Colorectal cancer vaccines: Tumor-associated antigens vs neoantigens

Therapeutic options for the treatment of colorectal cancer(CRC) are diverse but still not always satisfying. Recent success of immune checkpoint inhibition treatment for the subgroup of CRC patients suffering from hypermutated tumors suggests a permanent role of immune therapy in the clinical management of CRC. Substantial improvement in treatment outcome could be achieved by development of efficient patient-individual CRC vaccination strategies. This mini-review summarizes the current knowledge on the two general classes of targets: tumor-associated antigens(TAAs) and tumorspecific antigens. TAAs like carcinoembryonic antigen and melanoma associated antigen are present in and shared by a subgroup of patients and a variety of clinical studies examined the efficacy of different TAA-derived peptide vaccines. Combinations of several TAAs as the next step and the development of personalized TAA-based peptide vaccines are discussed. Improvements of peptidebased vaccines achievable by adjuvants and immunestimulatory chemotherapeutics are highlighted. Finally, we sum up clinical studies using tumor-specific antigens-in CRC almost exclusively neoantigens-which revealed promising results; particularly no severe adverse events were reported so far. Critical progress for clinical outcomes can be expected by individualizing neoantigen-based peptide vaccines and combining them with immunestimulatory chemotherapeutics and immune checkpoint inhibitors. In light of these data and latest developments, truly personalized neoantigen-based peptide vaccines can be expected to fulfill modern precision medicine's requirements and will manifest as treatment pillar for routine clinical management of CRC.

Autoantibodies against tumor-associated antigens for detection of hepatocellular carcinoma

Hepatocellular carcinoma(HCC) is one of the most common tumors worldwide. The survival rate after the onset of symptoms is generally less than one year for the late presentation of HCC, and reliable tools for early diagnosis are lacking. Therefore, novel biomarkers for the early detection of HCC are urgently required. Recent studies show that the abnormal release of proteins by tumor cells can elicit humoral immune responses to self-antigens called tumor-associated antigens(TAAs). The corresponding autoantibodies can be detected before the clinical diagnosis of cancer. Therefore, there is growing interest in using serum autoantibodies as cancer biomarkers. In this review, we focus on the advances in research on autoantibodies against TAAs as serum biomarker for detection of HCC, the mechanism of the production of TAAs, and the association of autoantibodies with patients' clinical characteristics.

Comparisons of voided urine cytology, nuclear matrix protein-22 and bladder tumor associated antigen tests for bladder cancer of geriatric male patients in Taiwan, China

Aim： To compare the results of bladder tumor associated antigen （BTA TRAK）, nuclear matrix protein 22 （NMP 22） and voided urine cytology （VUC） in detecting bladder cancer. Methods： A total of 135 elderly male and 50 healthy volunteers enrolled in this study were classified into three groups： （i） 93 patients with bladder cancer; （ii） 42 patients with urinary benign conditions; and （iii） 50 healthy volunteers. BTA TRAK and NMP 22 kits were used to detect bladder cancer. Voided urine cytology was used to compare the sensitivity and specificity of the screening tests. Results： The sensitivity and specificity of cytology, BTA TRAK and NMP 22 were 24% and 97%, 51% and 73%, 78% and 73%, respectively. The level of NMP 22 increased with tumor grading. The BTA TRAK kit has the lowest sensitivity among the screening tests. The NMP 22 with the best sensitivity can be an adjunct to cytology for evaluating bladder cancer. Conclusion： The NMP 22 test has a better correlation with the grading of the bladder cancer than BTA TRAK. As cytology units are typically not available in hospitals or in outpatient clinics, NMP 22 might be a promising tool for screening bladder cancer.

HCA520, A NOVEL TUMOR ASSOCIATED ANTIGEN, INVOLVED IN CELL PROLIFERATION AND APOPTOSIS

Objective: Tumor associated antigen encoding gene HCA520 (AF146019) was identified by screening a human hepatocellular carcinoma expressing cDNA library using SEREX technique. In this experiment we studied the effect of HCA520 on cell proliferation and apoptosis. Methods: Gene HCA520 was gained by PCR and transfected into 293 cells. The stable expression cells were obtained by G418 selection. The cell proliferation was measured by [3H]-TdR uptake and apoptosis assay was measured by FACS. Results: Eukaryotic expression plasmid pcDNA3-HCA520 was constructed and its stable transfectants were obtained. Overexpression of HCA520 inhibited the cell proliferation and enhanced cell apoptosis after serum deprivation. Conclusion: HCA520 is a novel tumor associated antigen that can affect cell proliferation and apoptosis.

