FAPα靶向标记化合物^(131)I-FAPI-03的合成及初步体内外实验研究

本研究以4-喹啉基-甘氨基-2-氰基吡咯烷为骨架,对连接基团进行碳链延长及羟基修饰成功合成FAPI衍生物ATE-FAPI-03;通过亲电取代反应实现其^(131)I标记,并对标记化合物^(131)I-FAPI-03的脂水分配比、体外稳定性等进行分析;开展细胞结合、内吞、流出等实验以评价^(131)I-FAPI-03的体外动力学特征;并考察了^(131)I-FAPI-03在荷胶质瘤小鼠体内的分布情况。结果表明:^(131)I-FAPI-03为亲脂性小分子,并具有良好的体外稳定性;与FAPα阳性细胞U87MG孵育10 min时的结合率为(22.00±0.35)%,且随着孵育时间的延长结合率有明显的上升趋势,而与FAPα阴性细胞MCF-7的结合率始终处于较低水平;通过竞争结合实验测得^(131)I-FAPI-03的IC50值为45.5 nM,表明其对FAPα具有较高的亲和力;大部分与U87MG细胞结合的^(131)I-FAPI-03可被细胞内吞,但其在细胞中的滞留能力偏低。^(131)I-FAPI-03在荷胶质瘤小鼠体内具有快速的肿瘤靶向能力:经尾静脉注射5 min后,肿瘤组织对^(131)I-FAPI-03的放射性摄取值为(14.90±3.21)%ID/g,注射2 h后,肿瘤/肌肉的放射性摄取比值达到(43.7±16.7)。上述结果为新型FAPα靶向药物的研发提供了重要的参考。

放射性标记小分子抑制剂用作靶向FAP肿瘤显像剂的现状与展望

成纤维细胞活化蛋白(FAP)存在于肿瘤基质成纤维细胞中,是近年来肿瘤诊断和治疗的一个重要靶点。在靶向FAP的放射性肿瘤显像剂中,小分子类显像剂受到了最广泛的关注。本文介绍了靶向FAP小分子显像剂的核心结构,并对2023年12月前新型FAP小分子显像剂的设计策略进行分类。此外,对目前表现优良或具有新颖结构的靶向FAP的PET显像剂和SPECT显像剂进行了系统梳理,并对其结构和设计思路进行总结和展望,以期对临床诊疗有所助益。

Fibroblast activation protein (FAP) as a prognostic biomarker in multiple tumors and its therapeutic potential in head and neck squamous cell carcinoma

Background:Fibroblast activation protein(FAP),a cell surface serine protease,plays roles in tumor invasion and immune regulation.However,there is currently no pan-cancer analysis of FAP.Objective:We aimed to assess the pan-cancer expression profile of FAP,its molecular function,and its potential role in head and neck squamous cell carcinoma(HNSC).Methods:We analyzed gene expression,survival status,immune infiltration,and molecular functional pathways of FAP in The Cancer Genome Atlas(TCGA)and Genotype Tissue Expression(GTEx)tumors.Furthermore,to elucidate the role of FAP in HNSC,we performed proliferation,migration,and invasion assays post-FAP overexpression or knock-down.Results:FAP expression was elevated in nine tumor types and was associated with poor survival in eight of them.In the context of immune infiltration,FAP expression negatively correlated with CD8+T-cell infiltration infive tumor types and positively with regulatory T-cell infiltration in four tumor types.Our enrichment analysis highlighted FAP’s involvement in the PI3K-Akt signaling pathway.In HNSC cells,FAP overexpression activated the PI3K-Akt pathway,promoting tumor proliferation,migration,and invasion.Conversely,FAP knockdown showed inhibitory effects.Conclusion:Our study unveils the association of FAP with poor tumor prognosis across multiple cancers and highlights its potential as a therapeutic target in HNSC.

