Prominent proliferative response of peripheral blood mononuclear cells to a recombinant non-structural (NS3) protein of hepatitis C virus in patients with chronic hepatitis C.

The proliferative response of peripheral blood mononuclear cells (PBMC) to a recombinant non-structural (NS3) protein of hepatitis C virus (HCV) was studied in 41 patients with chronic hepatitis C. Of them, 28 had chronic persistent hepatitis (CPH) and 13 chronic active hepatitis (CAH). The positive proliferation rate of PBMC to the recombinant NS3 protein, T9Ag, was 66% in the 41 patients (77% in CAH versus 61% in CPH; P > 0.05) when stimulation index (SI) = 4 was set as the cut-off value. However, mean SI of CAH patients was significantly higher than that of CPH patients (8.3 +/- 5.2 versus 5.1 +/- 3.6; P < 0.05). Six other chronic hepatitis patients who were repeatedly negative for anti-HCV antibody but positive for serum HCV RNA also had an SI of > or = 4.0. The frequency of cellular immune response to the T9Ag is among the highest results obtained by using HCV antigens tested so far. Our studies thus indicate that NS3 is an immunologically important region of HCV for T cells. Moreover, the proliferative response to T9Ag may help to establish hepatitis C etiology in chronic hepatitis patients who are seronegative with currently available anti-HCV assays.     

Thymoma and hypogammaglobulinemia (Good's syndrome): a case report.

Good's syndrome is extremely rare and refers to an acquired B and T cell immunodeficiency in thymoma patients. We report a 51-year-old female thymoma patient who presented with recurrent herpes zoster, pneumonia, diarrhea and opportunistic infections. She was found to have acquired hypogammaglobulinemia with absent B cells. Despite repeat intravenous immunoglobulin replacement and antibiotic therapy, she died of bacterial pneumonia-induced acute respiratory distress syndrome. Clinicians should look for evidence of immunologic dysfunction in thymoma patients presenting with recurrent infections.     

A tctex1-Ca2+ channel complex for selective surface expression of Ca2+ channels in neurons

Voltage-gated Ca(2+) channels (VGCCs) are important in regulating a variety of cellular functions in neurons. It remains poorly understood how VGCCs with different functions are sorted within neurons. Here we show that the t-complex testis-expressed 1 (tctex1) protein, a light-chain subunit of the dynein motor complex, interacts directly and selectively with N- and P/Q-type Ca(2+) channels, but not L-type Ca(2+) channels. The interaction is insensitive to Ca(2+). Overexpression in hippocampal neurons of a channel fragment containing the binding domain for tctex1 significantly decreases the surface expression of endogenous N- and P/Q-type Ca(2+) channels but not L-type Ca(2+) channels, as determined by immunostaining. Furthermore, disruption of the tctex1-Ca(2+) channel interaction significantly reduces the Ca(2+) current density in hippocampal neurons. These results underscore the importance of the specific tctex1-channel interaction in determining sorting and trafficking of neuronal Ca(2+) channels with different functionalities.     

卡介苗多糖核酸对过敏性支气管哮喘外周血单个核细胞TH1/TH2反应的作用

目的观察卡介苗多糖核酸(BCG-PSN)对支气管哮喘患者外周血淋巴细胞TH1/TH2反应的作用,并与结核菌素纯蛋白衍生物(TB-PPD)进行比较. 方法缓解期过敏性支气管哮喘患者16例,对照组健康成人13例,分离外周血单个核细胞(PBMC),分别加入不同浓度的BCG-PSN(1、10、100、1000 μg/ml)、TB-PPD(10 μg/ml)、尘螨抗原(DerP, 10 μg/ml)体外培养4 d,不加刺激剂者为阴性对照.收集培养上清,ELISA检测IFN-γ、IL-5浓度的变化. 结果 PSN(1～100 μg/ml)刺激正常人PBMC分泌IFN-γ水平均高于哮喘患者(P＜0.05).BCG-PSN(10 μg/ml)可以刺激哮喘患者PBMC分泌IFN-γ(358.7 pg/ml,范围0～2433.0 pg/ml),但显著低于同等浓度的TB-PPD刺激作用(13 036 pg/ml,范围600.5～35 100.0 pg/ml,P＜0.01).PSN刺激PBMC分泌IFN-γ呈浓度依赖性,当浓度达到100 μg/ml时,与低浓度相比刺激作用显著增强(P＜0.01),与TB-PPD的刺激作用类似.DerP刺激哮喘患者PBMC分泌IL-5水平显著高于正常人(P＜0.05).BCG-PSN刺激PBMC分泌IL-5的作用较弱,显著低于TB-PPD和DerP的刺激作用. 结论 BCG-PSN具有一定的TH1刺激作用,但低于TB-PPD的刺激作用,有待对BCG-PSN组分进一步优化以增强疗效.     

Epstein-Barr virus-associated smooth muscle tumor in patients with acquired immunodeficiency syndrome.

Epstein-Barr virus (EBV)-associated smooth muscle tumor (SMT) is a recognized but uncommon disease that is found to occur in patients with immunocompromised conditions such as acquired immunodeficiency syndrome (AIDS). These tumors may be multifocal and located at unusual sites, such as the brain and liver. This report describes the case of 2 AIDS patients with EBV-associated SMT and highlights the features and outcome of this rare but potentially important tumor in human immunodeficiency virus management.     