Preliminary study of the diagnosis of pancreatic cancer with a serum pancreatic cancer－associated antigen

The serum of 40 normal subjects, 61 cases of various malignant diseases except pancreatic cancer,53 cases of various benign diseases and 33 cases of pancreatic cancer was examined with ELISA to determine the serum level of pancreatic cancer-associated ant

MAGEA12在胃肠道间质瘤中的表达及其与危险度分级的关系

目的:探讨胃肠道间质瘤(gastrointestinal stromal tumors,GIST)中黑色素瘤相关抗原基因A12(melanomaassociated antigen gene A12,MAGEA12)的表达水平及其与GIST危险度分级的关系。方法:收集5例GIST患者的肿瘤组织及癌旁组织,采用转录组测序的方法,通过主成分分析(principal components analysis,PCA)、基因集富集分析(gene set enrichment analysis,GSEA)及差异表达基因分析法,明确GIST组织异常信号通路及异常表达基因;采用实时荧光定量PCR(quantitative real-time PCR,qRT-PCR)法验证90对GIST组织中异常表达基因MAGEA12的表达水平,并通过χ2检验分析MAGEA12的表达水平与GIST患者临床病理特征的相关性。结果:PCA显示GIST组织基因表达谱与癌旁组织比较差异有统计学意义;GSEA发现,GIST组织中多种肿瘤相关信号通路异常高表达;差异表达基因分析发现,MAGEA12是GIST组织中表达上调最高的基因(表达升高25倍);qRT-PCR验证了MAGEA12在GIST样本中显著高表达,且与GIST危险度分级呈正相关。结论:MAGEA12在GIST中高表达,其表达水平与GIST危险度相关,可能成为治疗的新靶点。

恶性肿瘤中免疫检查点抑制剂与甲状腺功能异常风险的Meta分析

目的 Meta分析免疫检查点抑制剂(immune checkpoint inhibitors,ICIs)治疗引起恶性肿瘤患者发生甲状腺功能异常的风险。方法 检索从建库至2022年10月15日Pub Med、Embase、Cochrane Library、中国知网及万方医学网中关于恶性肿瘤ICIs治疗的相关不良反应研究。根据纳入与排除标准筛选文献,提取研究数据,采用Stata 12.0软件进行Meta分析。结果 共纳入32项随机对照试验,其中使用程序性细胞死亡蛋白1(programmed cell death protein-1,PD-1)、程序性细胞死亡配体1(programmed cell death ligand-1,PD-L1)、细胞毒性T淋巴细胞相关蛋白4(cytotoxic T lymphocyte-associated antigen-4,CTLA-4)抑制剂单药治疗分别为17篇、6篇、3篇,两种ICIs联合使用为8篇。Meta分析显示,ICIs单药治疗引起恶性肿瘤患者发生甲状腺功能减退(RR=9.04,95%CI为7.21~11.33)、甲状腺功能亢进(RR=10.83,95%CI为6.96~16.90)、甲状腺炎(RR=7.61,95%CI为2.99~19.37)的风险明显高于对照组。PD-1(RR=8.61,95%CI为6.47~11.46)、PD-L1(RR=6.75,95%CI为4.33~10.52)、CTLA-4(RR=7.12,95%CI为3.16~16.08)和联合应用(RR=52.56,95%CI为13.15~210.12)引起的甲状腺功能减退的风险比对照组均升高。与单一ICIs比较,ICIs联合使用引起甲状腺功能减退(RR=1.77,95%CI为1.41~2.22)及甲状腺功能亢进(RR=3.79,95%CI为2.42~5.96)的风险进一步升高。结论 ICIs治疗引起恶性肿瘤患者甲状腺功能异常的风险明显升高,以发生甲状腺功能减退的风险最高,其次是甲状腺功能亢进和甲状腺炎。与ICIs单药比较,ICIs联合使用可进一步升高风险。