Sinonasal Polyposis: About 60 Cases at Fann University Hospital Center, Senegal

Introduction: Sinonasal polyposis (SNP) is a chronic inflammatory disease of the mucosa of the nasal cavities and facial sinuses. It is characterized by an oedematous, multifocal and bilateral degeneration of the nasosinus mucosa, which originates in the lateral masses of the ethmoid, where it causes the formation of smooth, gelatinous, translucent and pyriform polyp lesions. The objective of this study was to review epidemiological, clinical, paraclinical data and evaluate the results of endoscopic surgical treatment. Patients and Methods: This is a retrospective study on 60 patients followed at the ENT department of the Fann National University Hospital Center, from January 2010 to December 2015. All patients with sinonasal polyposis were included in the study. Results: The average age of our patients was 38 years and the sex ratio (M/F) was 0.8. In the patients’ histories, we found 18% asthma and 10% Widal’s disease. The average consultation time was 8.5 years. All patients had consulted for nasal obstruction;rhinorrhea was bilateral and found in 67.7% of cases, with olfactory disorders accounting for 50%. The CT scan performed in 58% of cases made it possible to specify the extent of the lesions;the involvement of the ethmoidal sinus was constant and extended to the other sinuses except in 2 cases. All patients had received medical treatment with local corticosteroids. Endoscopic surgical treatment was initiated in 43% of cases after failure of corticosteroid-based medical treatment. The evolution under treatment marked by the reappearance of symptoms that increased each month. At one month postoperatively, all clinical symptomatology had improved with the exception of olfactory disorders, which persisted in 3 patients. At 12 months we noted 12 cases of reappearance of nasal obstruction. Conclusion: SNP is a disease of little known etiology. The diagnosis is almost always clinical. Endoscopic surgery remains a recourse to medical treatment. For good local control, patients should be more respectful of good compliance with corticosteroid therapy.

^(177)Lu-FAP-2286 RLT治疗晚期肺癌患者的效果和安全性

目的:放射配体治疗(radioligand therapy,RLT)是一种结合靶向治疗和辐射细胞杀伤能力的新兴疗法。本文探讨了^(177)Lu-成纤维细胞活化蛋白(fibroblast activation protein,FAP)-2286 RLT在晚期肺癌患者中的疗效和安全性,通过临床试验和患者结果分析,全面评估该疗法的治疗潜力,旨在改善晚期肺癌患者的预后。方法:本研究纳入了2022年9月—2024年4月在西南医科大学附属医院接受^(177)Lu-FAP-2286 RLT治疗的晚期肺癌患者。所有患者在治疗前进行了68Ga-FAP-2286正电子发射体层成像(positron emission tomography,PET)/计算机体层成像(computed tomography,CT),并显示病灶内FAP高表达。每个治疗周期的^(177)Lu-FAP-2286剂量约为200 mCi(7.4 GBq),通过静脉输注于4 h内完成,治疗间隔为8~12周,总治疗次数为4~6周期。安全性和有效性评估包括实验室检查、不良事件记录、与实体瘤临床疗效评价标准(response evaluation criteria in solid tumor,RECIST)1.1和基于PET/CT的实体瘤PET疗效评价标准(PET response criteria in solid tumor,PERCIST)1.0标准评估。数据分析使用SPSS 26.0进行,正态性检验后采用配对样本t检验比较治疗前后的差异。结果:纳入的10例患者中(8例男性和2例女性,年龄范围为53~73岁),治疗周期分布为1例接受6个周期,3例接受4个周期,1例接受3个周期,4例接受2个周期,1例仅接受1个周期。中位随访时间为13个月。治疗显示,^(177)Lu-FAP-2286具有良好的耐受性,主要不良反应为疲劳和腹胀,无严重血液系统毒性和肝肾功能损伤。疗效评估显示,PR率为30.0%,SD率为50.0%,进展性疾病(progressive disease,PD)率为20.0%。总体缓解率为30.0%,疾病控制率为80.0%。根据改良的PERCIST 1.0标准,PR率为30.0%,SD率为50.0%,PD率为20.0%。结论:^(177)Lu-FAP-2286 RLT在晚期肺癌患者中显示出良好的安全性和显著的疗效,具有较高的疾病控制率和总体缓解率。虽然本研究的样本量较小,但结果支持了^(177)Lu-FAP-2286 RLT作为一种有效治疗晚期肺癌的新策略。未来需要更大规模和长期随访的研究来进一步验证其疗效和安全性。

