Toxoplasma ROP16Ⅰ/Ⅲ ameliorated inflammatory bowel diseases via inducing M2 phenotype of macrophages

BACKGROUND Inflammatory bowel disease（IBD） is characterized by chronic and non-specific inflammation of the intestinal mucosa and mainly includes ulcerative colitis and Crohn’s disease.AIM To explore the beneficial effect of Toxo ROP16Ⅰ/Ⅲ-induced M2 phynotype macrophages in homeostasis of IBDs through downregulation of M1 inflammatory cells.METHODS RAW264.7 macrophages stimulated by lipopolysaccharide（LPS）（M1 cells） were co-cultured with Caco-2 cells as an inflammatory model of IBD in vitro.The expression of Toxo ROP16Ⅰ/Ⅲ was observed in RAW264.7 macrophages that were transfected with p EGFP-rop16Ⅰ/Ⅲ.The phenotypes of M2 and M1 macrophage cells were assessed by quantitative real-time reverse transcriptase polymerase chain reaction and the expression of tumor necrosis factor（TNF）-α,interleukin（IL）-1β,IL-6,transforming growth factor（TGF）-β1,IL-10,inducible nitric oxide synthase（i NOS）,and arginase-1（Arg-1） was detected.The expression of i NOS,Arg-1,signal transducer and activator of transcription 3（Stat3）,p-Stat3,Stat6,pStat6,programmed death ligand-2（PD-L2）,caspase-3,-8,and-9 was analyzed by Western blotting,and Griess assays were performed to detect nitric oxide（NO）.TNF-α,IL-1β,IL-6,TGF-β1,and IL-10 expression in the supernatants was detected by enzyme-linked immunosorbent assay,and Caco-2 cell apoptosis was determined by flow cytometry after mixing M1 cells with M2 cells in a Caco-2 cell co-culture system.RESULTS M1 cells exhibited significantly increased production of i NOS,NO,TNF-α,IL-1β,and IL-6,while Toxo ROP16Ⅰ/Ⅲ induced macrophage bias to M2 cells in vitro,showing increased expression of Arg-1,IL-10 and TGF-β1 and elevated production of p-Stat3 and p-Stat6.The mixed M1 and M2 cell culture induced by Toxo ROP16 Ⅰ/Ⅲ exhibited decreased production of NO and i NOS and upregulated expression of Arg-1 and PD-L2.Accordingly,Caco-2 cells became apoptotic,and apoptosis-associated proteins such as caspase-3,-8 and-9 were dampened during co-culture of M1 and M2 cells.Flow cytometry analysis showed that co-culture of M1 cells with Caco-2 cells facilitated the apoptosis of Caco-2 cells,but co-culture of M1 and M2 cells alleviated Caco-2 cell apoptosis.CONCLUSION Toxo ROP16 Ⅰ/Ⅲ-induced M2 macrophages inhibited apoptosis of Caco-2 cells caused by M1 macrophages.This finding may help gain a better understanding of the underlying mechanism and represent a promising therapeutic strategy for IBDs.

A first-in-man study of the Firesorb Sirolimus Target Eluting Bioresorbable Vascular Scaffold in Patients with Coronary Artery Disease(FUTURE-Ⅰ):two-year clinical and imaging outcomes

Background A newer generation bioresorbable scaffold Firesorb(MicroP ort,Shanghai,China),with thinner-strut(100~125μm),is constructed from a PLLA backbone abluminally coated with a PDLLA layer eluting sirolimus.FUTURE-I study intended to assess the feasibility,preliminary safety and effectiveness of the Firesorb BRS in patients with single de novo coronary artery lesions.We evaluated the long-term performance of the new generation BRS with thinner struts serially(post-procedure,at 6 months,1,2 year)after implantation.