miR-487a通过靶向调控TIA1对胃癌肿瘤相关巨噬细胞M2型极化的抑制作用

目的:探讨微小RNA(miR)-487a对胃癌肿瘤相关巨噬细胞(TAMs) M2型极化的抑制作用,并阐明其对胃癌AGS细胞增殖、侵袭和迁移的影响。方法:分离和培养原发性胃癌患者胃癌组织TAMs及癌旁组织来源的正常巨噬细胞(NTMs),体外诱导人单核细胞THP-1分化为TAMs,将分化得到的M0、M1和M2型巨噬细胞经条件培养基(CM)刺激培养24 h,分别获取TAMs、M1-TAMs和M2-TAMs。转染TAMs,分为空白组、 inhibitor-NC组、 miR-487a inhibitor组、 miR-487a inhibitor+si-NC组和miR-487ainhibitor+si-TIA1组,采用实时荧光定量PCR(RT-qPCR)法和Western blotting法验证转染效率。将M2-TAMs与AGS细胞共培养,分为AGS组、AGS+inhibitor-NC组、AGS+miR-487ainhibitor组、AGS+miR-487ainhibitor+si-NC组和AGS+miR-487ainhibitor+si-TIA1组,RT-qPCR法检测胃癌组织TAMs和癌旁组织NTMs及各组TAMs中miR-487a和T淋巴细胞胞浆内抗原-1(TIA1) mRNA表达水平,Western blotting法检测胃癌组织TAMs和癌旁组织NTMs及各组TAMs中TIA1蛋白表达水平,流式细胞术检测各组TAMs中CD206和CD163水平,酶联免疫吸附试验(ELISA)法检测各组TAMs培养上清中白细胞介素10(IL-10)、转化生长因子β(TGF-β)、血管内皮生长因子A(VEGF-A)和精氨酸酶1(Arg-1)水平,CCK-8法检测各组AGS细胞增殖活性,细胞划痕实验检测各组AGS细胞迁移率,Transwell实验检测各组AGS细胞侵袭细胞数。结果:RT-qPCR法,与癌旁组织NTMs比较,胃癌组织TAMs中miR-487a表达水平明显升高(P<0.01),TIA1 mRNA表达水平明显降低(P<0.01);与TAMs比较,M1-TAMs中miR-487a表达水平明显降低(P<0.01),TIA1 mRNA表达水平明显升高(P<0.01);M2-TAMs中miR-487a表达水平明显升高(P<0.01),TIA1 mRNA表达水平明显降低(P<0.01);转染后,与空白组和inhibitor-NC组比较,miR-487a inhibitor组细胞中miR-487a表达水平明显降低(P<0.01),提示细胞转染成功。Western blotting法,与癌旁组织NTMs比较,胃癌组织TAMs中TIA1蛋白表达水平明显降低(P<0.01);与TAMs比较,M1-TAMs中TIA1蛋白表达水平明显升高(P<0.01),M2-TAMs中TIA1蛋白表达水平明显降低(P<0.01);共转染后,与inhibitor-NC组比较,miR-487a inhibitor组细胞中TIA1蛋白表达水平明显升高(P<0.01);与miR-487a inhibitor+si-NC组比较,miR-487a inhibitor+si-TIA1组细胞中TIA1蛋白表达水平明显降低(P<0.01)。流式细胞术,与空白组和inhibitor-NC组比较,miR-487a inhibitor组细胞中CD206和CD163水平明显降低(P<0.01);共转染后,与inhibitor-NC组比较,miR-487a inhibitor组细胞中CD206和CD163水平均明显降低(P<0.01);与miR-487a inhibitor+si-NC组比较,miR-487a inhibitor+si-TIA1组细胞中CD206和CD163水平均明显升高(P<0.01)。ELISA法,与空白组和inhibitor-NC组比较,miR-487a inhibitor组TAMs细胞培养上清中IL-10、TGF-β、VEGF-A和Arg-1水平均明显降低(P<0.01);共转染后,与inhibitor-NC组比较,miR-487a inhibitor组TAMs细胞培养上清中IL-10、TGF-β、VEGF-A和Arg-1水平均明显降低(P<0.01);与miR-487a inhibitor+si-NC组比较,miR-487a inhibitor+si-TIA1组TAMs细胞培养上清中IL-10、TGF-β、VEGF-A和Arg-1水平均明显升高(P<0.01)。CCK-8法,与AGS组比较,AGS+inhibitor-NC组细胞增殖活性明显升高(P<0.01);与AGS+inhibitor-NC组比较,AGS+miR-487a inhibitor组细胞增殖活性明显降低(P<0.01);与AGS+miR-487a inhibitor+si-NC组比较,AGS+miR-487a inhibitor+si-TIA1组细胞增殖活性明显升高(P<0.01)。细胞划痕实验,与AGS组比较,AGS+inhibitor-NC组AGS细胞迁移率明显升高(P<0.05);与AGS+inhibitor-NC组比较,AGS+miR-487a inhibitor组AGS细胞迁移率明显降低(P<0.01);与AGS+miR-487a inhibitor+si-NC组比较,AGS+miR-487a inhibitor+si-TIA1组AGS细胞迁移率明显升高(P<0.05)。Transwell实验,与AGS组比较,AGS+inhibitorNC组AGS细胞侵袭细胞数明显升高(P<0.01);与AGS+inhibitor-NC组比较,AGS+miR-487a inhibitor组AGS细胞侵袭细胞数明显降低(P<0.01);与AGS+miR-487a inhibitor+si-NC组比较,AGS+miR-487a inhibitor+si-TIA1组AGS细胞侵袭细胞数明显升高(P<0.01)。结论:沉默miR-487a表达可通过靶向上调TIA1抑制胃癌肿瘤相关巨噬细胞M2型极化,并抑制胃癌细胞增殖、迁移和侵袭。

