Inactivated influenza vaccine formulated with single-stranded RNA-based adjuvant confers mucosal immunity and cross-protection against influenza virus infection

Influenza vaccination is considered the most valuable means to prevent and control seasonal influenza infections, which causes various clinical symptoms, ranging from mild cough and fever to even death. Among various influenza vaccine types, the inactivated subunit type is known to provide improved safety with reduced reactogenicity. However, there are some drawbacks associated with inactivated subunit type vaccines, with the main ones being its low immunogenicity and the induction of Th2-biased immune responses. In this study, we investigated the role of a single-stranded RNA (ssRNA) derived from the intergenic region in the internal ribosome entry site of the Cricket paralysis virus as an adjuvant rather than the universal vaccine for a seasonal inactivated subunit influenza vaccine. The ssRNA adjuvant stimulated not only well-balanced cellular (indicated by IgG2a, IFN-γ, IL-2, and TNF-α) and humoral (indicated by IgG1 and IL-4) immune responses but also a mucosal immune response (indicated by IgA), a key protector against respiratory virus infections. It also increases the HI titer, the surrogate marker of influenza vaccine efficacy. Furthermore, ssRNA adjuvant confers cross-protective immune responses against heterologous influenza virus infection while promoting enhanced viral clearance. Moreover, ssRNA adjuvant increases the number of memory CD4⁺ and CD8⁺ T cells, which can be expected to induce long-term immune responses. Therefore, this ssRNA-adjuvanted seasonal inactivated subunit influenza vaccine might be the best influenza vaccine generating robust humoral and cellular immune responses and conferring cross-protective and long-term immunity.     

The Current Role of Calcineurin Inhibitors in Posttransplant Immunosuppression?

It is important to determine when to use and when to avoid calcineurin inhibitors (CNIs). CNIs are associated with kidney dysfunction in some, but not all, transplant recipients. CNI-sparing protocols have their own drug-specific limitations. Two major clinical series suggest the benefit of routine CNI-sparing approaches, but our review suggests weaknesses in both. Ongoing studies are needed to determine which subgroups of recipients will benefit from CNIs.     

血管生成抑制剂YH-16联合氟尿嘧啶抑制结直肠癌肝转移的研究

目的探讨血管生成抑制剂YH-16和氟尿嘧啶（5-FU）联合应用对结直肠癌肝转移的抑制作用。方法用MTT方法测定血管生成抑制剂YH-16和5-FU对血管内皮细胞和结肠癌细胞的IC50；建立小鼠肝转移模型。随机分为对照组、YH-16组（又分为低、中、高剂量3组）和5-Fu组及联合治疗组（YH-16加5-FU），术后2周观察各组小鼠肝转移瘤数目、原发灶大小和毒性反应。并检测肝转移瘤血管内皮生长因子（VEGF）的表达和肿瘤微血管密度（MVD）。结果YH-16对结肠癌细胞的IC50是血管内皮细胞的3．38倍，而5-Fu对两种细胞的IC50差别不大。高剂量YH-16组、5-FU组和联合治疗组肝转移瘤数目明显低于对照组。而联合治疗组又低于高剂量YH-16组和5-FU组（均P〈0．05）。YH-16各剂量组的脾原发瘤体积与对照组比较均P〉0．05。差异无统计学意义；而5-FU组和联合治疗组则小于对照组（均P〈0．05）。YH-16的毒性明显低于5-FU（P〈0．05），且两者联合使用其毒性与单用5-FU比较，差异无统计学意义（P〉0．05）。5-FU组和联合治疗组肝转移瘤组织中VEGF的表达明显降低，中、高剂量YH-16组和5-FU组及联合治疗组肝转移瘤组织中的MVD计数明显降低（均P〈0．05）。结论血管生成抑制剂YH-16明显抑制结直肠癌肝转移，YH-16与5-FU联合应用对结直肠癌肝转移的抑制具有协同作用。     