宫颈CINⅠ伴高危型HPV感染患者治疗中宫颈微波的应用安全性探究

研究观察宫颈微波在治疗宫颈上皮内瘤变Ⅰ(CINⅠ)伴高危型人乳头瘤病毒(human papilloma vrius,HPV)感染患者中的应用效果。。方法 利用信封法将90例于2022年9月-2023年9月期间在本院接受治疗的宫颈CINⅠ伴高危型人乳头瘤病毒感染患者分为参照组(瑞贝生)及观察组(瑞贝生+宫颈微波)各45例。观察宫颈微波的临床治疗效果。结果 观察组的临床治疗总有效率(91.11%)较参照组(75.56%)更高,差异具有统计学意义(P<0.05)。然而,在比较治疗前组间的HPV病毒载量、血清IL-2水平以及血清IL-6水平时,并未观察到具有统计学意义的差异(P>0.05);相较于治疗前HPV病毒载量、血清IL-2水平及血清IL-6水平,治疗后均有所降低,且观察组明显低于参照组(P<0.05)。结论 宫颈微波应用于宫颈CINⅠ伴高危型HPV感染患者治疗中,应用价值显著。

Establishment of a Real-time Fluorescent Quantitative RTPCR Method for Detecting NP Gene of Class Ⅰ Newcastle Disease Virus(NDV)

Newcastle disease( ND) is one of the most serious infectious diseases that infect the poultry industry.There is only one serotype of Newcastle disease virus( NDV),but NDVs can be divided into two distinct classes( class Ⅰ,and class Ⅱ) according to their genetic relationship.To develop a method for rapid quantitative detection of class Ⅰ NDV,a pair of primers and a TaqM an probe were designed and synthesized according to the conservative sequence of NP gene of class Ⅰ NDV.The positive recombinant plasmid harboring NP gene of JS-18-05 isolate was used as a positive template to establish the standard curve.A real-time fluorescent quantitative RT-PCR method was established for rapid detection of class Ⅰ NDV with strong specificity,high sensitivity and good repeatability.The established method exhibited a good linear relationship within the concentration of 102 to 108 copies of NDV,by which 1 μl of 10 copy of NDV nucleic acid could be detected in the initial template.Compared with conventional virus isolation methods,the established method had similar sensitivity and led to the same results in detecting33 class Ⅰ,class Ⅱ NDV isolates.The study provided the basis for rapid quantitative detection of class Ⅰ NDVs and further clarification of their pathogenicity and pathogenic mechanism in poultry.

唯阴康联合宫颈射频消融术治疗持续CINⅠ的临床效果观察

目的:探讨宫颈射频消融术后使用唯阴康(阴道吸附器)治疗持续CINⅠ的临床疗效。方法:对137例持续CINⅠ患者,随机分为两组,单纯宫颈射频消融治疗70例(单纯射频组),宫颈射频消融术后使用唯阴康治疗67例(射频+唯阴康组),连续阴道用药至宫颈创面愈合。观察两组愈合、术后排液、出血、感染发生及治愈情况。结果:两组术后6个月随访治愈率均较好,分别为91.4%和94.0%,两组比较差异无统计学意义(P>0.05);射频+唯阴康组患者宫颈创面愈合时间(32.78±4.52天)低于单纯射频组(47.53±3.46天)(P<0.05),术后阴道流液、出血等情况优于单纯射频组;术后随访4周,射频+唯阴康组愈合率(56.7%)高于单纯射频组(27.1%)(P<0.05)。结论:宫颈射频消融联合唯阴康治疗持续CINⅠ疗效满意,患者依从性好、安全性高,是较为理想的方法。

P16蛋白表达强度与CINⅠ病变转归的相关性研究

目的：研究P16蛋白表达强度与宫颈上皮内瘤样病变（CINⅠ病变）转归的相关性。方法：选取2010年5月~2013年2月我院收治的CINⅠ病患者37例为研究对象,进行回顾性分析,进行病理活检与免疫组化,分析随访期间与随访结束时病理检查患者病变转归结局。结果：37例患者中,P16蛋白阳性检出率为51.35%,其中阳性（＋）29.73%,阳性（＋＋）16.21%,阳性（＋＋＋）5.50%;37例患者随访期间病变进展患者5例,比例13.51%,阴性组患者未见病情进展,随着P16蛋白表达增强,病变进展率逐步增加,对比差异具有统计学意义（P〈0.05）;以P16蛋白表达强度做预测CIN病变指标,灵敏度、特异度、阳性预测值及阴性预测值均较佳。结论：P16蛋白表达强度可有效预测CINⅠ病变转归情况,对指示患者病情进展有积极意义,临床应用价值高,可作为评价CINⅠ病变进展的重要参考指标。