血清癌胚抗原相关细胞黏附分子1 脂质运载蛋白-2 恶性肿瘤特异生长因子联合检测鉴别诊断乳腺癌的价值

目的 探讨血清癌胚抗原相关细胞黏附分子1(CEACAM1)、脂质运载蛋白2(LCN-2)、恶性肿瘤特异生长因子(TSGF)联合检测鉴别诊断乳腺癌的价值。方法 本研究为回顾性分析,对我院2021年1月至2023年1月收治的40例良性乳腺肿瘤患者临床资料进行收集,作为对照组;并对同期医院收治的40例乳腺癌患者临床资料进行收集,作为观察组。设计基线资料填写表,详细对2组基线资料、血清检查指标进行填写、比较,重点分析血清CEACAM1、LCN-2、TSGF联合检测鉴别诊断乳腺癌的价值。结果 观察组血清CEACAM1、LCN-2、TSGF水平比对照组高,差异有统计学意义(P<0.05),组间年龄、体质指数(BMI)、肿瘤直径、绝经及患侧比较,差异无统计学意义(P>0.05);绘制受试者工作曲线(ROC)结果显示,血清CEACAM1、LCN-2、TSGF检测鉴别诊断乳腺癌的曲线下面积(AUC)均>0.70,且以联合检测(并联)价值最佳。结论 血清CEACAM1、LCN-2、TSGF联合检测鉴别诊断乳腺癌有较高的灵敏度、特异度,鉴别诊断价值满意。

Chimeric antigen receptor-engineered T-cell therapy for liver cancer

Background: Chimeric antigen receptor-engineered T-cell(CAR-T) therapy is a newly developed immunotherapy used in the treatment of cancers. Because CAR-T therapy has shown great success in treating CD19-positive hematological malignancies, its application has been explored in the treatment of solid tumors, such as liver cancer. In this review, we discuss the immune characteristics of liver cancer, the obstacles encountered during the application of CAR-T therapy, and preclinical and clinical progress in the use of CAR-T therapy in patients with liver cancer.Data sources: The data on CAR-T therapy related to liver cancers were collected by searching Pub Med and the Web of Science databases prior to December 2017 with the keywords "chimeric antigen receptor","CAR-T", "liver cancer", "hepatocellular carcinoma", and "solid tumor". Additional articles were identified by manual search of references found in the primary articles. The data for clinical trials were collected by searching Clinical Trials.gov.Results: The liver has a tolerogenic nature in the intrahepatic milieu and its tumor microenvironment significantly affects tumor progression. The obstacles that reduce the efficacy of CAR-T therapy in solid tumors include a lack of specific tumor antigens, limited trafficking and penetration of CAR-T cells to tumor sites, and an immunosuppressive tumor microenvironment. To overcome these obstacles, several strategies have emerged. In addition, several strategies have been developed to manage the side effects of CAR-T, including enhancing the selectivity of CARs and controlling CAR-T activity. To date, no clinical trials of CAR-T therapy against HCC have been completed. However, preclinical studies in vitro and in vivo have shown potent antitumor efficacy. Glypican-3, mucin-1, epithelial cell adhesion molecule, carcinoembryonic antigen, and other targets are currently being studied.Conclusions: The application of CAR-T therapy for liver cancer is just beginning to be explored and more research is needed. However, we are optimistic that CAR-T therapy will offer a new approach for the treatment of liver cancers in the future.

