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find Keyword "免疫反应" 18 results
  • EFFECT OF TRANSFORMING GROWTH FACTOR β1 PLASMID ON FROSTED ALLOGENIC NERVE TRANSPLANTATION

    Objective To study the effect of transforming growth factor β1 (TGF-β1) plasmid on poly frosted-defrosted allogenic nerve transplantation. Methods Forty Wistar rats were randomly divided into two groups equally. A 2.0 cm sciatic nerve segment, 5 mm away from infrapiriformis muscle space, was removed and the defect was repaired with poly frosteddefrosted allogenic nerve. The TGF-β1 plasmids were injected into the nerve anastomosis and adjacent muscles in the experimental group, normal saline in the control group. The nerve specimens were sectioned for staining in the 6th and 12th weeks . Axonal count and statistical analyses were done. Results The grafted and distal nerve segments showed regenerated fibers in both groups. In the experimental group,less edema and more nerve fibers were observed in the 6th week. The grafted nerve segment was filled with regeneration axons, the myelinated nerve fibers arranged regularly, and the axons and the myelin sheaths developed well in the 12th week. There was significant difference in the number of regenerating axons between the experimental group 98.6±4.8/μm2 and control group 75.8±5.1/μm2 (Plt;0.01). Conclusion Multiple frost-defrost of allogenic nerve can reduce its antigenicity and increase itsusefulness in repairing nerve defects. Local use of TGF-β1 plasmid can enhance immunosuppression to reduce immuno rejection.

    Release date:2016-09-01 09:33 Export PDF Favorites Scan
  • Effects of histone demethylase JMJD3 in macrophages

    ObjectiveTo analyze effects of histone demethylase Jumonji-domaincontaining protein 3 (JMJD3) in macrophages in order to provide a new target for treatment of macrophage-related inflammatory reactions, autoimmune diseases, and organ transplantation rejection.MethodThe related literatures of researches on the effects of JMJD3 in the macrophages in recent years were searched and reviewed.ResultsThe macrophages played the important roles in maintaining tissue homeostasis and host response, clearing pathogens and apoptotic cells, and promoting tissue repair and wound healing. The JMJD3 could regulate the balance of M1 and M2 types of macrophages through the different ways and had different effects on the polarization of M2 macrophages when it was stimulated by the different extracellular substances. In some immune diseases and wound repairing, the JMJD3 could not only promote the inflammatory responses, but also polarize the M2 macrophages so as to inhibit the inflammation and promote the tissue repair. Clinically, the JMJD3 expression might be different in the different diseases and its low or high expression both might be involved in the occurrence of diseases.ConclusionHistone demethylase enzyme JMJD3 is involved in macrophage polarization and expression of inflammatory genes, but there are still many problems that require further to be investigated.

    Release date:2019-06-05 04:24 Export PDF Favorites Scan
  • 同种瓣的生物活性与耐久性

    液氮保存的同种瓣具有生物活性,在临床应用中显示了良好的近中期效果,但长期耐久性还有待提高.研究表明,同种瓣的供者来源、热缺血时间、灭菌时间和温度、灭菌液的配方、保存方法均能影响瓣膜的生物活性.有活性的同种瓣临床应用效果和使用寿命明显优于无活性的同种瓣,在移植后能诱发机体产生供体特异性的体液免疫和细胞免疫反应.瓣膜中存活的成纤维细胞和移植免疫反应与同种瓣耐久性的关系目前意见尚未统一.同种瓣植入的手术方式、供者瓣膜尺寸、宿主因素(年龄、体重、健康状态)等均能影响同种瓣的耐久性.

    Release date:2016-08-30 06:32 Export PDF Favorites Scan
  • RESEARCH PROGRESS OF IMMUNO-INFLAMMATORY RESPONSE AND PATHOLOGICAL SCAR

    ObjectiveTo review the research progress of the roles of inflammation and immune response in the formation of pathological scar. MethodsThe recent literature concerning the formation mechanism of pathological scar was extensively consulted, inflammation and immune response involved in the formation of pathological scar was reviewed. ResultsThe formation of pathological scar is associated with inflammation and immune response, some inflammatory factors will promote the activation of immune cells, then induce immune cells releasing cytokines and aggravate inflammatory response. However, inflammation response also affects the level of immune response. So they work together to promote the formation of pathological scar by the immuno-inflammatory cells and media. ConclusionThe formation of pathological scar is not only related to inflammation response, but also involves in immune response. Moreover, immune response is the new progress in the study of pathological scar mechanism in recent years. Further research of immuno-inflammatory response will provide new ideas and corresponding basis for the prevention of pathological scar.