超声辐射下FAP-10000催化2-芳氧甲基苯并咪唑的aza-Michael加成反应

采用超声辐射,以FAP-10000作为催化剂,对丙烯腈和2-芳氧甲基苯并咪唑衍生物之间的aza-Michael反应进行了深入研究.经过不断优化条件,以简便、高效且环保的方法获得了目标化合物.利用FT-IR、^(1)H NMR以及^(13)C NMR等对其结构进行了确证.化合物4f的晶体结构揭示了其独特的自组装特性,该化合物通过分子间的π—π相互作用,形成了无限延伸的一维链状超分子结构.

探究^(64)Cu-FAPI-XT PET/CT不同采集条件对图像质量的影响

目的:探讨在不同采集时间、注射剂量与重建算法下对^(64)Cu-FAPI-XT正电子发射体层成像(positron emission tomography,PET)/计算机体层成像(computed tomography,CT)图像质量的影响,从而为临床实践提供参考。方法:回顾并选取2023年6—9月于广州医科大学附属第一医院行PET/CT检查的11例肿瘤患者,其中6例患者为高剂量组(^(64)Cu-FAPI-XT剂量2.22~3.22 MBq/kg),5例患者为低剂量组(^(64)Cu-FAPI-XT剂量1.59~2.18 MBq/kg)。所有患者均在静卧60 min后行PET/CT全身扫描,采集时间均为3.0 min/床位。采用有序子集最大期望值法(ordered subset expectation maximization,OSEM)和贝叶斯惩罚似然重建法(HYPER Iterative)两种算法对3.0 min/床位图像进行时间切割重建,分为以下5组:1.0 min/床位、1.5 min/床位、2.0 min/床位、2.5 min/床位、3.0 min/床位。由2名医师对所有图像进行主观评分,比较不同组图像的图像质量、噪声水平与诊断价值。测量肝脏、纵隔血池的平均标准摄取值(mean standard uptake value,SUVmean)、标准差(standard deviation,SD)和信噪比(signal-to-noise ratio,SNR)以进行半定量分析。结果:主观评价中高剂量组,HYPER Iterative重建与OSEM重建采集2.0 min/床位图像,图像质量能达到日常诊断要求(评分均≥3分)。低剂量组,HYPER Iterative重建采集2.0 min/床位图像,或OSEM重建采集2.5 min/床位图像,图像质量能达到日常诊断要求(评分均≥3分)。客观半定量分析:在相同采集时间下,注射不同剂量^(64)Cu-FAPI-XT扫描PET图像,HYPER Iterative重建图像质量均明显优于OSEM重建(P<0.05)。在高剂量组中1.5 min/床位组的图像质量明显优于1.0 min/床位组(P<0.05),而1.5 min/床位组的图像与2.5 min/床位组的图像质量差异无统计学意义(P>0.05)。在低剂量组中2.0 min/床位组与3.0 min/床位组的图像质量差异无统计学意义(P>0.05)。结论:以^(64)Cu-FAPI-XT为显像剂的uMI Panorama PET/CT图像采用HYPER Iterative重建方法的高剂量组需要采集1.5 min/床位PET图像质量可达到日常诊断要求;而在低剂量组中需要采集2.0 min/床位才可达到日常诊断要求。

