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OBJECTIVE: To determine viral DNA load in peripheral blood mononuclear cells (PBMC) from HIV-1-infected individuals. DESIGN: HIV-1 copy numbers were determined using a quantitative polymerase chain reaction (PCR), the PCR-aided template titration assay (PATTY). PATTY utilizes an internal plasmid control DNA, which is amplified within the same tube and using the same primers as the PBMC target DNA. HIV-1 copy numbers were confirmed by limiting-dilution PCR analysis. RESULTS: PBMC viral load of 19 long-term (greater than 4 years) HIV-1-infected individuals ranged from 0.8 to 100 copies per 10(3) PBMC. Significantly higher copy numbers were found among p24-antigen-positive than among p24-antigen-negative individuals. In addition, the PBMC viral load of two HIV-1-infected individuals was monitored during the first 3 months after acute infection. For both patients, the HIV-1 copy numbers were shown to peak at the time of HIV-1-antibody seroconversion and decline subsequently (range, 0.6-10 copies per 10(3) PBMC). CONCLUSIONS: PATTY is a useful method for assessing the HIV-1 copy numbers in PBMC DNA. Viral DNA load peaks shortly after infection and reaches an individual specific level that is probably stable within a few months of infection. Viral DNA load in PBMC varies widely among long-term HIV-1-infected individuals. 相似文献
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目的通过对广西艾滋病病毒Ⅰ型(HIV-1)新近感染者耐药基因变异的研究,了解当地HIV耐药毒株传播的水平。方法通过序贯抽样的方法,采集70例2007年8-10月新确证的、年龄在15~25岁的HIV感染者的全血样本,使用In-house法扩增HIV-1 pol区部分基因片段,并进行耐药基因变异分析。结果得到47条序列,其中有1份在蛋白酶区发生主要耐药突变M46L,可引起对ATV和NFV的低水平耐药性;在反转录酶区存在T69NT突变,仅引起对d4T和DDI的潜在耐药性。根据WHO HIV耐药警戒线监测方法判断,广西HIV耐药株属于低传播水平(<5%)。结论广西HIV新近感染者中已有HIV耐药株的传播,但是目前传播水平还较低,应继续开展HIV耐药毒株传播的监测工作。 相似文献
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Neopterin concentrations in cerebrospinal fluid and serum of individuals infected with HIV-1 总被引:4,自引:0,他引:4
D Fuchs F Chiodi J Albert B Asj? L Hagberg A Hausen G Norkrans G Reibnegger E R Werner H Wachter 《AIDS (London, England)》1989,3(5):285-288
Neopterin, a biochemical marker for the activation of cell-mediated immune reactions, was determined in serum and cerebrospinal fluid (CSF) from patients infected with HIV-1. A significant correlation was found between serum and CSF neopterin concentrations, although concentrations of neopterin in serum were more closely correlated with the clinical severity of HIV-1 infection than those in CSF. However, higher CSF levels were observed in patients with neurologic/psychiatric symptoms than in unaffected patients. Also, quotients of CSF neopterin versus serum neopterin concentrations were increased, indicating intrathecal production of neopterin. Positive HIV-1 isolation from peripheral blood mononuclear cells (PBMC) was associated with higher neopterin concentrations in serum, when compared with negative HIV-1 isolation. Neopterin in CSF appears to be a suitable biochemical marker in patients with HIV-1 infection for detecting overt neurologic/psychiatric disturbances. The data suggest that in HIV-1 infected patients, cell-mediated immune reactions might be activated intrathecally and might contribute to neuropsychiatric disease. 相似文献
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Similar rate of disease progression among individuals infected with HIV-1 genetic subtypes A-D. 总被引:16,自引:0,他引:16
OBJECTIVE: HIV-1 is characterized by a high degree of genetic variation and can be divided into at least 10 distinct genetic subtypes. The purpose of this study was to investigate whether the rate of disease progression shows subtype-specific differences. DESIGN: The investigation was divided into two parts; one study in which 49 ethnic Africans were compared with 49 ethnic Swedes irrespective of the subtype of the infecting virus, and a second study in which 126 individuals infected with different genetic subtypes (28 with subtype A, 59 with subtype B, 21 with subtype C and 18 with subtype D) were compared. METHODS: CD4 cell counts, the rate of CD4 cell decline, plasma HIV-1 RNA levels, clinical status and antiviral treatment were prospectively and retrospectively recorded. The HIV-1 subtype had previously been determined by direct sequencing of the V3 domain of the env gene. RESULTS: There were no significant differences in the rate of CD4 cell decline or clinical disease progression between Africans and Swedes over an observation period of 2 years. Similarly, there were no differences in the rate of CD4 cell decline, clinical progression or plasma HIV-1 RNA levels between individuals infected with subtypes A, B, C or D over a mean observation period of 44 months. CONCLUSION: Neither the genetic subtype of the virus nor the ethnicity of the host appear to be major determinants of disease progression. 相似文献