Identification of novel HLA-A 0201-restricted epitopes from anterior gradient-2 as a tumor-associated antigen against colorectal cancer

Anterior gradient-2 （AGR2） promotes tumor growth, cell migration and cellular transformation and its enhanced expression is almost completely restricted to malignant tissues, thus making AGR2 an interesting target for the development of immunotherapeutic strategies. We investigated whether the AGR2 molecule comprises human leukocyte antigen （HLA）-A 0201-binding epitopes recognized by human cytotoxic T lymphocytes （CTLs）, which could be targeted in dendritic cell （DC）-based cancer immunotherapy against colorectal cancer （CRC）. We reviewed the sequence of AGR2 for peptides that could potentially bind to HLA-A 0201 with the aid of a computer-based program. Five candidate peptides with different binding scores were synthesized and tested. These peptides were then assessed for their immunogenicity to elicit specific immune responses mediated by CTLs in vitro by means of enzyme-linked immunospot assays and CTL assays. AGR2 was highly expressed in several CRC cell lines, including DK01, DLD1, KM 12C, HCT-8 and HT-29. DCs pulsed with AGR2-P2 （aa 11-19; LLVALSYTL） or AGR2-P4 （aa 127-135; RIMFVDPSL） generated potent CTLs that could lyse T2 cells pulsed with AGR2-P2 or AGR2-P4 and HLA-A0201＋ AGR2-positive CRC cell lines in a strong dose-dependent and HLA-A 0201-restricted manner. In conclusion, these novel epitopes derived from AGR2 protein may be attractive candidates for DC-based immunotherapy for CRC.

A Novel Putative Tumor Associated Antigen

A is a tumor associated antigen. Monoclonal antibody (mAb) against 17 1A has been used in adjuvant therapy of colorectal carcinoma. Using mAb against 17 1A antigen on affinity chromatography, a novel putative tumor associated antigen (P50) whose relative molecular mass is 5 0×10 4 has been isolated from human colorectal tumor tissues which are recognized by mAbs 17 1A and M79, while the relative molecular mass of 17\|1A antigen isolated from several colorectal tumor cell lines is 3 3×10 4. P50 was recognized by mAbs 17 1A and M79 which are specific mAbs against 17 1A antigen.

负载MAGE-A3抗原的树突状细胞与细胞因子诱导杀伤细胞共培养对子宫内膜癌肿瘤干细胞及恶性进展的影响

目的:探究负载黑色素瘤相关抗原基因A3(MAGE-A3)的树突状细胞(DC)与细胞因子诱导杀伤细胞(CIK)对子宫内膜癌肿瘤干细胞及恶性进展的影响。方法:采集人外周血分离单个核细胞,利用细胞因子分别诱导生成DC和CIK;MAGE-A3孵育DC后与CIK共培养,流式细胞仪检测DC-CIK、MAGE-A3-DC-CIK的表型;流式细胞仪分选子宫内膜癌细胞系Ishikawa的CD133^(+)干细胞,以子宫内膜癌干细胞作为靶细胞,分别以CIK、DC-CIK及MAGE-A3-DC-CIK作为效应细胞,MTT法检测效靶比为10∶1、20∶1、40∶1的细胞杀伤活性,ELISA法检测联合培养细胞上清液中IFN-γ、IL-2、IL-12、IL-17水平,Annexin V-FITC/PI双染法检测子宫内膜癌干细胞凋亡;建立子宫内膜癌干细胞移植瘤裸鼠模型,尾静脉注射DC-CIK或MAGE-A3-DC-CIK,观察裸鼠肿瘤生长情况,每隔2 d测量瘤体大小,21 d后取肿瘤组织,电子天平称重,HE染色观察肿瘤组织病理形态学变化,免疫组织化学染色检测肿瘤组织内Ki-67表达。结果:分离获得细胞表面CD80、CD86、HLA-DR表达分别达到88%、86%和90%的DC;MAGE-A3-DC-CIK组细胞表面CD8^(+)CD3^(+)、CD56^(+)CD3^(+)比例均高于DC-CIK组(P<0.01);经磁珠分选后获得CD133^(+)细胞比例高达90.23%的子宫内膜癌干细胞;与CIK组和DC-CIK组比较,MAGE-A3-DC-CIK组在不同效靶比下对子宫内膜癌干细胞的杀伤能力升高,细胞上清中IFN-γ、IL-2、IL-12及IL-17的分泌水平升高,培养液上清处理的子宫内膜癌干细胞凋亡率增加,差异均具有统计学意义(P<0.01);同时,与对照组和DC-CIK组比较,MAGE-A3-DC-CIK组移植瘤裸鼠的肿瘤体积小,肿瘤重量轻,肿瘤组织内细胞稀疏,Ki-67阳性细胞率减小,差异均具有统计学意义(P<0.01)。结论:负载MAGE-A3的DC与CIK联合培养能促进CIK成熟,提高对子宫内膜癌干细胞的杀伤性,并抑制移植瘤裸鼠的恶性进展。