The B/C gene of simian virus 40.

Temperature-sensitive B, C, and BC mutants of Simian virus 40 (SV40) map in the late region of the viral genome inHin fragments K, F, J, and G, a DNA segment of about 1200 nucleotide pairs (Lai, C.-J., and Nathans, D. (1975)Virology 66, 70–81). To define the B/C region further, mutants of SV40 with deletions in this genomic segment were constructed by enzymatic excision of DNA from the viral genome, followed by cloning in the presence of a complementing tsA mutant of SV40. After localization of deleted genome segments by analysis of endo R fragments and electron microscopic heteroduplex mapping, selected deletion mutants were tested for complementation by ts mutants and were screened for their ability to produce new viral proteins in infected cells. Complementation tests indicated that B/C deletion mutations are in a cistron distinct from that of tsA and tsD mutations and that the junction between the B/C and D genes is within Hin-K. Two of the deletion mutants produced new proteins detectable in infected cells. More detailed analysis of one of these proteins (of molecular weight 25,000) indicated that it precipitated with antiserum against dissociated SV40 capsids, and that all but one of its lysine-containing tryptic peptides cochromatographed with SV40 VP1 tryptic peptides. We conclude that the B/C gene, containing approximately 1200 nucleotide pairs, codes for VPl. Since deletion mutants lacking Hin-E do not complement B mutants, we suggest that the Hin-E DNA segment has a signal required for expression of the B/C gene.     

Status of hepatitis B virus DNA in hepatocellular carcinoma: a study based on paired tumor and nontumor liver tissues

To investigate the hepatitis B virus (HBV) DNA status in the liver when hepatocellular carcinoma (HCC) has developed, 35 paired nontumorous and tumorous liver tissues from 27 hepatitis B surface antigen (HBsAg)-seropositive and 8 HBsAg-negative patients with HCC were studied by Southern blot analysis. The hybridization patterns of HBV DNA were different in the nontumor and tumor parts in 26 (96.3%) of the 27 HBsAg-positive patients. In the nontumor parts, integration of HBV DNA into the host genome was significantly less when compared to the tumor parts (15/27 vs. 25/27, P less than 0.05), whereas free replicative viral forms were significantly more frequent (17/27 vs. 7/27). The integrated HBV DNA in the nontumor parts showed discrete band patterns in the majority of cases (13/15). Hepatitis B e antigen (HBeAg) was significantly associated with the expression of free replicative forms of HBV DNA in the tumor tissues. An integrated HBV DNA sequence was detected in the tumor part of one HBsAg-negative patient, but not in her nontumor counterpart. Our observation that discrete integrated HBV DNAs are present in the nontumor part, representing subclinical clonal expansion that precedes the development of HCC, suggests the risk of future new tumor growth from these cell clones.     

Identification of four distinct regions of allelic imbalances on chromosome 1 by the combined comparative genomic hybridization and microsatellite analysis on hepatocellular carcinoma.

Frequent chromosome 1 abnormalities detected in human hepatocellular carcinoma have been implicated in early genetic events of liver carcinogenesis. Recurrent loss of 1p with a common deleted region 1p36-p34 has been reported from microsatellite analysis, whereas common gain of the whole chromosome q-arm was described from several comparative genomic hybridization studies. The relationships between copy number changes and allelic status however remains unclear. In this study, we have conducted a simultaneous comparative genomic hybridization and microsatellite analysis study on chromosome 1 in 31 hepatocellular carcinoma cases. Microsatellite analysis revealed frequent loss of heterozygosity on 1p at loci D1S468 (74%), D1S450 (67%), D1S2667 (65%), D1S2697 (75%), D1S199 (52%), and D1S234 (67%) corresponded to the distal 1p36 region and coincided with 12 cases (86%) that presented losses on 1p by comparative genomic hybridization analysis. Although comparative genomic hybridization indicated a common deleted region of 1p36-p35 in the current series, microsatellite analysis has refined the smallest overlapping region (SOR) to 1p36.13-p36.22. Gain of 1q as revealed by comparative genomic hybridization suggested low and high-level gains, and cases that displayed an amplicon below the heterochromatic region 1q21-q25. Common allelic imbalances of polymorphic markers D1S2635 (64%), D1S484 (67%), D1S2878 (65%), D1S196 (70%), D1S249 (64%) D1S2785 (75%), D1S2842 (73%) and D1S2836 (74%) that corresponded to the regions 1q23.1-q24.2, 1q32.1 and 1q43-q44 were detected. Three distinct regions of allelic imbalances were thus suggested on recurring 1q gain found in hepatocellular carcinoma. Furthermore, microsatellite analysis has enabled a mapping of common overrepresented regions and suggested SOR on 1q23.1-q23.3 (D1S2635-D1S2878), 1q25.1-q31.1 (D1S452-D1S238), and 1q43 (D1S2785-D1S2842). Our current study has refined chromosome 1 aberrations in hepatocellular carcinoma to four regions of allelic imbalances. The SORs delineated should provide basis for further molecular investigation in hepatocarcinogenesis on genes residing on these chromosomal regions.