干扰素治疗慢性乙型肝炎45例临床观察

目的探讨重组人干扰素α-1b对慢性乙型病毒性肝炎抗病毒的临床治疗效果。方法选择45例慢性乙型肝炎患者为治疗组,另设同期接诊的42例慢性乙型肝炎患者为对照组,治疗组给予干扰素α-1b500万U,对照组给予口服维生素及一般护肝药物,疗程均为6个月,两组病例在治疗前和治疗结束后检测HBV-M、HBV-DNA、肝功能。结果治疗组HbeAg和HBV-DNA转阴率分别为42.22%和46.66%,显著高于对照组。结论干扰素α-1b具有明显的清除和抑制乙型肝炎病毒的作用。

干扰素α-2b治疗48例流行性出血热临床分析

目的观察干扰素α-2b对流行性出血热的疗效及安全性。方法以利巴韦林为对照药,对96例确诊为流行性出血热7病日内的患者,随机分为治疗组(n=48)及对照组(n=48)。治疗组予干扰素α-2b3MU肌内注射,1/d,治疗4d;对照组使用利巴韦林0.8￣1.0g/次,静脉滴注,1/12h,治疗7d。结果治疗组患者主要临床表现消失时间、临床越期、并发症、透析情况及预后与对照组比较,差异有显著性(P<0.05)。结论干扰素α-2b对7病日内的流行性出血热患者安全有效,优于利巴韦林,值得推广应用。

重组干扰素α2b治疗小儿病毒感染性腹泻疗效观察

目的观察重组干扰素α2b治疗小儿病毒感染性腹泻疗效。方法将84例病毒感染性腹泻患儿分为治疗组45例用干扰素α2b治疗,对照组39例用黄连素治疗,疗程均5天。结果治疗组显效17例,有效19例,无效9例,总有效率80%;对照组显效7,有效13例,无效19例,总有效率51.3%。两组比较有显著差异性(P<0.05)。结论重组干扰素α2b是治疗小儿病毒感染性腹泻的有效药物,其疗效与年龄等因素有关。

丙型肝炎病毒血清型对慢性丙型肝炎干扰素抗病毒疗效影响的研究

目的研究丙型肝炎病毒血清型对慢性丙型肝炎于扰素抗病毒疗效的影响。方法对慢性丙型肝炎患者的血清进行ALT检测，采用Cobas amplicor monitor test，version 2．0（v2．0）试剂进行HCVRNA定量和Abbott公司的Murex HCV Serotyping 1-6 Assay试剂进行HCV血清学分型检测。对慢性丙型肝炎患者进行聚乙二醇于扰素a-2a（派罗欣）与罗荛愫（Roferon—A）治疗24周和24周随访结束的生化指标和病毒学应答进行观察，分析不同HCV血清型患者在抗病毒治疗后生化和病毒学应答的差异。结果98例患者共检出血清6型2例、5型1例、4型1例、3型10例、2型23例和1型44例，仍有17例未能分出血清型。派罗欣治疗组24周治疗结束时各血清型和未分型组之间的ALT复常率和病毒应答率无差异，而48周随访结束血清非1型的ALT复常率（76．2％）和持续病毒应答率（66．7％）高于血清1型，血清1型ALT复常率和持续病毒应答率分别为27.3％和27．3％，差异有统计学意义（P=0．035）。罗荛愫组末分型组、血清1型和非1型之间24周治疗结束时和随访结束时的ALT复常率和病毒学应答率均无差异。结论在6个月的IFN抗病毒疗程时，HCV血清型仅在派罗欣治疗组影响慢性丙型肝炎抗病毒治疗的持续病毒应答率。

Hepatitis C virus NS5A region mutation in chronic hepatitis C genotype 1 patients who are non-responders to two or more treatments and its relationship with response to a new treatment

To determine the number of mutations in the NS5A region of the hepatitis C virus (HCV) and its relationship to the response to antiviral therapy in patients with chronic hepatitis C genotype 1 who are non-responders to two or more treatments. METHODSSequences within HCV NS5A [PKR binding domain (PKRBD) and the interferon-sensitivity-determining region (ISDR)] were analysed via direct sequencing in a selected cohort of 72 patients, with a total of 201 treatments [interferon-alpha (IFN-α), n = 49; IFN-α + ribavirin (RBV), n = 75; pegylated (peg) IFN-α + RBV, n = 47; first-generation direct-acting antivirals (DAAs), n = 13; and second-generation DAAs, n = 17]. Of these, 48/201 achieved a sustained virological response (SVR) and 153/201 achieved no virological response (NVR). RESULTSFor both regions, treatments resulting in SVR were associated with more baseline mutations than were treatments resulting in NVR (SVR vs NVR; PKRBD: 5.82 ± 3 vs 4.86 ± 2 mutations, P = 0.045; ISDR: 2.65 ± 2 vs 1.51 ± 1.7 mutations, P = 0.005). A decrease or no change in the number of mutations over time between treatments in the PKRBD or ISDR, as shown by sequencing, was associated with patients who usually failed to respond to treatment (PKRBD, P = 0.02; ISDR, P = 0.001). Moreover, patients showing a post-treatment baseline viral load > 600000 IU/mL and increased ISDR mutations with respect to the previous treatment were 9.21 times more likely to achieve SVR (P = 0.001). CONCLUSIONThe obtained results show that among patients who have shown no response to two or more antiviral treatments, the likelihood of achieving SVR increases with the genetic variability in the ISDR region (≥ 2 mutations or number of substitutions from the HCV-J and HCV-1 prototype), especially when the viral load is greater than 600000 IU/mL.

UVB诱导皮肤免疫抑制和表没食子儿茶素没食子酸酯光保护作用

目的探讨表没食子儿茶素没食子酸酯(EGCG)对不同剂量中波紫外线(UVB)慢性辐射BALB/c小鼠皮肤的保护作用。方法EGCG局部外用于小鼠背部皮肤后予不同强度UVB辐射,每日1次,连续1个月,RT-PCR法检测IFN-γ和IL-10 mRNA的表达水平变化。结果不同剂量UVB慢性辐射后小鼠皮肤中IFN-γmRNA表达水平较对照组降低(P＜0．01),IL-10 mRNA表达水平较对照组升高(P＜0．01),并与UVB辐射强度呈一定剂量依赖关系。EGCG处理后可影响UVB辐射诱导上述细胞因子表达(P＜0．01)。结论UVB辐射下调IFN-γ和上调IL-10转录水平,可能与UVB辐射诱导局部免疫抑制有关。