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M C Re G Zauli G Furlini M Vignoli E Ramazzotti S Ranieri M La Placa 《AIDS research and human retroviruses》1992,8(7):1289-1295
In this study we evaluated interleukin-6 (IL-6) plasma levels in 80 human immunodeficiency virus type 1 (HIV-1) seropositive (+) individuals and 51 HIV-1 seronegative (-) blood donors. Plasma IL-6, detectable only in a subset of HIV-1(+) individuals (45 of 80) and normal blood donors (28 of 51), was significantly (p less than 0.01) increased in HIV-1(+) subjects 187 +/- 20.5 vs. 86.3 +/- 14 pg/ml). Among HIV-1-infected individuals, ARC/AIDS patients showed the highest IL-6 values (243.3 +/- 43.3 pg/ml). HIV-1(+) subjects showed, at all the different stages of the disease, a significant increase in total gammaglobulins, particularly IgG (2071 +/- 101 vs 1265 +/- 34 of HIV-1 seronegative controls). Although among HIV-1-infected individuals, the group with detectable plasma levels of IL-6 shows the highest levels of IgG (2243 +/- 146 vs. 1790 +/- 105, p less than 0.05), no positive correlations were observed between plasma levels of IL-6 and total gamma globulins (r = 0.2) or IgG (0.17). IL-6 production was also examined in the endotoxin-free supernatants of peripheral blood cultured monocytes and CD4+ T lymphocytes, in the presence or absence of specific stimuli. The amount of IL-6 released in monocyte and CD4+ T-lymphocyte culture supernatants was similar in 40 HIV-1(+) individuals and 35 HIV-1(-) controls. Our data show that plasma levels of IL-6 are significantly increased in HIV-1-infected individuals, in particular in ARC/AIDS patients. However, such an increase does not strictly correlate with the degree of hypergammaglobulinemia in the same HIV-1-infected individuals. 相似文献
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Lack of autologous neutralizing antibodies in the cerebrospinal fluid of HIV-1 infected individuals. 总被引:1,自引:0,他引:1
A von Gegerfelt F Chiodi B Keys G Norkrans L Hagberg E M Feny? K Broliden 《AIDS research and human retroviruses》1992,8(6):1133-1138
The cerebrospinal fluids (CSF) and sera from HIV-1-infected individuals at different clinical stages were monitored for neutralizing activity against CSF-derived HIV-1 isolates. None of the CSF samples and only one of seven serum samples could neutralize the autologous CSF isolate. CSF samples collected one to two years later from the same patients also lacked autologous neutralizing antibodies against these isolates. However, some CSF samples were able to neutralize heterologous CSF isolates albeit in low titers. HIV antibody positive control sera could readily neutralize all of the CSF isolates demonstrating that these isolates were not resistant to neutralization per se. IgG antibodies against the HIV-1 envelope protein and, specifically, against the V3 loop of HIV-1 gp120 (MN) were present in some CSF samples, although the samples lacked neutralizing activity. In summary, this study demonstrates a lack of autologous neutralizing antibodies in CSF samples when assayed against CSF-derived HIV-1 isolates. 相似文献
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Galán I Jiménez JL González-Rivera M De José MI Navarro ML Ramos JT Mellado MJ Gurbindo MD Bellón JM Resino S Cabrero E Muñoz-Fernández MA 《AIDS (London, England)》2004,18(2):247-255
OBJECTIVE: To investigate the effects of salvage therapy with lopinavir-ritonavir on HIV-1 phenotype in heavily antiretroviral experienced HIV-infected children. DESIGN: Twenty antiretroviral experienced HIV-infected children were studied during a mean of time of 16.1 months from initiation of the treatment with lopinavir-ritonavir. METHODS: Besides CD4 T cells, viral load and clinical status, we analyzed 91 serial viral isolates to study the phenotype, and biological clones derived from co-cultivation techniques. RESULTS: We observed an increase in CD4 T cells, a statistically significant decrease in viral load and clinical benefits from 3 months after treatment. Ninety per cent of children had SI/X4 bulk isolates in peripheral blood mononuclear cells at study entry. The viral phenotype changed to non syncitium-inducing (NSI)/R5 in 94% of the children after a mean of 5.7 