediators of inflammation are generated, it is suggested that the activation of complement, possibly triggered by uveal deposition of immune complexes, has an important role in the pathogenesis of uveitis. [ABSTRACT FROM PUBLISHER]

Published
1986

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