The haematological findings in cryptogenetic splenomegaly with and without cirrhosis and in primary carcinoma of the liver

Todd, David, 達安輝

January 1958

published_or_final_version / Medicine / Master / Doctor of Medicine

Liver - Diseases.

Liver - Tumors.

Blood - Examination.

Spleen - Diseases.

The effect of nicotine on liver functions in rats and its modulation of the hepatotoxicity induced by carbon tetrachloride

Gogo, Arturo R.

January 1992

published_or_final_version / Medical Sciences / Master / Master of Medical Sciences

Nicotine - Physiological effect.

Liver - Diseases.

Rats - Physiology.

Hepatotoxicology.

Carbon tetrachloride.

Glutathione metabolism in the rat under varied nutritional conditions

Hum, Susan

January 1991

We developed a methodology to measure plasma hepatic glutathione (GSH) turnover and we tested it in rats treated with an inhibitor of GSH synthesis. Our goal was to determine whether protein intakes above NRC recommendations maximize hepatic GSH stores and turnover in vivo. We also wished to learn if plasma GSH, cysteine, or methionine concentrations or plasma GSH turnover could be used as noninvasive predictors of liver GSH status. Rats were fed purified diets containing 0, 5, 10, 20 or 40% casein for one week. The 0 and 5% casein diets were considered inadequate in protein, 10% marginal, 20% adequate and 40% excessive. Liver GSH content (mmol/liver) of rats fed 0 and 5% casein diets was 12.29 $ pm$ 1.11 and 16.43 $ pm$ 0.95, respectively, and increased to 23.62 $ pm$ 1.82 in the 10% group. Liver GSH content did not differ between the 20 and 40% groups. As dietary casein increased from 0-20%, free plasma GSH and cysteine concentrations and plasma GSH turnover increased, but did not increase further with the 40% diet. A sigmoidal relationship between plasma GSH turnover and hepatic GSH content was demonstrated. The best predictor of liver GSH content was not free plasma GSH concentration nor plasma GSH turnover, but the free plasma cysteine concentration.

Rats -- Nutrition.

Glutathione -- Metabolism.

The application of DNA hybridisation methods to a determination of the association of hepatitis B virus with cirrhosis and hepatoma.

Nair, Shamila.

January 1987

Autopsy liver material from patients having died of chronic liver disease, cirrhosis, hepatocellular carcinoma (HCC) and causes unrelated to liver diseases was examined by dot blot hybridisation for the presence of HBV DNA. The results indicate that of the patients with chronic liver disease 6/9 were positive for HBV DNA in the liver tissue; of the patients with HCC 3/4 were positive for HBV DNA; of the patients with cirrhosis 4/4 showed the presence of HBV DNA in the liver. Thus by this technique 13/17 (76%) of these patients, all of whom were HBsAg positive, were shown to have HBV DNA present in liver tissue. However, autopsy liver samples were found to be unsuitable for Southern blot hybridisation. Biopsy liver/tumour tissue was examined for the presence of integrated or non-integrated HBV DNA by Southern blot analysis using the enzymes Eco R1 and Hind 111. 5/5 patients who were both HBsAg and HBeAg positive had extrachromosomal HBV DNA and 2/5 also showed the presence of integrated HBV DNA. 3/4 patients who were HBsAg positive and HBeAg negative had extrachromosomal HBV DNA and all three also had integrated HBV DNA. One control patient was negative for both markers and also for Southern blot hybridisation with the HBV DNA probe. These results support the hypothesis that HBV is a factor in the development of HCC, and indicate that the dot blot hybridisation method would be suitable for routine evaluation of patients with chronic liver disease or cirrhosis. / Thesis (M. Med.)-University of Natal, Durban, 1987.

Hepatitis B.

Hepatitis, Viral.

Liver--Cirrhosis.

Liver--Diseases.

Theses--Virology.

The role of hepatic regeneration and angiogenesis in the response to surgical attenuation of congenital portosystemic shunts in dogs

Tivers, Michael Samuel

January 2013

No description available.