months (95% confidence interval, 2.1-9.3 months) of salvage therapy. The remaining 10% of children had NSI/R5 isolates at entry and at all follow-up study. Similar results were found at the clonal level. Thus, at study entry in PBMC of three children with bulk syncitium-inducing (SI) phenotype, we recovered 65 biologic clones, 56 being SI and nine NSI. After salvage therapy bulk isolates changed to NSI and of 40 biologic clones recovered only five were SI and the rest were NSI. CONCLUSIONS: Our data suggest that lopinavir-ritonavir salvage therapy led not only to a viral load decrease but also to a phenotypic change. X4 virus appeared to be preferentially suppressed. Shifts in co-receptor usage may thereby contribute to the clinical efficacy of anti-HIV drugs in vertically infected infants. 相似文献
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Focal tuberculous lymphadenitis in an HIV-1 infected patient 总被引:1,自引:0,他引:1
Horiba M Takeuchi M Okada C Tada A Kawahara S Mishima Y Soda R Yamashita M Takahashi K 《Internal medicine (Tokyo, Japan)》2002,41(11):1065-1068
A 41-year-old man was admitted to the hospital because of focal swelling of the left supraclavicular lymph nodes. Eighteen months prior to admission, he had been diagnosed with human immunodeficiency virus type 1 (HIV-1) infection and was started on highly active antiretroviral therapy (HAART). He responded well to HAART with an increase in CD4+ cell count and improvement in symptoms. However, one year after the initiation of HAART, he developed progressive enlargement of left supraclavicular lymph nodes. An excisional lymph node biopsy was performed for diagnosis, which revealed tuberculous lymphadenitis. Rifabutin, isoniazid, and ethambutol were initiated for treatment. 相似文献
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Ana M. Rivas-Estilla Eda Ramírez-Valles Ramón Martinez-Hernández Claudia Charles-Niño Ericka Ramírez-Camacho Felix Rositas-Noriega Maria L. Garza-Rodriguez Hugo A. Barrera-Saldaña Karina Trujillo-Murillo Javier Ramos-Jimenez 《Hepatology research》2007,37(5):311-316
Aims: The prevalence of hepatitis C virus (HCV) infection, risk factors and HCV genotypes in 140 HIV-1 infected individuals from northern Mexico was determined. Methods: Hepatitis C infection was confirmed by the detection of anti-HCV antibodies and HCV-RNA in sera, and genotyping was performed by the InnoLiPA-HCV genotype assay. Results: Seventeen (12.1%) out of 140 HIV-infected individuals were found to be HCV-positive. Coinfected individuals were more likely to be male (87%). The most frequent genotype was 1a (41%), followed by 1b (29.4%), 2a/c (17.6%), 2b (5.9%) and 3 (5.9%). Serum transaminase concentrations (AST and ALT) were higher in coinfected patients. Among the risk factors for coinfection: sexual transmission was the most frequently observed (men who have sex with men (MSM); 64.7% and bisexual behavior; 64.7%) followed by intravenous drug users (IVDU) (53%). There was no association of the HCV genotypes with the age and risk factors for HIV-1 and HCV infection observed in the studied patients. Conclusion: The results suggest that the prevalence of HIV-1/HCV coinfection in Mexico is lower than in other American countries. 相似文献
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Moss RB Giermakowska WK Wallace MR Savary JR Jensen FC Carlo DJ 《AIDS (London, England)》2000,14(16):2475-2478
OBJECTIVE: We hypothesized that cell mediated immune responses to an HIV-1 immunogen (whole-killed, gp120-depleted HIV-1 in IFA, REMUNE) would include those to autologous virus. METHODS: Five chronically HIV-1 infected individuals were examined for HIV-specific immune responses to their own virus (autologous viral antigen) after treatment with an HIV-1 immunogen. RESULTS: Subjects had low proliferative responses to HIV and p24 antigens prior to immunization and mounted strong lymphocyte proliferative responses to the immunizing HIV-1 virus, native p24, and autologous viral antigen post immunization. Similarly, subjects produced low amounts of interferon-gamma in response to HIV and p24 antigens prior to immunization and increased their interferon-gamma production in response to HIV-1, native p24, and to autologous antigen post-immunization. Furthermore, beta-chemokine responses measured as migratory inhibitory protein-1beta production were low at baseline in response to HIV-1 and native p24 antigens and were enhanced post immunization to HIV-1, native p24, and autologous antigen. CONCLUSIONS: In this study HIV-specific immune responses to autologous virus were observed after treatment with an HIV-specific immunogen. 相似文献