Preliminary laboratory based diagnostic criteria for immune thrombocytopenic purpura: evaluation by multi-center prospective study

BACKGROUND: We proposed diagnostic criteria for immune thrombocytopenic purpura (ITP) by modifying the existing guidelines for diagnosis of ITP and by incorporating laboratory tests found useful for predicting its diagnosis, for example erythrocyte count, leukocyte count, anti-GPIIb/IIIa antibody-producing B cells, platelet-associated anti-GPIIb/IIIa antibodies, percentage of reticulated platelets, and plasma thrombopoietin. OBJECTIVE AND METHODS: To validate our criteria, we conducted a multi-center prospective study involving 112 patients with thrombocytopenia and a morphologically normal peripheral blood film at the first visit. Each patient underwent a physical examination, routine laboratory tests, and specialized tests for the anti-GPIIb/IIIa antibody response and platelet turnover. RESULTS: Ninety-one patients (81%) satisfied the proposed criteria at first visit. Clinical diagnosis was made by skilled hematologists > 6 months after the first visit; ITP was diagnosed in 88 patients and non-ITP disorders in 24. The proposed criteria had 98% sensitivity, 79% specificity, a 95% positive predictive value, and a 90% negative predictive value. A relatively low specificity appears to be attributed to a few patients who had both ITP and aplastic anemia or myelodysplastic syndrome. CONCLUSIONS: Our preliminary diagnostic criteria based on ITP-associated laboratory findings were useful for the differential diagnosis of ITP, but additional evaluations and modifications will be necessary to develop criteria that can be used routinely.     

Economic Issues in the Treatment of BPH

The long-term cost of effective management for benign prostatic hyperplasia (BPH) remains an important issue in pharmacoeconomics because about 25% of men aged 50 yr and older experience voiding problems due to BPH. With the ageing population and the increase in the percentage of patients with BPH for whom any type of treatment can be considered, a substantial increase in total costs to society can be expected. The up-front costs of interventional approaches to BPH are being replaced by a pattern of long-term medical and preventive therapy. The age-adjusted rate of transurethral resection of the prostate (TURP) reached a high point in 1987 and TURP rates, but not costs, have been in decline ever since. Mean 1-yr treatment costs (medical therapy and TURP) have been estimated in a pan-European study to be 858 Euros per patient, 75% of which were medication costs. Using a 2-yr time frame for treatment, Medicare costs for finasteride, terazosin, and TURP have been estimated as $3874, $2161, and $1820, respectively. The available models of the total long-term cost for all therapies for BPH remain compromised by a lack of inclusion of indirect costs, the lack of true long-term data and, critically, the lack of human cost information (patient preference). Only medical therapy provides a preventive as well as symptomatic potential and, if all of the issues were fully incorporated, it is likely that medical therapy would be increasingly recognised as economically preferable.     

转hCTLA4Ig树突状细胞诱导T细胞免疫耐受的实验研究

目的　通过逆转录病毒载体将人CTLA4Ig转染DCs ,探讨转人CTLA4Ig(hCTLA4Ig)树突状细胞 (DCsRev)诱导T细胞免疫耐受的可能性。方法　通过重组逆转录病毒将目的基因hCTLA4Ig转染到大鼠骨髓来源的DCs中 ,通过流式细胞检测目的基因hCTLA4Ig表达及DCs表面分子的改变 ;通过混合淋巴细胞反应 (MLR)检测DCsRev抑制T细胞免疫反应的能力。 结果　重组逆转录病毒转染DCs的最大效率为 91 2 5 % ;在功能上 ,DCsRev不但丧失了刺激MLR的能力 ,并且能够强烈抑制MLR中反应T细胞的增殖 ,而且抑制率与加入DCsRev的数量和DCsRev预处理反应T细胞的时间长短有关。具体来说 ,DCsRev数量在 10 3 ～ 10 4之间时 ,抑制率与剂量呈正相关 ,最高为 71 96%。而当DCsRev数量达到 5× 10 4抑制率下降为 5 9 2 %。在 12～ 48h之间 ,随着预处理时间的延长 ,抑制率却不断下降 ,预处理 12h抑制率最高 ,为 99 6%。但不做预处理 ,在反应开始时同时加入DCsRev ,则抑制率明显降低 ,仅为 5 9 2 %。对腹腔注射DCsRev大鼠脾T淋巴细胞体外分析表明 ,DCsRev也能在动物体内诱导耐受 ,但这种免疫耐受状态不能维持终身。结论　通过逆转录病毒载体将人CTLA4Ig转染DCs,不但DCs表面CD86分子被CTLA4Ig有效的封闭 ,并且能够诱导抗原特异性T细胞的免疫耐受     

