Inhibition of Rgs10 Expression Prevents Immune Cell Infiltration in Bacteria-induced Inflammatory Lesions and Osteoclast-mediated Bone Destruction

Regulator of G-protein Signaling 10 （Rgsl0） plays an important function in osteoclast differentiation. However, the role of Rgsl0 in immune cells and inflammatory responses, which activate osteoclasts in inflam- matory lesions, such as bacteria-induced periodontal disease lesions, remains largely unknown. In this study, we used an adeno-associated virus （AAV-） mediated RNAi （AAV-shRNA-Rgs10） knockdown approach to study Rgsl0＇s function in immune cells and osteoclasts in bacteria-induced inflammatory lesions in a mouse model of periodontal disease. We found that AAV-shRNA-Rgs10 mediated Rgs10 knockdown impaired osteoclastogenesis and osteoclast-mediated bone resorption, in vitro and in vivo. Interestingly, local injection of AAV-shRNA-Rgs10 into the periodontal tissues in the bacteria-induced inflammatory lesion greatly decreased the number of dendritic cells, T-cells and osteoclasts, and protected the periodontal tissues from local inflammatory damage and bone destruction. Importantly, AAV-mediated Rgs10 knockdown also reduced local expression of osteoclast markers and pro-inflammatory cytokines. Our results demonstrate that AAV- shRNA-Rgs10 knockdown in periodontal disease tissues can prevent bone resorption and inflammation simultaneously. Our data indicate that Rgsl0 may regulate dendritic cell proliferation and maturation, as well as the subsequent stimulation of T-cell proliferation and maturation, and osteoclast differentiation and acti- vation. Our study suggests that AAV-shRNA-Rgs10 can be useful as a therapeutic treatment of periodontal disease.

Glycosylation-independent binding to extracellular domains 11-13 of mannose-6-phosphate/insulin-like growth factor-2 receptor mediates the effects of soluble CREG on the phenotypic proliferation of vascular smooth muscle cells

Background The present study aimed to investigate the detailed mode and specific sites for their binding as well as the functional relevance of this binding in the phenotypic proliferation of vascular smooth muscle cells(SMCs). Methods CREG knocked-down SMCs were employed to evaluate the biological activity of wtCREG and mCREG.Expressions of SMC differentiation markers SM myosin heavy chain(SM-MHC),SM-actin,heavy caldesmon and myocardin were determined by Western blotting using specific antibodies. Cellular growth of SMCs was assessed by bromide dewuridine (BrdU) incorporation and cell cycle analysis on fluorescence-activated cell sorting(FACS).A solid-phase binding assay was used to study the binding of CREG to extracellular domains of M6P/IGF2R.The cellular co-localization of the two recombinant CREGs with M6P/IGF2R was detected on SMC surface by immunoprecipitation and immunofluorescence analysis.Results The molecular weight of wtCREG was around 30 kD while that of the mCREG was～25 kD.Treatment of wtCREG with PNGase F reduced its molecular weight from～30 kD to～25 kD,whereas PNGase F treatment had no effect on the molecular weight of mCREG.Both wtCREG and mCREG proteins enhanced SMC differentiation,inhibited BrdU incorporation,and arrested cell cycle progression when added to the culture medium.In CREG knocked-down SMCs,the amount of CREG detected by immunoblotting in M6P/IGF2R immunoprecipitates was significantly reduced when compared to normal cells.Both recombinant CREGs co-immunoprecipitated with M6P/IGF2R, although slightly reduced amount of the mutant CREG was detected in M6P/IGF2R immunoprecipitates.Immunostaining revealed that His-tagged CREGs co-localized with IGF2R on the cell surface in a glycosylation-independent manner.In vitro binding assay showed that CREGs bound to M6P/ IGF2R extracellular domains 7-10 and 11-13 in a glycosylation -dependent and -independent manner,respectively.Further blocking experiments using soluble M6P/IGF2R fragments and M6P/IGF2R neutralizing antibody indicated that the biological activities of recombinant CREGs in SMC growth and the up-regulation of SMC differentiation markers were all abolished by treatment with the M6P/IGF2R neutralizing antibody. However,although the growth inhibitory effect of wtCREG was nearly abolished by D7-10 or D11-13,the effect of mCREG was only reversed by Dll-13,indicating that the binding to domains 11-13 is required for CREG to modulate the proliferation of SMCs.Conclusions These data suggest that solubleCREG proteins can exert their biological function via binding to the extracellular domains 7-10 and 11-13 of cell surface M6P/IGF2R in both a glycosylation-dependent and -independent manner.