^(68)Ga-FAP-2286 PET/CT对晚期消化系统恶性肿瘤治疗后的生存预测价值

目的:探究与临床参数相比,^(68)Ga-FAP-2286正电子发射体层成像(positron emission tomography,PET)/计算机体层成像(computed tomography,CT)是否可以识别总生存期(overall survival,OS)更短的晚期消化系统恶性肿瘤患者。方法:回顾并分析2023年4月—2024年6月于西南医科大学附属医院经病理学检查证实为晚期消化系统肿瘤且在经手术治疗、放化疗及靶向免疫治疗后行^(68)Ga-FAP-2286 PET/CT检查的患者的影像学资料与临床资料。通过手动分割肿瘤负荷[计算肿瘤体积、峰值/平均值/最大标准化摄取值(standard uptake value,SUV)、肿瘤背景比值(tumor-to-background ratio,TBR)和细胞表面上的肿瘤受体结合(tumor receptor binding,TRB),TRB定义为SUV_(mean)乘以肿瘤体积],对扫描进行目视和定量评估。临床参数包括性别、既往治疗的方式和年龄。成像后,记录OS。结果:本研究共纳入32例患者,其中男性22例,女性10例,年龄30~83岁。在单变量COX回归分析中,较高的TBR(HR=1.217,95%CI 1.022~1.448,P=0.027)、TRB(HR=1.001,95%CI 1.000~1.002,P=0.029)和淋巴结转移的存在(HR=3.783,95%CI 1.033~13.854,P=0.045)与较短的OS显著相关。较大的肿瘤体积有显著性趋势(HR=1.004,95%CI 1.000~1.009,P=0.066),而其他参数都不能预测OS。在多变量COX回归中,只有TRB被确定为OS的重要独立预后因素(HR=1.001,95%CI 1.000~1.003,P=0.018)。在Kaplan-Meier分析中,TRB高于中位数142、TBR高于中位数8.3和存在淋巴结转移与较短的OS相关。结论:在晚期消化系统恶性肿瘤中,通过^(68)Ga-FAP-2286 PET/CT检测到的TRB升高是OS的独立预测因子。

基于FAP和TOC的工艺问题分析方法研究

为了帮助企业工艺创新时快速准确地识别出问题的根原因,提高工艺创新的成功概率,提出了一种基于流程功能分析(FAP)和约束理论(TOC)的工艺问题分析方法。首先,构建面向工艺系统的功能结构,并在此基础上改进流程功能模型;其次,应用改进后的流程功能模型分析工艺流程的问题区域,利用当前现实树识别问题的根原因;最后,应用层次分析法确定工艺问题的核心原因。结果表明:1)相对于其他模型,研究所提模型不仅可以有效降低根原因识别的误差,而且识别的时间也节省了数倍,提高了工艺问题根原因识别的准确性和效率;2)实例验证中采用新方案后的齿轮弯曲疲劳强度为706.4 MPa,接触疲劳强度值为1658.56 MPa,达到了齿轮工艺创新项目的技术指标要求,验证了研究模型的有效性和实用性。研究成果建立了符合工艺流程特征的工艺问题分析方法,其可作为通用方法为企业在工艺创新问题分析阶段提供理论参考。