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  • Advances of three oxysterols in inflammation and immunology

    ObjectiveTo summarize progress of 25-hydroxycholesterol (25-OHC), 27-hydroxycholesterol(27-OHC), and 7α,25-hydroxycholesterol (7α,25-OHC) three oxidized cholesterols in inflammation and immunology and to provide evidence for related basic researches and diseases treatments.MethodThe relevant literatures about these three important oxidized cholesterols in the inflammation and immunology in recent years were reviewed.ResultsThe 25-OHC and 27-OHC could exert the antiviral effects by interfering with various viruses invading the host via various mechanisms. Moreover, the 25-OHC and 27-OHC also played the important regulatory roles in a variety of inflammatory processes and inflammatory diseases. The 7α,25-OHC played the important role in a variety of inflammatory processes by acting on the inflammatory and immune cell membrane receptor G-protein coupled receptor 183 (also known as Epstein-Barr virus-inducible receptor 2).Conclusion25-OHC, 27-OHC and 7α,25-OHC play an important roles in occurrence and development of various inflammatory and immune responses and diseases of inflammatory and immune by acting on a variety of nuclear receptors and membrane receptors.

    Release date:2019-06-26 03:20 Export PDF Favorites Scan
  • 免疫性癫痫研究进展

    癫痫是一种具有永久致痫倾向的慢性脑部疾病,同时具有一定的致残率和致死率。经过正规的抗癫痫治疗,临床上仍有近 1/3 的癫痫发展为耐药性癫痫,为抗癫痫药物治疗带来挑战。最新的研究证实,相当比例的耐药性癫痫为自身免疫性癫痫,免疫反应的异常激活参与其发病。免疫性癫痫是基于自身免疫性脑炎提出的概念,它是免疫介导的、通常伴有新发难治性癫痫发作、亚急性进行性认知衰退以及行为或精神功能障碍的自身免疫性疾病,此类患者脑脊液中可检测到神经元特异性相关抗体。早期免疫调节治疗除了能有效控制癫痫症状外,还可有效缓解某些癫痫综合征的发展。因此,早期进行免疫调控治疗可能成为未来免疫性癫痫治疗的关键。

    Release date:2020-07-20 08:13 Export PDF Favorites Scan
  • THE INFLUENCE OF TISSUE ENGINEERED TENDON ON SUBGROUP OF T LYMPHOCYTES AND ITS RECEPTOR IN ROMAN CHICKENS

    OBJECTIVE: To investigate the influence of tissue engineered tendon on subgroup of T lymphocytes and its receptor in Roman chickens. METHODS: The flexor digitorum profundus of the third toes of right feet in 75 Roman chickens were resected and made 2.5 cm defects as experimental model. They were randomly divided into five groups according to five repair methods: no operation (group A), autograft (group B), fresh allograft (group C), polymer combined with allogenous tendon cells (group D), derived tendon materials combined with allogenous tendon cells (group E). The proliferation and transformation of lymphocytes and contribution of CD4+, CD8+, CD28 and T cell receptor (TCR) were detected to study the immune response. RESULTS: The CD4+, CD8+ and TCR of group D and E were increased slightly than that of group B after 7 days, while after 14 days, those data decreased gradually and no significant difference between tissue engineered tendon and autografts (P gt; 0.05), and there was significant difference between fresh allograft and tissue engineered tendon (P lt; 0.05). Lymphocytes transformation induced by conA also showed no significant difference between tissue engineered tendon and autografts (P gt; 0.05). CONCLUSION: Tendon cells are hypoantigen cells, there are less secretion of soluble antigen or antigen chips dropped out from cells. Tissue engineered tendon has excellent biocompatibility.