CpG DNA预防小鼠哮喘模型的形成

目的　研究含胞嘧啶鸟嘌呤核苷酸的免疫刺激元件 (CpGDNA)能否预防卵蛋白致敏小鼠哮喘模型的形成。方法　将 18只BALB/c小鼠均分为 3组 ,其中卵蛋白致敏哮喘组 (OVA组 )和CpG预防组 (CpG组 )皮下注射卵蛋白致敏制作哮喘模型 ,然后用卵蛋白激发 2次 ;阴性对照组 (NS组 )皮下注射生理盐水 ,然后生理盐水激发 2次。CpG组在致敏前腹腔注射CpGDNA 10 0 μg/ 10 0 μL ,其他两组不作干预。 3组分别在第 2次激发后 2 4h测外周血OVA特异性IgE、IgG1、IgG2a,并处死小鼠测肺泡灌洗液 (BALF)中的细胞总数及嗜酸性粒细胞 (EOS)计数 ,肺组织病理切片观察形态学改变 ,并测定脾细胞培养上清液中OVA特异性IFN γ。结果　CpG组BALF中细胞总数和嗜酸性粒细胞明显低于OVA组 ,P <0 .0 5 ;CpG组肺组织炎症反应较OVA组明显减轻 ;CpG组脾细胞培养上清液中OVA特异性IFN γ的浓度明显高于OVA组 ,P <0 .0 5 ;CpG组外周血OVA特异性IgE和IgG1均低于OVA组 ,P <0 .0 5 ;CpG组IgG2a较OVA组为高 ,P <0 .0 5。结论　CpGDNA能预防卵蛋白致敏小鼠哮喘模型的形成     

核酸及核苷酸用于营养及免疫调节治疗的早期卫生技术评估

目的 评价核酸或核苷酸用于临床营养支持和免疫调节治疗的安全性、有效性和经济学价值。方法 检索中国生物医学文献数据库、Cochrane图书馆、MEDLINE光盘数据库、EMBASE光盘数据库,并联机检索SCI数据库,鉴定有关随机对照试验(RCTs),采用RevMan4.l进行Meta-分析。结果 纳入46个随机对照试验,涉及核酸/核苷酸用于肠内营养支持、婴儿营养、免疫调节治疗。18个研究报告了含核苷酸组分的免疫增强型肠内营养对外科术后和危重症患者预后的影响,合并分析发现免疫营养对患者感染率、住院时间和费用有肯定意义。发现1个报告在母乳代用品中加入核苷酸对婴儿免疫功能影响的研究,但报告对临床结局无明显影响。27个对“免疫核酸”用于免疫调节治疗的随机对照试验均为低质量研究,合并分析无法肯定iRNA的临床价值。结论 在外科术后患者应用免疫肠内营养制剂可降低感染率、缩短住院时间并可能减少住院费用,但不能确定作为组分之一的核苷酸的作用。尚无证据支持在母乳代用品中添加核苷酸具有临床意义。不能肯定免疫核酸是否具有免疫调节作用,亦未发现核酸在延缓衰老、改善老年人健康状况方面的可用证据。建议对核酸、核苷酸用于营养支持治疗和免疫调节治疗进行进一步研究,严格规范“核酸营养品”的宣传和应用。