TAA自身抗体联合CA125检测对卵巢癌早期诊断的价值

目的探讨六种肿瘤相关抗原(P53、Sur、IMP1、Cyclin D1、C-myc、Cyclin E)自身抗体联合CA125检测对卵巢癌早期诊断的价值。方法选取我院2012年1月至2013年1月住院的卵巢癌患者94例作为肿瘤组,其中早期卵巢癌患者54例,晚期卵巢癌患者40例,并收集同期健康体检者122例作为对照组,采用ELISA方法检测各组患者血清中六种TAA抗体和CA125情况,比较各组TAA抗体及CA125阳性率及敏感性。结果卵巢癌组患者血清中6种TAA抗体的阳性率均高于对照组;CA125联合6种TAA抗体检测在卵巢癌组的阳性率中达96.81%,较单独检测TAA抗体或6种TAA抗体联合检测阳性率及敏感性均高,6种TAA抗体联合CA125检测其约登指数为0.763,阳性似然比为4.72,阴性似然比为0.04;6种TAA抗体联合检测在早期和晚期卵巢癌患者中的阳性率比较无统计学差异;CA125单独检测在晚期卵巢癌患者阳性率(敏感性)明显高于早期患者;6种TAA抗体联合CA125检测在晚期卵巢癌患者阳性率(敏感性)明显高于早期患者,在早期患者明显高于单独CA125检测。结论采用6种TAA抗体联合CA125检测方法可靠真实,能有效提高早期卵巢癌的敏感性和特异性,对早期卵巢癌的诊断有一定参考价值。

MAGE-A4在肿瘤诊断与免疫治疗中的作用研究进展

肿瘤免疫治疗已成为继放化疗、靶向治疗后最终攻克癌症的希望之一,而肿瘤相关性抗原是免疫治疗的重要靶点。黑色素瘤相关抗原-A4(MAGE-A4)作为癌睾丸抗原,是MAGE-A亚家族的重要成员,具有很好的组织学特异性,在多种肿瘤组织中呈高表达,在正常组织(除睾丸、胎盘外)中均呈低表达。MAGE-A4参与细胞功能的调节,具有调控细胞周期、诱导细胞分化和生长、参与上皮-间质转化等重要作用,与肿瘤的发生、发展、转移及预后密切相关。目前,以MAGE-A4为靶点的T细胞受体转基因T细胞(TCR-T)免疫治疗,其Ⅰ期临床试验结果显示总体反应率(ORR)为23.7%、病情稳定率为47.4%,Ⅱ期临床试验正在开展,提示以MAGE-A4为靶点的TCR-T免疫治疗具有较高的临床应用价值。本文总结了MAGE-A4的结构和生物学功能及其在多种实体肿瘤中的最新研究进展和临床应用,旨在为MAGE-A4的临床转化及免疫靶向治疗提供理论基础。