苏淮猪背最长肌FAPs细胞体外成脂能力及其基因表达模式的研究

旨在体外获得纯度较高的苏淮猪背最长肌纤维/脂肪形成祖细胞(fibro/adipogenic progenitors,FAPs),并评价其在体外传代过程中成脂能力与基因表达模式的变化。本研究取1日龄苏淮公猪背最长肌,消化获得悬浮混合细胞,利用抗表面特异抗原血小板衍生生长因子受体α(PDGFRα)抗体通过免疫荧光评价4种不同差速贴壁时间分离的FAPs细胞的纯度,确定最佳差速贴壁时间。然后比较不同代数FAPs细胞(P1、P3和P5代)的体外成脂分化能力,并利用RNA-Seq比较不同代数FAPs细胞的基因表达模式,鉴别差异表达基因、KEGG通路与GO功能分类。研究结果表明,差速贴壁30 min分离的苏淮猪背最长肌FAPs细胞的纯度较高。对不同代数FAPs成脂能力评价发现,随着体外传代次数的增加,其成脂能力显著下降。利用RNA-Seq发现P3和P5代FAPs细胞的基因表达模式相近,P3和P5代分别与P1代FAPs细胞相比,鉴定到2336个共有的差异表达基因,其中差异上调基因1102个,差异下调基因1234个,KEGG和GO分析表明共有的差异上调基因主要富集在PI3K-AKT-FoxO、PI3K-AKT-HIF-1和cGMP-PKG等通路,共有的差异下调基因主要富集在DNA复制和修复等通路,其中可抑制细胞增殖与成脂分化的IRS1、FOXO3、CCNG2、EGFR、FGF1基因表达上调,可促进细胞增殖的CSF1R和SIPA1L2基因表达下调。P3与P5相比发现,差异上调基因主要富集在NOD-like、MAPK和非典型Wnt信号等通路;差异下调基因主要富集在VEGF、PPAR、Notch以及IL-17等信号通路,其中可抑制细胞成脂分化的TNFAIP3、AREG、FGF1、FGF9基因表达上调,可促进成脂分化的PPARγ、C/EBPα、LCN2基因下调。本研究结果表明,差速贴壁30 min能够得到纯度较高的猪FAPs细胞,FAPs细胞在体外培养过程中成脂分化能力不断下降,其基因表达模式发生了较大变化,主要表现为可促进细胞增殖和成脂分化的信号通路及其相关基因表达水平下降,本研究结果可为开发能维持猪FAPs细胞体外成脂能力的培养基配方提供参考。

Hereditary polyposis syndromes remain a challenging disease entity:Old dilemmas and new insights

In this editorial we present an overview and insights of the management of hereditary polyposis syndromes.The primary focus was on familial adenomatous polyposis,juvenile polyposis syndrome and Peutz-Jegher syndrome.Genetic testing has become increasingly available and is easier than ever to integrate into clinical practice.Furthermore,several genes have been added to the expanding list of genes associated with hereditary polyposis syndromes,allowing for precise diagnostics and tailored follow-up.Endoscopic evaluation of patients with hereditary polyposis syndromes is paramount in the surveillance strategies.Current endoscopic procedures include both diagnostic procedures and surveillance as well as therapeutic interventions.Recommendations for endoscopic procedures in the upper and lower gastrointestinal canal were described.Surgery is still a key component in the management of patients with hereditary polyposis syndromes.The increased cancer risk in these patients often render prophylactic procedures or intended curative procedures in the case of cancer development.Surgical interventions in the upper and lower gastrointestinal canal were described with relevant considerations.Development of chemopreventive medications is ongoing.Few drugs have been investigated,including nonsteroidal anti-inflammatory drugs.It has been demonstrated that cyclooxygenase-2 inhibitors may lower the number of polyps.Other medications are currently under investigation,but none have,to date,consistently been able to prevent development of disease.

Hsa_circ_0036740 in familial adenomatous polyposis:Immune regulation and neutrophil effects in CRC based on highthroughput assay