Effect of TCM Combined with Chemotherapy on Immune Function and Quality of Life of Patients with Non-small Cell Lung Cancer inStage Ⅲ-Ⅳ

Objective: To observe and compare the effect of traditional Chinese medicine (TCM) combined with chemotherapy (CT) on immune function and quality of life (QOL)of patients with non-small cell lung cancer (NSCLC) in stage Ⅲ-Ⅳ. Methods: One hundred cases with stage Ⅲ-Ⅳ NSCLC were randomly divided into two groups. The treated group (n=50) received CT combined with TCM, and the control group received CT alone. The percentage of T lymphocyte subset in peripheral blood and the change of natural killer (NK) cell count were observed after treatment. The QOL and tolerance of CT were also compared between the two groups after treatment. Results: In the treated group, CD3 cell count, CD4 cell count, CD4/ CDg ratio and NK cell activity were higher than those in control group, while CD8 cell count in the treated group was lower than that in the control group (P<0.05), and QOL and tolerance of CT in the treated group were also better (P<0.05). Conclusion: TCM combined with CT could raise the patients' ability in tolerating CT in stage Ⅲ-ⅣNSCLC.

低剂量白细胞介素-2在免疫相关性皮肤病中的研究进展

免疫相关性皮肤病是一类因自身免疫耐受破坏导致的皮肤病,包括红斑狼疮、皮肌炎等。调节性T细胞与效应性T细胞之间失衡在免疫相关性皮肤病发病机制中起重要作用。低剂量白细胞介素-2可优先激活调节性T细胞,逆转调节性T细胞与效应性T细胞失衡,恢复免疫耐受,在免疫相关性皮肤病的治疗领域中逐渐受到关注。本文综述了低剂量白细胞介素-2的免疫调控机制及临床研究进展,为免疫相关性皮肤病的治疗提供新的思路。

Atherosclerosis and the role of immune cells

Atherosclerosis is a chronic inflammatory disease arising from lipids, specifically low-density lipoproteins, and leukocytes. Following the activation of endothelium with the expression of adhesion molecules and monocytes, inflammatory cytokines from macrophages, and plasmacytoid dendritic cells, high levels of interferon(IFN)-α and β are generated upon the activation of tolllike receptor-9, and T-cells, especially the ones with Th1 profile, produce pro-inflammatory mediators such as IFN-γ and upregulate macrophages to adhere to the endothelium and migrate into the intima. This review presents an exhaustive account for the role of immunecells in the atherosclerosis.

Role of T cell death in maintaining immune tolerance during persistent viral hepatitis

Virus-specific T cells play an important role in the resolution of hepatic infection. However, during chronic hepatitis infection these cells lack their effector functions and fail to control the virus. Hepatitis B virus and hepatitis C virus have developed several mechanisms to generate immune tolerance. One of these strategies is the depletion of virus-specific T cells by apoptosis. The immunotolerogenic liver has unique property to retain and activate na ve T cell to avoid the over reactivation of immune response against antigens which is exploited by hepatotropic viruses to persist. The deletion of the virus-specific T cells occurs by intrinsic (passive) apoptotic mechanism. The pro-apoptotic molecule Bcl-2 interacting mediator (Bim) has attracted increasing attention as a pivotal involvement in apoptosis, as a regulator of tissue homeostasis and an enhancer for the viral persistence. Here, we reviewed our current knowledge on the evidence showing critical role of Bim in viral-specific T cell death by apoptotic pathways and helps in the immune tolerance.

Alpha-fetoprotein specific CD4 and CD8 T cell responses in patients with hepatocellular carcinoma

The presence of CD8 T cell responses to tumor associated antigens have been reported in patients with different malignancies. However, there is very little inf ormation on a comparable CD8 and CD4 T cell response to a tumor antigen in liver cancer patients. Here, we re-examine the kinetic and the pattern of T helper 1 and cytotoxic T lymphocyte responses to alpha-fetoprotein (AFP),a tumor rejection antigen in hepatocellular carcinoma (HCC). Then, we discuss the possibility of using AFP-based immunotherapy in combination with necrotizing treatments in HCC patients.