636.7089

Studies of the bipolar inline radiofrequency ablation device (ILRFA) in liver and kidney transection.

Yao, Peng, St. George Clinical School, UNSW

January 2007

Surgical resection is the best option for both liver and kidney cancers, which providing the long term survival. However intraoperative blood loss can be a significant challenge, and is clearly associated with morbidity and mortality. Radiofrequency ablation (RFA) precoagulation has been introduced into liver and kidney surgery. Promising results have already achieved in reduction of intraoperative blood loss. In this thesis, a detailed explanation on precoagulation by RFA has been given. Our group developed a novel bipolar multi-array RFA device ??? InLine (ILRFA). In this thesis, we have investigated the performance in a variety of fields. In the study of ILRFA-assisted laparoscopic liver resection, ILRFA was easily employed through a hand port and achieved significant decrease of blood loss compared to control group (p < 0.05). In the liver trauma study, ILRFA produced a 63.88% reduction of blood loss in peripheral injury and 53.57% in central injury respectively. In postoperative evaluation of ILRFA-assisted liver resection, animals underwent an uneventful recovery, no complications occurred. Histological examination revealed a typical post RFA evolution. In ILRFA-assisted partial nephrectomy, the mean intraoperative blood loss 35 ?? 7 ml in the ILRFA and 152 ?? 94 ml in the control, a 77.0% reduction (P = 0.024). The mean blood loss per centimetre resection area was 2.09 ?? 1.41 ml/cm2 in the ILRFA compared with 12.79 ?? 1.68 ml/cm2 in controls, the reduction was 79.0% (P = 0.019). In ILRFAassisted laparoscopic partial nephrectomy, the mean intraoperative blood loss was 32 ?? 15 ml in the ILRFA and 187 ?? 69 ml in the control group, a 77.0% reduction (P = 0.043). The mean blood loss per centimetre resection area was 2.27 ?? 0.95 ml/cm2 in the ILRFA compared with 26.46 ?? 8.81 ml/cm2 in controls, the reduction was 79.0% (P = 0.047). In the renal trauma experiment, ILRFA also achieved promising results in haemostasis. We believe that ILRFA is a useful device which may help in the treatment of patients with liver and kidney illness.

Liver -- Diseases -- Treatment.

Kidneys -- Diseases -- Treatment.

Radiofrequency spectroscopy.

IgA nephropathy and liver disease / by Jane Lomax-Smith

Lomax-Smith, Jane

January 1984

Bibliography: leaves 331-381 / xxiv, 381 leaves : ill ; 31 cm. / Title page, contents and abstract only. The complete thesis in print form is available from the University Library. / Thesis (Ph.D.)--University of Adelaide, 1986

616.61 19

Immunoglobulin A.

Kidneys Diseases.

Liver Diseases.

Liver Cirrhosis.

Studies on alcoholic liver disease /

Stokkeland, Knut,

January 2006

Diss. (sammanfattning) Stockholm : Karolinska institutet, 2006. / Härtill 4 uppsatser.

Hepatitis B virus associated antigens (HBAgS) in patients with liver diseases /

Sirirat Rengpipat.

January 1979

Thesis (M.Sc. (Microbiology))--Mahidol University, 1979. / Financial support from University Development Committee and National Cancer Institute.

Perfil imunofenotípico e nível de citocinas plásmáticas em portadores de hepatite C crônica com diferentes graus de comprometimento hepático

Magnoni, Mariana Sartori [UNESP]