重组人干扰素α-2b凝胶治疗CINⅠ合并高危型HPV感染的疗效探讨

目的:研究重组人干扰素α-2b凝胶(商品名:尤靖安)治疗宫颈上皮轻度不典型增生(CINⅠ)合并高危型人乳头瘤病毒(HPV)感染的疗效。方法:对临床20例CINⅠ合并高危型HPV-DNA阳性的患者采用重组人干扰素α-2b凝胶治疗;观察CINⅠ治愈及HPV-DNA转阴的情况。结果:CINⅠ治愈率:3个月为85.5%、6个月为90%;高危型HPV-DNA的转阴率:3个月为40%、6个月为50.5%。结论:重组人干扰素α-2b凝胶治疗CINⅠ合并高危型HPV感染的疗效肯定,无明显副作用,值得推广及应用。

抗HPV生物蛋白敷料阴道上药治疗HPV高危感染并CINⅠ的效果观察

目的观察抗人乳头瘤病毒(HPV)生物蛋白敷料阴道上药治疗HPV高危感染并宫颈上皮内瘤变(CIN)Ⅰ的效果。方法 148例HPV高危感染并宫颈CINⅠ患者,按就诊顺序分为实验组(81例)和对照组(67例)。实验组行抗HPV生物蛋白敷料阴道上药治疗,对照组未使用药物。比较两组干预后第4个月的HPV检测和宫颈脱落细胞学检查结果。结果实验组清除HPV感染的总有效率为80.25%,显著高于对照组的46.27%(P <0.05)。实验组HPV合并宫颈细胞学ASCUS/LSIL患者的转阴率为80.00%,显著高于对照组的33.33%(P <0.05)。结论抗HPV生物蛋白敷料阴道上药治疗HPV高危感染并CINⅠ患者有利于HPV的清除,还可提高宫颈脱落细胞学ASCUS/LSIL的转阴率。

保妇康栓用于经LEEP刀治疗后的重度宫颈糜烂伴CINⅠ、Ⅱ级患者的应用效果观察

目的研究保妇康栓用于经LEEP刀治疗后的重度宫颈糜烂伴CINⅠ、Ⅱ级患者的预后效果,为临床治疗提供有效依据。方法 2014年6月～2015年5月贵州省安顺市妇幼保健院经LEEP刀治疗的重度宫颈糜烂伴CINⅠ、Ⅱ级的病例中选取103例患者作为研究对象,将患者按照随机数表法分为观察组(n(n=48)。观察组患者在LEEP刀治疗后,采用保妇康栓进行后期的治疗,对照组患者则在LEEP刀治疗后,采用常规治疗方法。观察、记录并分析两组患者的治疗效果及预后情况。结果观察组术后恢复明显优于对照组,观察组在术后的阴道排液时间、阴道排液时间、创面愈合时间分别为(11.02±2.98)d、(16.10±3.25)d、(33.21±10.23)d,优于对照组的(25.46±5.21)d、(18.62±5.21)d、(46.78±11.28)d(P<0.05);观察组的治愈率90.91%明显高于对照组72.92%(P<0.05);观察组患者并发症5.45%,明显少于对照组患者的27.08%(P(37.65±4.01)分、(33.01±3.56)分、(28.73±2.91)分,对照组分别为(33.01±3.40)分、(33.02±3.56)分、(31.66±3.89)分、(24.98±3.02)分,观察组均明显高于对照组(P<0.05)。结论妇康栓用于经LEEP刀治疗后的重度宫颈糜烂伴CINⅠ、Ⅱ级患者能产生较好的预后,在术后恢复、治疗效果等方面均具有良好的效果,能有效降低并发症的发生率,同时还可改善患者的生活质量,值得临床推广。