Immune checkpoint inhibitor-induced colitis:A comprehensive review

Immune checkpoint inhibitors(ICIs) are monoclonal antibodies that target downregulators of the anti-cancer immune response: Cytotoxic T-lymphocyte antigen-4, programmed cell death protein-1, and its ligand programmed death-ligand 1.ICIs have revolutionized the treatment of a variety of malignancies. However,many immune-related adverse events have also been described which mainly occurs as the immune system becomes less suppressed, affecting various organs including the gastrointestinal tract and causing diarrhea and colitis. The incidence of immune-mediated colitis(IMC) ranges from 1%-25% depending on the type of ICI and if used in combination. Endoscopically and histologically there is a significant overlap between IMC and inflammatory bowel disease,however more neutrophilic inflammation without chronic inflammation is usually present in IMC. Corticosteroids are recommended for grade 2 or more severe colitis while holding the immunotherapy. About one third to two thirds of patients are steroid refractory and benefit from infliximab. Recently vedolizumab has been found to be efficacious in steroid and infliximab refractory cases. While in grade 4 colitis, the immunotherapy is permanently discontinued, the decision is controversial in grade 3 colitis.

Cancer Immunothearapy More than Vaccines “Psychoneuro-Immunooncology: Cancer, the Host, and the Surgeon”

Cancer immunology is extremely complex with numerous interactions between the tumor and the host. It is time for those that treat cancer, especially surgeons, to learn more about these complex interactions. We need to know more about host immunity and immunosuppressive mechanisms which are not directly related to the disease, but caused by stress and therapy of the disease. The diagnosis of cancer initiates stress that can be very detrimental to the host immune system. Most cancer physicians (surgical, medical, and radiation oncologist) do not appreciate the impact on host cell mediated immunity (CMI) caused by cancer therapy, and definitely do not know how devastating, psychic stress is on host immunity. This communication is an attempt to bring awareness to this problem.

Acute Morphine Administration Reduces Cell-Mediated Immunity and Induces Reactivation of Latent Herpes Simplex Virus Type 1 in BALB/c Mice

Acute morphine administration is known to alter the course of herpes simplex virus infection. In this study, the effect of acute morphine administration on the reactivation of latent herpes was investigated in a mouse model. Because of the important role of cytolytic T lymphocyte （CTL） activity in the inhibition of herpes simplex virus type 1 （HSV-1） reactivation, the effect of acute morphine administration on CTL responses was also evaluated. Furthermore, lymphocyte proliferation and IFN-γ production were evaluated for their roles in the induction of the CTL response. The findings showed that acute morphine administration significantly reduced CTL responses, lymphocyte proliferation, and IFN-γ production. Furthermore, acute morphine administration has been shown to reactivate latent HSV-γ. Previous studies have shown that cellular immune responses have important roles in the inhibition of HSV reactivation. These findings suggest that suppression of a portion of the cellular immune response after acute morphine administration may constitute one part of the mechanism that induces HSV reactivation.

Identification of a T-cell epitope in the <i>Staphylococcus aureus</i>Panton-Valentine LukS-PV component

We previously observed the elicitation of a significant delayed-type hypersensitivity response to the Panton-Valentine leukocidin (PVL) LukS-PV subunit following subcutaneous immunization (Brown et al., Clinical Microbiology and Infection, 2009, 156: 156-164). A LukS-PV-specific cell line (LST) was screened for proliferative responses against a panel of 25 amino acid-long peptides spanning the length of LukS-PV (amino acids 29-312). This analysis demonstrated that stimulation of LST with LukS-PV resulted in significant proliferative responses and adoptive transfer of LST into na?ve mice conferred a LukS-PV-specific DTH response following challenge. Challenge of mice adoptively transferred with LST with peptides 7 (149-173), 8 (169-193) and 14 (289-312) also elicited a measurable DTH response suggesting that these peptides contained T cell epitopes.