Familial adenomatous polyposis(FAP)is an autosomal dominant disease with a high probability of becoming cancerous.Many RNAs potentially associated with FAP have not been identified.In this study,a circRNA(circular RNA)expression profile of FAP was established using a circRNA microarray,and differentially expressed circRNAs were verified by RT-qPCR.The effects of hsa_circ_0036740 on the malignant behavior of tumor cells(proliferation,apoptosis,and epithelial mesenchymal transition)and the levels of C3A complement protein expression were evaluated.Moreover,neutrophils were isolated and co-cultured with colorectal cancer cells(CRCs),followed by measurements of MPO-DNA,citrullinated histone H3,interleukin(IL)-1β,IL-6,and IL-8 levels.Nuclear translocation of arginine deiminase 4(PAD4)was observed using immunofluorescence assays.Based on the high-throughput assay,238 downregulated circRNAs,and 38 upregulated circRNAs were identified.A Kyoto Encyclopedia of Genes and Genomes enrichment analysis suggested that immune regulation might be involved in FAP.A total of 10 DECs(differentially expressed circular RNAs)were identified by RT-qPCR,and among them,hsa_circ_0036740 showed the highest fold-change in upregulation.Results of gain-of-and loss-of-function studies revealed that hsa_circ_0036740 enhanced the malignant behavior of tumor cells,such as metastasis,proliferation,and apoptosis,with an increasing level of C3A complement.Moreover,hsa_circ_0036740 also significantly increased neutrophil extracellular trap formation and inflammation in neutrophils,as shown by an increased expression of PAD4.In conclusion,this study revealed the expression profiles of circRNAs in FAP and confirmed the possible involvement of hsa_circ_0036740 in the immune regulation mediated by neutrophils.Finally,hsa_circ_0036740 was suggested as a new therapeutic target for CRC.

Polyposis found on index colonoscopy in a 56-year-old female-BMPR1A variant in juvenile polyposis syndrome:A case report

BACKGROUND Juvenile polyposis syndrome(JPS)is a rare hereditary polyposis disease frequently associated with an autosomal-dominant variant of the SMAD4 or BMPR1A gene.It often manifests with symptoms in children and adolescents and is infrequently diagnosed in asymptomatic adults.Establishing the diagnosis is important as patients with JPS have a high risk of developing gastrointestinal cancer and require genetic counselling and close routine follow-up.CASE SUMMARY We report on the case of a 56-year-old female diagnosed with JPS after genetic testing revealed a rare variant of the BMPR1A gene BMPR1A c.1409T>C(p.Met470Thr).She was initially referred for colonoscopy by her general practitioner after testing positive on a screening faecal immunochemical test and subsequently found to have polyposis throughout the entire colorectum on her index screening colonoscopy.The patient was asymptomatic with a normal physical examination and no related medical or family history.Blood tests revealed only mild iron deficiency without anemia.To date,there has only been one other reported case of JPS with the same genetic variant.Subsequent colonoscopies were organised for complete polyp clearance and the patient was returned for surveillance follow-up.CONCLUSION JPS patients can present with no prior symptoms or family history.Genetic testing plays an important diagnostic role guiding management.

MUTYH-associated polyposis: Is it time to change upper gastrointestinal surveillance? A single-center case series and a literature overview

BACKGROUND The presence of Spigelman stage(SS)IV duodenal polyposis is considered the most significant risk factor for duodenal cancer in patients with MUTYH-associated polyposis(MAP).However,advanced SS disease is rarely reported in MAP patients,and no clear recommendations on small bowel(SB)surveillance have been proposed in this patient setting.AIM To research more because that case reports of duodenal cancers in MAP suggest that they may develop in the absence of advanced benign SS disease and often involve the distal portion of the duodenum.METHODS We describe a series of MAP patients followed up at the Regina Elena National Cancer Institute of Rome(Italy).A literature overview on previously reported SB cancers in MAP is also provided.RESULTS We identified two(6%)SB adenocarcinomas with no previous history of duodenal polyposis.Our observations,supported by literature evidence,suggest that the formula for staging duodenal polyposis and predicting risk factors for distal duodenum and jejunal cancer may need to be adjusted to take this into account rather than focusing solely on the presence or absence of SS IV disease.Core Tip:Case reports of duodenal cancers in MUTYH-associated polyposis suggest that they may develop in the absence of advanced Spigelman stage(SS)benign disease and often involve the distal portion of the duodenum.In our case series,we identified two(6%)small-bowel adenocarcinomas with no previous history of duodenal polyposis.Our observations,supported by literature evidence,suggest that the formula for staging duodenal polyposis and predicting risk factors for distal duodenum and jejunal cancer should be adjusted to take into consideration the presence of SS IV disease,rather than focusing only on this feature.suggestive of invasive adenocarcinoma.