探讨抗HPV生物蛋白敷料治疗HPV高危感染合并宫颈CIN Ⅰ的临床疗效

目的探讨抗HPV生物蛋白敷料治疗HPV高危感染合并宫颈CIN Ⅰ的临床疗效。方法收集2017年1月~2017年6月间在本院门诊就诊HPV高危感染合并宫颈CIN Ⅰ患者160例,随机分为试验组和对照组,试验组80例,采用抗HPV生物蛋白敷料阴道上药,每次1支,隔日1次,每月10次为1个疗程,连用3个疗程;对照组80例,给予观察不使用药物。结果治疗后6个月,试验组总有效率(80.95%)优于对照组(46.67%);试验组宫颈脱落细胞学检查转阴率(80.77%)优于对照组(31.58%);治疗后3个月和6个月,试验组HPV-DNA的负荷量均明显减少,减少程度明显优于对照组;以上三项两组间比较差异均有统计学意义(P <0.05)。结论抗HPV生物蛋白敷料治疗HPV高危感染合并宫颈CIN Ⅰ临床疗效显著,无不良反应。

解毒益肾汤联合冷冻疗法治疗持续性CINⅠ级疗效观察

目的:观察解毒益肾汤联合冷冻疗法治疗持续性CINⅠ级的临床疗效。方法:52例患者随机分为两组各26例。治疗组采用解毒益肾汤联合冷冻疗法。对照组采用银离子妇用凝胶外用。结果:治疗组总有效率92.3%,明显高于对照组80.7%(P<0.05)。结论:解毒益肾汤联合冷冻疗法治疗持续性CINⅠ级疗效较好。

聚焦超声治疗持续CINⅠ临床观察

目的观察聚焦超声治疗持续C INⅠ(宫颈上皮肉瘤变)的临床疗效及安全性。方法采用焦聚超声技术治疗持续C INⅠ患者64例,观察其临床症状、疗效及副反应。结果焦聚超声治疗持续C INⅠ的总有效率达90.63%。术后阴道排液和流血量少,治愈后宫颈恢复常态,无瘢痕形成。结论聚焦超声治疗持续C INⅠ具有安全可靠、治愈率高、创伤小、副作用小等特点,值得临床推广。

参柏祛毒汤联合干扰素栓治疗CINⅠ～Ⅱ级LEEP术后病变残存的临床研究

目的 探讨参柏祛毒汤联合干扰素栓治疗CINⅠ～Ⅱ级LEEP术后病变残存的临床疗效.方法 将CIN Ⅰ～Ⅱ级LEEP 术后病变残存的80例患者随机分为两组,每组各40例.两组均于月经净后予α-干扰素栓塞阴道,隔日1次,每次10万U,晚睡前使用,连续10次用药;治疗组联用参柏祛毒汤口服1周.疗程结束及随后3、6个月及12个月进行宫颈薄层细胞学及高危型人乳头瘤病毒16/18型DNA检查.结果 疗程结束及治疗后3、6、12个月的治愈率试验组高于对照组（P＜0.05）,差异有统计学意义;无不良反应.结论 参柏祛毒汤联合干扰素栓治疗CIN Ⅰ～Ⅱ级LEEP术后病变残存是安全、有效的.

两种方法治疗持续CINⅠ的疗效观察

目的：观察聚焦超声（HIFU）及环形电刀切除术（LEEP）治疗持续CINⅠ的临床疗效及安全性.方法：采用HIFU治疗持续CINⅠ患者64例、LEEP治疗61例,观察两组临床症状、疗效及副反应.结果：HIFU及LEEP组总有效率分别为90.63%、93.44%,差异无统计学意义（P〉0.05）.HIFU组术后阴道排液和流血量少,治愈后宫颈恢复常态,无瘢痕形成,与LEEP组术后副反应比较差异有统计学意义（P＜0.05）.结论：HIFU治疗持续CINⅠ具有安全可靠、治愈率高、创伤小、副作用小等特点,值得推广.

微波联合保妇康栓治疗CINⅠ合并HPV感染的临床疗效观察

目的观察应用微波联合保妇康栓治疗CINⅠ合并HPV感染的临床疗效。方法选取236例入我院治疗且确诊为CINⅠ合并HPV阳性的患者为研究对象,随机分为对照组和治疗组,对照组120例患者仅予以保妇康栓治疗,而治疗组116例患者予以微波治疗仪烧灼联合保妇康栓治疗,16天为一个疗程,均连用三个疗程,治疗4个月后复查并比较其临床疗效。结果治疗4个月后,对照组的治愈率为60%,有效率为10.8%,治疗组的治愈率为75%,有效率为16.4%,均显著高于对照组(P<0.05);对照组HPV阳性率为25.8%,而治疗组为10.3%,显著低于对照组(P<0.05)。结论微波联合保妇康栓治疗CINⅠ合并HPV感染较单用保妇康栓治疗的疗效更好,值得临床应用和推广。