肥大细胞在哮喘发生发展中的作用机制及中医药调控作用

哮喘在中医学中属于哮病、喘症的范畴,是以气道平滑肌收缩、免疫细胞浸润和气道重塑等为特征的气道炎症疾病。肥大细胞为非特异性免疫细胞,在哮喘的形成和发展中扮演关键角色。中医药对哮喘的防治具有独特优势,但具体机制尚不明确。通过对相关研究综述后发现,肥大细胞活化后释放的组胺、蛋白酶、细胞因子等介质在哮喘气道损伤及重塑的病理过程中起重要作用。此外,中药复方制剂、单味中药及其活性成分、中成药及中医外治法等中医药方法可通过调节肥大细胞活化,抑制多种炎症介质和细胞因子的表达,进而发挥对哮喘的治疗作用。

Immune-mediated neuromuscular complications after haploidendtical hematopoietic stem cell transplantation

Allogeneic hematopoietic stem cell transplantation （Allo-HSCT） is associated with neuromuscluar complications in fewer than 5% of patients.1 The most common causes are associated with the toxicity of the conditioning regimen,infections,bleeding,and malignant disease relapse.Allo-HSCT related neuromuscular complications can also be caused by immune-mediated mechanisms,which are usually present in the form of myositis/polymyositis or demyelinating polyneuropathy.Keywords：allogeneic hematopoietic stem cell transplantation; immune mediated; chronic demyelinating polyneuropathy;steroid myopathy

淫羊藿-蜂胶合剂对雏鸡细胞免疫功能的影响

３日龄雏鸡皮下注射淫羊藿－蜂胶合剂，于７，２１，３５，４９日龄分别采用微量全血＾３Ｈ－胸腺嘧啶核苷掺入法和乳酸脱氢酸（ＬＤＨ）释放法测定雏鸡外周血Ｔ淋巴细胞转化率和自然杀伤细胞（ＮＫ）活力。注射剂量０．４ｍｌ／羽能极显著地提高２１日龄和３５日龄雏鸡Ｔ淋巴细胞转化率和３５日龄雏鸡ＮＫ活力。０．２ｍｌ／羽与０．４ｍｌ／羽作用相似。０．４ｍｌ／羽效果优于０．２ｍｌ／羽，结果表明。

C3d-P28增强乙肝病毒基因免疫诱导的特异性细胞免疫应答

目的 :研究补体C3d中P2 8分子对HBV基因免疫诱导的细胞免疫应答的调节作用 ,为增强基因疫苗细胞免疫的效果寻求新方法。方法 :分别分离获取C3d P2 8和HBV preS2 /S编码基因 ,并克隆入真核表达载体 pVAON33中 ,构建相应重组质粒pVAON33 S2 /S (仅含HBV preS2 /S编码基因 )和pVAON33 S2 /S P2 8.4 (含HBV preS2 /S和 4拷贝C3d P2 8的编码基因 ) ,并以PCR、酶切和DNA序列测定进行鉴定。以肌肉注射法对BALB/c小鼠实施 3次基因免疫 ( 10 0 μg/10 0 μL·只 ) ,间隔 3wk ,并以空质粒免疫小鼠作为对照。免疫小鼠脾细胞体外经HBsAg刺激后 ,用3 H TdR掺入法和同位素释放法 ,分别检测特异性淋巴细胞增殖和CTL杀伤活性。结果 :pVAON33 S2 /S和 pVAON33 S2 /S P2 8.4免疫小鼠的脾细胞 ,均显示较强的特异性增殖活性和CTL杀伤活性 ,但后者显著强于前者 (P <0 .0 5 )。结论 :C3d P2 8可增强HBV preS2

乙型肝炎病毒前S1抗原(1-42)与核心抗原(1-144)在大肠杆菌中表达的融合蛋白CS1的免疫原性研究

对重组乙型肝炎 (乙肝 )病毒前S1抗原 (1- 42 )及核心抗原 (1- 144 )表达的融合蛋白CS1进行了免疫原性的研究分析 ,以便为探索HBV治疗性疫苗的研制提供实验依据。用脂质体转染的方法转染小鼠肥大细胞瘤细胞系P815 ,用乳酸脱氢酶的方法检测了该融合蛋白诱导小鼠的细胞毒T淋巴细胞 (CTL)反应 ,用ELISA方法测定了小鼠的体液免疫反应。结果表明 ,用脂质体转染的方法建立了表达乙肝核心和前S1抗原的细胞系 (P99- 815 ) ,该融合蛋白诱导出小鼠的细胞毒T淋巴细胞 (CTL)反应 ,小鼠的体液免疫反应也较好。这为今后进一步探索慢性乙肝治疗性疫苗奠定了必要的基础。