儿童胃肠道息肉的超声检查诊断分析

目的探讨超声检查在儿童胃肠道息肉诊断中的应用价值。方法选取超声检查诊断胃肠道息肉患儿681例,所有患儿均经消化道内镜、腹腔镜或开腹手术行息肉摘除术,将超声检查与手术、病理对照。结果超声检查诊断胃肠道息肉的总的敏感度、特异度、阳性预测值、阴性预测值、Youden指数及准确度均在97.00%以上,Kappa值为0.975,P<0.001,超声检查诊断与术后病理对照具有高度一致性。息肉病理类型最多见的是幼年性息肉647例(95.00%)、其次Peutz-Jeghers综合征肠息肉25例(3.67%)、幼年性息肉病4例(0.59%),三种病理类型的胃肠道息肉均具有典型的临床特征和声像图表现。结论不同病理类型的儿童胃肠道息肉声像图各具特点,超声检查诊断与病理具有高度一致性,可为临床诊断和治疗提供可靠的影像学依据。

Yb∶FAP晶体的光谱特性

研究了Ｙｂ∶ＦＡＰ晶体的光谱特性．用９８０ｎｍ的ＩｎＧａＡｓ激光二极管激发测量了Ｙｂ∶ＦＡＰ晶体的偏振发射光谱和荧光寿命，结合晶体的偏振吸收光谱，采用对易法计算了晶体的吸收截面和发射截面．讨论了Ｙｂ３＋掺杂浓度对Ｙｂ∶ＦＡＰ的光谱参数的影响．在较低掺杂浓度下，Ｙｂ∶ＦＡＰ晶体π偏振方向在９０３ｎｍ处的吸收截面为１０×１０－２０ｃｍ２，在１．０４３μｍ处的发射截面为５．８×１０－２０ｃｍ２，激光上能级的荧光寿命为１．１ｍｓ．

食管鳞癌间质组织中FAP、CD68的表达及意义

目的观察FAP与CD68蛋白在食管鳞癌组织中的表达,探讨二者在食管鳞癌发生、发展过程中的作用及意义。方法采用免疫组化EnVision法检测FAP与CD68蛋白在143例食管鳞癌组织中的表达。结果 FAP表达于食管鳞癌间质中活化的成纤维细胞和浸润的炎症细胞。食管鳞癌组织中FAP阳性率在复发患者高于未复发者(P<0.05);死亡患者高于生存者(P<0.01)。FAP在食管鳞癌组织中的表达与患者年龄、性别、肿瘤分化程度、T分期、淋巴结转移、远处转移、TNM分期、肿瘤周围微血管密度、化疗和放疗均无相关性。食管鳞癌中CD68阳性率在微血管密度高组高于微血管密度低组(P<0.01);复发者高于未复发者(P<0.01);放疗患者高于未放疗患者(P<0.05);死亡患者高于生存患者(P<0.01)。CD68在食管鳞癌组织中的表达与患者年龄、性别、肿瘤分化程度、T分期、淋巴结转移、远处转移、TNM分期、化疗情况均无相关性。食管鳞癌组织中FAP表达与CD68表达成正相关(P<0.05)。结论 FAP与CD68在食管鳞癌组织中的表达对判定患者预后有重要意义,且两种蛋白可能相互协调,共同促进食管鳞癌的进展。