157例CINⅠ～Ⅱ宫颈光疗疗效分析

2004年2月至2007年2月我院妇科门诊以KS系列光热治疗仪治疗157例宫颈上皮内瘤样病变（CIN）Ⅰ～Ⅱ患者,现将其治疗效果、不良反应及并发症报告如下。

宫颈电环切除术联合重组人干扰素治疗CINⅠ级合并HPV感染的效果观察

目的观察宫颈电环切除术联合重组人干扰素治疗宫颈上皮内瘤变(CIN)Ⅰ级合并人乳头瘤病毒(HPV)感染的治疗效果。方法将41例CINⅠ合并HPV感染患者随机分为2组,观察组21例给予宫颈电环切除术(LEEP)联合重组人干扰素治疗,对照组20例给予单纯LEEP治疗,观察2组总有效率和HPV持续感染情况。结果观察组愈合率为85.7%显著高于对照组的60.0%,差异有统计学意义(P<0.05);2组总有效率比较差异无统计学意义(P>0.05);观察组HPV持续感染率低于对照组,差异有统计学意义(P<0.05)。结论宫颈电环切除术联合重组人干扰素治疗CINⅠ合并HPV感染疗效显著,无明显不良反应,可显著降低HPV持续感染率,值得临床推广应用。

宫颈电环切除术治疗持续性CINⅠ患者69例的临床分析

宫颈上皮内瘤变（CIN）是一组与宫颈浸润癌密切相关的癌前病变的统称。大量临床研究表明CIN并无典型临床表现和症状,也是导致诸多宫颈癌患者错过最佳治疗时机的主要原因之一。随着生活环境的改变,宫颈癌前病变的高危因素随之相应增多,如免疫功能紊乱及HPV病毒感染。且研究已证实,CIN及宫颈癌均呈发病年轻化趋势,且发病率也逐年上升,严重影响年轻女性的生活质量。

宫颈电环切除术与射频消融术治疗持续性宫颈CINⅠ的效果比较

目的比较宫颈电环切除术(LEEP)与射频消融术(RFA)治疗持续性宫颈上皮内瘤变Ⅰ级(CINⅠ)的治疗效果。方法将经阴道镜及活检病理证实为CINⅠ患者137例随机分为LEEP治疗组69例和RFA治疗组68例,对高危型HPV阳性患者术后均给予重组人干扰素α-2b凝胶治疗,比较两种治疗方式的临床疗效。结果 2组患者手术时间、治愈率、病变持续率及手术残留率比较差异均无统计学意义(P>0.05);LEEP治疗组术中出血量少于RFA治疗组(P<0.05),复发率低于RFA治疗组(P<0.05);2组术后并发症发生率比较差异无统计学意义(P>0.05)。结论 LEEP手术简便、廉价,患者无痛苦,术后恢复快,是目前治疗持续性CINⅠ安全有效的方法,只要掌握手术指征,规范手术步骤,可获得满意疗效,具有较好的临床推广价值。

Osteoporosis and fractures in liver disease: Relevance, pathogenesis and therapeutic implications

It is being increasingly recognized that patients with liver disease develop bone loss that can be severe enough to lead to atraumatic fractures and thus markedly diminish life quality and expectancy. The estimated prevalence for liver-related osteoporosis is between 20-420/100000 of the general population, and fractures between 60-880/100000. It should be kept in mind that up to 40% of patients with chronic liver disease may experience a fracture. The pathogenic mediators include fibronectin, insulin like growth factor-I, and various cytokines, but decreased vitamin D and/or treatment with corticosteroids contribute to worsening bone health. Despite the advances in bone biology that have shed some light on the pathogenesis of this bone loss, treatment options remain nonspecific and tightly linked to treatments of other forms of osteoporosis. Thus, treatment should include calcium and vitamin D supplementation in all patients with chronic liver disease. Therapy with bisphosphonates should be considered, especially in patients receiving corticosteroids. This review focuses on the prevalence of this entity as well as the evidence available with regard to the pathogenesis of bone loss in liver disease, the diagnostic steps required in all patients, and the therapeutic options available.