27 February 2014

Made available in DSpace on 2014-11-10T11:09:57Z (GMT). No. of bitstreams: 0 Previous issue date: 2014-02-27Bitstream added on 2014-11-10T11:57:30Z : No. of bitstreams: 1 000783135.pdf: 4785949 bytes, checksum: 6679e25c8d6dcfd9b73004d8151c331e (MD5) / O vírus da hepatite C crônica (VHC) é causa de doença hepática crônica afetando cerca de 3% da população mundial, aproximadamente 170 milhões de pessoas. Investigações sobre a resposta imune em indivíduos infectados com HCV é justificável pelo fato desta constituir doença infecciosa cujas alterações imunológicas têm relação direta com o desenvolvimento e a manutenção da infecção. Este projeto visou avaliar aspectos que compõem a resposta imune de pacientes com hepatite C crônica com diferentes graus de lesão hepática. Foram incluídos no estudo pacientes VHC+ (n=83), genótipo 1, pré-tratamento, os quais foram estratificados conforme o grau de fibrose hepática determinada por biópsia (classificação METAVIR), compondo: G1 (n = 15) pacientes nos estágios F0 (nenhuma fibrose) + F1 (fibrose em expansão dos espaços porta); G2 (n = 21) pacientes no estágio F2 (poucas fontes de fibrose nos espaços porta); G3 (n = 15) pacientes em estágio F3 (início da formação de nódulos); G4 (n = 32) pacientes em estágio F4 (fibrose severa); G5 (n = 16) doadores de sangue voluntários (grupo controle). Foram avaliadas características imunofenotípicas de subpopulações de leucócitos do sangue periférico (células NK totais, NKdim, NKbright, células dendríticas mielóides e plasmocitóides, monócitos clássicos e pro-inflamatórios, linfócitos T CD4+/CD8+), níveis de citocinas e quimiocinas plasmáticas (TGF-β, TNF-α, CCL2, CCL3, CCL4, CCL5, CXCL8, CXCL9, CXCL10), analisando a relação destes com a progressão da fibrose. Todas as frequências das subpopulações leucocitárias avaliadas estão alteradas em portadores de hepatite C crônica comparados com indivíduos saudáveis. Além disso, há correlação entre o grau de fibrose e a quantidade de linfócitos T CD4, T CD8, monócitos pro-inflamatórios e células NKbright circulantes. Níveis aumentados de TNF-α foram observados ... / The chronic hepatitis C virus (HCV) is the cause of chronic liver disease affecting about 3% of world population, approximately 170 million people. Investigations of the immune response in individuals infected with HCV is justifiable because this form infectious disease whose immunological changes are directly related to the development and maintenance of infection. This project aimed to evaluate aspects that make up the immune chronic hepatitis C patients with different degrees of liver damage response. The study included patients HCV+ (n = 83), genotype 1, pretreatment, which were classified according to the rate of hepatic fibrosis determined by biopsy (METAVIR classification), composed of: G1 (n = 15) patients in stages F0 (no fibrosis) + F1 (fibrosis expansion of port spaces), G2 (n = 21) patients in the F2 stage (few sources of fibrosis in portal ), G3 ( n = 15 ) patients with stage F3 (early nodule formation), G4 (n = 32) patients with stage F4 (severe fibrosis), G5 (n = 16) volunteer blood donors (control group). Immunophenotypic characteristics of subpopulations of peripheral blood leukocytes (total NK cells, NKdim , NKbright , myeloid dendritic cells and plasmacytoid , classical monocytes, pro- inflammatory CD4 + / CD8 + cells), cytokine levels and plasma chemokines (were evaluated TGF- β , TNF - α , CCL2 , CCL3 , CCL4 , CCL5 , CXCL8 , CXCL9, CXCL10), analyzing their relationship with the progression of fibrosis. All frequencies of evaluated leukocyte subpopulations are altered in patients with chronic hepatitis C compared with healthy subjects. In addition, no correlation between the degree of fibrosis and the amount of CD4, CD8, pro-inflammatory monocytes and circulating NKbright cells. Increased levels of TNF-α were observed in cirrhotic patients (G4) and TGF - β in HCV + groups with moderate hepatic fibrosis (G2 and G3). Plasma chemokine CXCL9/MIG, CXCL10/IP-10, CXCL8/IL-8, CCL2/MPC-1, ...

Hepatite C

Citocinas

Marcadores biologicos

Figado - Doenças

Fibromialgia

Liver Diseases