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Occult HBV infection

机译:隐匿性HBV感染

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The presence of hepatitis B virus genome in HBsAg-negative subjects is known as “occult infection” from HBV. Patients with occult infection may express markers of previous exposure to B virus (anti-HBs and / or anti-HBc positive). 20% is negative for all HBV markers except for the presence of HBV-DNA. Occult infection is associated with a strong suppression of viral replication that is responsible for both HBsAg negativity and the very low or undetectable HBV-DNA in serum but seen in the liver tissue. The pathogenesis of occult infection is considered multifactorial. Infection by mutants of HBV (HBsAg mutants), suppression of viral replication and expression of genes of HBV, HBV-DNA integration into the host genome, infection of HBV in mononuclear peripheral blood, abnormalities of the immune response, interference with other virus. HBV DNA with high sensitivity and specificity, can shorten the “window period” elapses between exposure to infection and responsiveness to the serological test.The presence of mutant HBV amino acid substitution of the determinant “a” gene “S” epitope of the surface protein of the virus, causes conformational changes that alter the binding with the specific antibody. Aim of this work is to assess negative or borderline subjects of HbsAg, with moderate increases of transaminase levels but - positive to HBV DNA test. The serological markers of HBV were determined with Architect (Abbott).The HBV-DNA was evaluated in Real-Time PCR Cobas TaqMan 48 (Roche) a quantitative test that detects the viral concentration. 15350.12 (0.07%) were positive for HBV-DNA test., 3 positive for HBsAg, 9 negative HBV markers showed anti-HBc reactivity in all 12 anti-HBe in 3, 4 anti-HBs with a titer of 13UI/ml.Le ALT were altered only for 2 to 12 and was detected viremia below the sensitivity test (<6 IU / ml).These data allow to draw some considerations: - Screening tests for infection with HBV do not show the “window period”.The slow replication of HBV with low viremia in the initial phase involves the impossibility of identifying HBsAg in serological screening, but detected by molecular biology tests. - The “window period”, the carrier state immunosilent chronic, low levels of viral proteins do not detect the infection. - Data in literature indicate the presence of different mutant strains of HBV characterized by altered expression of the antigenic determinant “a” of HbsAg. - The majority of screening tests for detection of HBsAg using monoclonal antibodies for the identification of the determinant “a” is needed to identify the different mutants using a mixture of monoclonal antibodies capable of recognizing even the most conserved regions.The gold standard methods to detect the mutant viruses are the techniques of molecular biology and the direct sequencing.
机译:HBsAg阴性受试者中乙型肝炎病毒基因组的存在被称为HBV的“隐性感染”。隐匿性感染患者可能表达先前暴露于B病毒的标志物(抗HBs和/或抗HBc阳性)。除HBV-DNA存在外,所有HBV标记均为20%阴性。隐匿性感染与病毒复制的强烈抑制有关,病毒复制导致HBsAg阴性和血清中很低或无法检测到的HBV-DNA,但在肝组织中可见。隐匿性感染的发病机理被认为是多因素的。感染HBV突变体(HBsAg突变体),抑制病毒复制和HBV基因表达,HBV-DNA整合入宿主基因组,在单核外周血中感染HBV,免疫应答异常,对其他病毒的干扰。具有高灵敏度和特异性的HBV DNA可以缩短暴露于感染与血清学检测反应之间的“窗口期”。表面蛋白决定簇“ a”基因“ S”表位的突变HBV氨基酸取代的存在病毒引起的构象变化会改变与特定抗体的结合。这项工作的目的是评估HbsAg阴性或临界受试者,转氨酶水平适度升高,但对HBV DNA测试呈阳性。 HBV的血清学标志物由Architect(Abbott)确定.HBV-DNA在Real-Time PCR Cobas TaqMan 48(Roche)中进行定量检测,以检测病毒浓度。 HBV-DNA试验阳性15350.12(0.07%)。HBsAg阳性3,HBsAg阴性9标志在3、4抗HBs中的所有12种抗HBe中均具有抗HBc反应性,滴度为13UI / ml.Le ALT仅改变了2到12,并在低于敏感性试验(<6 IU / ml)的情况下被检测出病毒血症。这些数据可以引起一些考虑:-HBV感染的筛查试验未显示“窗口期”。在初期,低病毒血症的HBV复制就涉及不可能在血清学筛查中鉴定HBsAg,但可以通过分子生物学测试进行检测。 -在“窗口期”,携带者免疫沉默的慢性,低水平的病毒蛋白无法检测到感染。 -文献中的数据表明存在不同的HBV突变株,其特征在于HbsAg抗原决定簇“ a”的表达改变。 -需要使用大多数单克隆抗体来鉴定行列式“ a”的筛查试验,以使用能够识别甚至最保守区域的单克隆抗体混合物来鉴定不同的突变体。金标准的检测方法突变病毒是分子生物学技术和直接测序技术。

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