    Release date:2016-09-01 10:20 Export PDF Favorites Scan
  • CD4+ T细胞介导的免疫反应在面神经损伤修复中的作用

    随着神经免疫学的发展,越来越多的研究表明免疫系统和神经系统之间存在着相互作用,最近研究也发现,CD4+T细胞介导的获得性免疫反应对面神经损伤后的面运动神经元活性的维持起着重要作用,其具体细胞亚群是由相关信号传导子及转录激活子介导的从CD4+T细胞分化来的Th2亚群。此类研究有助于指导相关临床工作。

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  • THERAPEUTIC ACTIONS AND MECHANISM OF TETRANDRINE ON EXPERIMENTAL UVEITIS

    Experimental uveitis was induced in rabbits by bovine serum albumin. Ocular inflammation,protein content of aqueous humor,T lymphocyte transformation and serum circulating immune complex were reduced markedly after the treatment of tetrandrine (Tet, 50mg/kg/d,ip)and dexamethasone(Dex, 5mg/kg/d,ip)for 8 days. Four days after withdrawal of Tet and Dex the protien content of the aqueous humor and serum eiucrlating immune complexes rose again,but these parameters in Tet group is lower than that in Dex group. The pathological study showed that inflammation of choroid in Tet treated group was lighter than that in untreated group. These results suggest that Tet is an effective inhibitory agent on bovine serum albumin-induced experimental uveitis. Its mechanism may be related to the suppression of cellular and humoral immune function aside from antiinflammation. (Chin J Ocul Fundus Dis,1994,10:149-152)

    Release date:2016-09-02 06:34 Export PDF Favorites Scan
  • STUDY ON IMMUNE RESPONSE AFTER REPAIR OF NERVE DEFECT WITH ACELLULAR NERVE XENOGRAFT LADEN WITH ALLOGENIC ADIPOSE-DERIVED STEM CELLS IN RHESUS MONKEY

    Objective To observe the systemic and local immune response after repair of nerve defect with acellular nerve xenograft laden with allogenic adipose-derived stem cells (ADSCs) in rhesus monkey so as to evaluate the safety of the proposed material for nerve reconstruction. Methods Bilateral tibial nerves were taken from a healthy adult male landrace (weighing 48 kg) to prepare acellular nerve xenograft by chemical extraction. ADSCs were isolated from a healthy adult male rhesus monkey (weighing 4.5 kg), and were seeded into the acellular nerve grafts. The radial nerve defect models with 25 mm in length were established in 10 healthy adult female rhesus monkeys (weighing 3-5 kg), and they were divided into cell-laden group (n=5) and non-cell-laden group (n=5) randomly. Defect was repaired with acellular nerve xenograft laden with allogenic ADSCs in cell-laden group, with acellular nerve xenograft only in non-cell-laden group. The blood samples were taken from peripheral vein preoperatively and at 14, 60, and 90 days after operation for lymphocyte analysis; at 5 months after operation, the grafts were harvested to perform histological examination for local immune response and nerve regeneration. The nerve autograft in rhesus monkey was used as control. Results In cell-laden group and non-cell-laden group, no significant difference was found in the count of lymphocytes and T lymphocytes, the percentage of T lymphocytes, CD8+ T lymphocytes, as well as the ratio of CD4+ T lymphocytes to CD8+ T lymphocytes between pre- and post-operation (P gt; 0.05); in cell-laden group, the percentage of CD4+ T lymphocytes at 14 days was significantly lower than that at 60 and 90 days postoperatively (P lt; 0.05). The percentage of CD4+ T lymphocytes in cell-laden group was significantly lower than that in non-cell-laden group at 14 days (P lt; 0.05), but no significant difference was found in the other indexes at the other time between 2 groups (P gt; 0.05). At 5 months after operation, mild adhesion was found on the surface of nerve xenografts; the epineurium of nerve xenografts was thicker than that of nerve autografts; and neither necrosis nor fibrosis was found. CD3+, CD4+, CD8+, CD68+, and CD163+ T lymphocytes were scattered within the grafts, in which regenerative axons were revealed. CD3+, CD4+, CD8+, CD68+, and CD163+ T lymphocytes were comparable in cell-laden group, non-cell-laden group, and autograft group. Conclusion Repair of nerve defect with acellular nerve xenograft elicits neither systemic nor local immune response in rhesus monkeys. Implantation of allogenic ADSCs might result in transient depression of CD4+ T lymphocytes proliferation early after surgery, no immune response can be found.

    Release date:2016-08-31 04:24 Export PDF Favorites Scan
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