鸭IFN-α真核表达质粒基因枪免疫对鸭瘟弱毒疫苗免疫鸭细胞免疫调节作用初探

为探索鸭α干扰素(IFN-α)真核表达质粒(pcDNA-SDIFN-α)对鸭瘟弱毒疫苗免疫鸭的细胞免疫调节作用,本研究将pcDNA-SDIFN-α以1、3和6μg/只3个剂量用基因枪轰击法分别免疫28日龄鸭,以PBS和空载体质粒pcDNA3.1(+)为对照,所有鸭15 d后接种鸭瘟(DP)弱毒疫苗。接种后第3、7、14、21、28、35、49、63、84天采血用淋巴细胞增殖试验(MTT法)测定鸭外周血中T淋巴细胞转化效果;第7、14、21、28、35、49天采血用流式细胞仪(FACS)测定CD3+T淋巴细胞数量的动态变化。结果发现:①T淋巴细胞对ConA的反应能力(OD值),不同剂量pcDNA-SDIFN-α免疫组鸭外周血T淋巴细胞转化功能于第3-84天均高于PBS和空载体pcDNA对照组,其中第3-84天1μg/只组极显著(P≤0.01)高于PBS和pcDNA对照组,3μg/只组极显著(P≤0.01)或显著(P≤0.05)高于PBS和pcDNA对照组,6μg/只组于第7-49天极显著(P≤0.01)或显著(P≤0.05)高于PBS和pcDNA对照组;1μg/只组第3-35天显著(P≤0.05)高于3、6μg/只组;3μg/只组于第14-35天高于6μg/只组,但差异不显著(P≥0.05);pcDNA对照组略高于PBS对照组,但差异不显著(P≥0.05);②CD3+T淋巴细胞数量变化,不同剂量pcDNA-SDIFN-α免疫组鸭于第7-49天均高于PBS和pcDNA对照组,其中1μg/只组于第14-49天极显著(P≤0.01)高于PBS和pcDNA对照组,3μg/只组于第21-49天极显著(P≤0.01)高于PBS对照组和显著(P≤0.05)高于pcDNA对照组,6μg/只组于第7-49天显著(P≤0.05)或极显著(P≤0.01)高于PBS和pcDNA对照组;1、3和6μg/只组之间差异不显著(P≥0.05);pcDNA组于第14-49天高于PBS组,但差异不显著(P≥0.05)。研究表明,pcDNA-SDIFN-α提前15 d免疫能显著增强DP弱毒疫苗诱导的鸭细胞免疫力,以基因枪免疫1μg/只的效果最佳,它是一种良好的增强DP弱毒疫苗细胞免疫的分子佐剂。

柯萨奇3m病毒和T-2毒素致小鼠慢性心肌损伤细胞免疫功能改变

目的观察慢性心肌损伤过程中小鼠细胞免疫功能的改变。方法BALB/C小鼠随机分成4组,病毒(柯萨奇3m,CVB3m)组、毒素(T鄄2)+病毒组、毒素组和对照组。观察各组小鼠脾淋巴细胞亚群及其在刀豆蛋白A(CoA)刺激下增殖及白细胞介素鄄2(IL鄄2)的分泌水平。结果毒素+病毒组小鼠心肌形成慢性损伤,感染病毒7 d时,毒素+病毒组脾淋巴细胞亚群、淋巴细胞增殖反应及IL鄄2的分泌水平均低于病毒组,14 d后虽有不同程度的提高,但低于病毒组最高值。结论T鄄2毒素染毒小鼠感染CVB3m后,心肌出现慢性损伤,这可能是由于淋巴细胞数量、功能和活性异常,细胞免疫功能紊乱,导致发病高峰延迟,阻碍早期清除病毒及杀伤受染细胞的作用有直接关系。