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Andersson S Norrgren H da Silva Z Biague A Bamba S Kwok S Christopherson C Biberfeld G Albert J 《Archives of internal medicine》2000,160(21):3286-3293
BACKGROUND: The intriguing differences in the natural course, transmissibility, and epidemiological characteristics of human immunodeficiency virus type 1 (HIV-1) and HIV-2 are still insufficiently explained. Differences in plasma viral load are an obvious possibility, but this has been difficult to investigate because of the lack of tests for HIV-2 RNA. OBJECTIVE: To compare plasma HIV RNA load between individuals infected with HIV-1 and HIV-2 in Guinea-Bissau, a West African country with high prevalence and incidence of HIV-1 and HIV-2 infection. METHODS: A total of 102 participants were recruited from ongoing prospective cohort studies. These included 19 HIV-1 and 29 HIV-2 seroincident cases tested at a median of less than 2 years after seroconversion as well as seroprevalent cases with single (9 HIV-1 cases and 31 HIV-2 cases) or dual (n = 14) infections. Plasma HIV RNA levels were determined by a commercial HIV-1 assay and an experimental HIV-2 assay based on the same principles. RESULTS: The viral set point, ie, the semi-equilibrium reached after seronconversion, was 28-fold lower in recent HIV-2 seroconverters than in recent HIV-1 seroconverters (median, 2500 and 70,000 RNA copies per milliliter, respectively; P<. 001). This difference appeared to persist to symptomatic stages of the diseases. Dually infected individuals had lower plasma HIV-1 RNA levels than singly infected individuals. CONCLUSIONS: The differences between HIV-1 and HIV-2 infection are likely to be caused by differences in plasma viral set point and load, but the mechanisms through which HIV-2 infection is contained to a higher degree than HIV-1 remain to be identified. Arch Intern Med. 2000;160:3286-3293. 相似文献
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不同病期HIV-1感染者的病毒学和免疫学研究 总被引:4,自引:0,他引:4
目的了解不同疾病阶段艾滋病病毒Ⅰ型(HIV-1)感染者体内的病毒载量和免疫学变化,探讨其在疾病发展过程中的作用。方法应用核酸序列扩增技术(NASBA)、流式细胞仪和定量酶联免疫吸附试验(ELISA)检测20例正常人、38例HIV无症状感染者、24例HIV有症状感染者和21例艾滋病(AIDS)病人的外周血浆病毒载量、T淋巴细胞亚群和Th1/Th2细胞因子浓度,并结合临床情况进行分析。结果处于不同疾病阶段的HIV无症状感染者、HIV有症状感染者和AIDS病人的血浆病毒载量不同,3组之间有显著性差异(P<0.01),艾滋病组的病毒载量为HIV-RNA 6.04±0.28 log/ml,远远高于HIV无症状组的3.84±0.26 log/ml。3组的CD4 细胞、CD4/CD8比值及IL-2浓度不断下降且明显低于正常人群(P<0.01),Th2细胞因子IL-4和IL-10则明显高于正常人群,且各组之间均有显著性差异(P<0.01)。各因素的相关性分析显示:HIV-RNA与CD4 、CD4/CD8、IL-2,IL-2与IL-4、IL-10,IL-4与IFN-γ、CD4 细胞之间有高度直线负相关关系(P<0.001);HIV-RNA与IL-4、IL-10,CD4 与CD8 、CD4/CD8、IL-2,IL-2与IFN-γ,IL-4与IL-10之间有高度直线正相关关系(P<0.001)。结论不同病期的HIV-1感染者其病毒载量水平、免疫学状况有明显不同。当HIV-RNA升高,CD4 细胞、CD4/CD8比值下降和细胞因子由Th1型为主转变为以Th2型为主时,提示疾病处于进展中。因此,检测这些指标变化可为HIV的临床分期、判断预后和治疗提供依据。 相似文献
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HIV-1 induces phenotypic and functional perturbations of B cells in chronically infected individuals 总被引:3,自引:0,他引:3 下载免费PDF全文
Moir S Malaspina A Ogwaro KM Donoghue ET Hallahan CW Ehler LA Liu S Adelsberger J Lapointe R Hwu P Baseler M Orenstein JM Chun TW Mican JA Fauci AS 《Proceedings of the National Academy of Sciences of the United States of America》2001,98(18):10362-10367
A number of perturbations of B cells has been described in the setting of HIV infection; however, most remain poorly understood. To directly address the effect of HIV replication on B cell function, we investigated the capacity of B cells isolated from HIV-infected patients to respond to a variety of stimuli before and after reduction of viremia by effective antiretroviral therapy. B cells taken from patients with high levels of plasma viremia were defective in their proliferative responses to various stimuli. Viremia was also associated with the appearance of a subpopulation of B cells that expressed reduced levels of CD21. After fractionation into CD21(high)- and CD21(low)-expressing B cells, the CD21(low) fraction showed dramatically reduced proliferation in response to B cell stimuli and enhanced secretion of immunoglobulins when compared with the CD21(high) fraction. Electron microscopic analysis of each fraction revealed cells with plasmacytoid features in the CD21(low) B cell population but not in the CD21(high) fraction. These results indicate that HIV viremia induces the appearance of a subset of B cells whose function is impaired and which may be responsible for the hypergammaglobulinemia associated with HIV disease. 相似文献