SIRT3 HIF-1αFAP和HGF在不同临床分期胃癌组织中的表达及意义

目的探讨去乙酰化酶3(SIRT3)、缺氧诱导因子-1α(HIF-1α)、成纤维细胞活化蛋白(FAP)和肝细胞生长因子(HGF)在不同临床分期胃癌组织中的表达及意义。方法选取2017年6月~2018年12月秦皇岛市第一医院收治的胃癌患者83例,取患者原发肿瘤组织为癌组织标本,同时选取相对应的癌旁正常组织标本为对照,采用免疫组化法检测癌组织和癌旁正常组织中SIRT3、HIF-1α、FAP和HGF的表达水平,分析SIRT3、HIF-1α、FAP和HGF表达与胃癌临床分期的关系及在胃癌组织中表达的相关性。结果SIRT3在胃癌组织中的阳性表达率低于癌旁组织(P<0.05),HIF-1α和HGF在胃癌组织中的阳性表达率高于癌旁组织(P<0.05),FAP在胃癌组织中的阳性表达率为51.81%,在癌旁组织中不表达(P<0.05);SIRT3、HIF-1α、FAP和HGF在胃癌组织中的表达与胃癌TNM分期显著相关(P<0.05);胃癌组织中SIRT3与HIF-1α、FAP、HGF的表达呈负相关(P<0.05);HIF-1α与FAP、HGF的表达呈正相关(P<0.05);FAP与HGF的表达呈正相关(P<0.05)。结论SIRT3、HIF-1α、FAP和HGF的表达水平与胃癌的TNM分期存在相关性,它们可能共同参与了胃癌的发生发展,SIRT3的表达可能起到负向调控HIF-1α、FAP和HGF的作用。

子宫颈浸润性癌组织中α-SMA和FAP表达及临床意义

目的探讨α-平滑肌肌动蛋白(ɑ-smooth muscle actin,α-SMA)、成纤维细胞活化蛋白(fibroblast-activating protein,FAP)在正常子宫颈、子宫颈上皮内瘤变(cervical intraepithelial neoplasias,CIN)、子宫颈浸润性癌组织的表达,并分析二者表达与子宫颈浸润性癌临床病理指标、浸润转移及预后的关系。方法应用免疫组化Eli Vision两步法检测20例正常子宫颈、20例CIN及98例子宫颈浸润性癌组织中α-SMA和FAP的表达。比较三组中α-SMA和FAP的表达水平,以及二者与子宫颈浸润性癌临床病理特征的相关性。结果α-SMA和FAP在正常子宫颈、CIN中不表达,二者在子宫颈浸润性癌中均表达于肿瘤间质成纤维细胞的胞质内,FAP在肿瘤细胞中有少量表达。α-SMA在子宫颈浸润性癌间质中的阳性率为82.7%(81/98),与临床分期、病理分级和淋巴结转移相关(P<0.05);FAP在子宫颈浸润性癌间质中的阳性率为79.6%(78/98),FAP表达与子宫颈浸润性癌的临床分期、病理分级和淋巴结转移相关(P<0.05);α-SMA和FAP均与患者年龄、肿瘤大小无关(P>0.05)。α-SMA和FAP在子宫颈浸润性癌组织标本中表达在区域上有一致性,在表达强度上呈明显正相关。经直线相关分析α-SMA和FAP呈直线相关(r=0.829,P=0.000)。结论α-SMA和FAP在子宫颈浸润性癌生长、浸润和转移方面发挥一定作用,可作为预测子宫颈浸润性癌预后的可靠指标。

FAP与E-cadherin\N-cadherin在大肠癌中的表达及相关性研究

目的探讨FAP与E-cadherin\N-cadherin的表达与大肠癌发生发展的关系及其相关性。方法采用免疫组化EN法检测150例大肠癌标本中FAP与E-cadherin\N-cadherin的表达。结果FAP表达与肿瘤分期及淋巴结转移呈正相关,差异有统计学意义(P<0.05),而与肿瘤分级之间没有明显的相关性,差异无统计学意义(P>0.05)。E-cadherin的阴性表达率及Ncadherin阳性表达率与大肠癌的肿瘤分级、分期及淋巴结转移呈正相关,差异有统计学意义(P<0.05)。E-cadherin、N-cadherin阳性表达呈负相关,差异有统计学意义(r=-0.745,P<0.05)。结论:FAP高表达、E-cadherin的低表达或不表达和Ncadherin的反常表达与大肠癌的浸润\恶化有密切关系。