CK20、P53、Ki67蛋白联合影像学特征与结肠癌分化程度及预后的关系

目的探讨细胞角蛋白20(CK20)、肿瘤抑制基因(p53)、细胞增殖核抗原Ki67(Ki67)联合影像学特征与结肠癌分化程度及预后的关系。方法以2017年1月至2021年6月首都医科大学附属北京友谊医院平谷医院收治的125例结肠癌患者为研究对象,均有保存切除的肿瘤组织,并按分化程度分为低分化组(n=41)、中分化组(n=51)、高分化组(n=33)。检测患者肿瘤组织中的CK20、P53、Ki67蛋白表达,CT记录结肠癌患者的影像学特征,比较不同分化程度患者肿瘤组织中的CK20、P53、Ki67蛋白表达及影像学特征。所有患者随访1年,并按预后情况分为预后良好组(n=107)及预后不良组(n=18),比较不同预后患者的CK20、P53、Ki67蛋白表达及影像学特征,ROC分析患者CK20、P53、Ki67蛋白对结肠癌患者不良预后的预测价值。结果不同分化程度组的CK20、P53、Ki67蛋白表达比较,低分组的CK20、P53、Ki67阳性蛋白表达均高于中、高分化组(χ^(2)=9.055,9.543,12.239,P<0.05);低分组的肠壁增厚程度、受累肠管长度、淋巴结数目及CT值均高于中、高分化组,差异有统计学意义(χ^(2)=7.571,6.493,F=24.101,22.491,6.373,P<0.05)。多因素Logistic回归分析显示,CK20、P53、Ki67阳性蛋白表达及影像学特征(肠壁增厚程度、受累肠管长度、淋巴结总数、最大淋巴结的短径及CT值)均是结肠癌患者预后的独立危险因素(P<0.05)。ROC曲线显示,CK20、P53、Ki67蛋白及三者联合检测曲线下面积为0.731、0.821、0.854、0.931。结论结肠癌患者肿瘤组织中CK20、P53、Ki67蛋白及影像学特征与患者的分化程度和预后有关,CK20、P53、Ki67蛋白联合检测对患者预后有较高的预测价值。

系统性硬化症发生肺动脉高压的独立危险因素分析

目的:探讨血清肿瘤相关抗原(TAAs)[包括癌胚抗原(CEA)、甲胎蛋白(AFP)、糖链抗原125(CA125)、糖链抗原15-3(CA15-3)、糖链抗原19-9(CA19-9)、糖链抗原72-4(CA72-4)和糖链抗原50(CA50)]与系统性硬化症(SSc)合并肺动脉高压(PAH)的关系。方法:采用病例对照方法探索7种血清肿瘤相关抗原与SSc-PAH及系统性硬化症不合并肺动脉高压(SSc-nonPAH)患者之间的关联。共纳入290例SSc患者,其中男41例,女249例,年龄中位数51岁,病程中位数7年。采用二元Logistic回归进行多因素分析。结果:SSc-PAH患者血清中的肿瘤相关抗原CEA、CA125、CA19-9、CA50均显著高于SSc-nonPAH患者(P<0.05)。多因素Logistic回归分析结果显示,SSc-PAH患者的血清CA125水平显著高于SSc-nonPAH患者(P=0.007)。结论:血清CA125是SSc发生PAH的独立危险因素,血清CA125含量可能是SSc合并PAH患者的有效生物标志物,可为SSc-PAH的诊断及预后提供一定的参考价值。

超声造影定量参数对Luminal型乳腺癌诊断价值及其与雄激素受体及Ki-67的相关性研究

目的:探讨超声造影定量参数在Luminal型乳腺癌诊断中的价值,分析Luminal型乳腺癌患者超声造影定量参数与其雄激素受体(AR)及肿瘤增殖细胞相关抗原Ki-67的相关性。方法:选取医院收治的90例Luminal型乳腺癌患者,并根据病理及免疫组化检测结果将其分为LuminalA型组(32例)和LuminalB型组(58例),比较两组患者超声造影表现差异及定量参数,同时比较定量参数与Ki-67及AR表达水平的相关性。结果:两组患者的超声造影增强强度、灌注缺损、增强边界及穿入血流表现比较,差异均有统计学意义(x^(2)=5.204,x^(2)=11.880,x^(2)=6.556,x^(2)=7.249;P<0.05)。LuminalB型组患者与LuminalA型组相比,病灶区域血流灌注的峰值强度(PI)上升,达峰时间(TTP)及平均渡越时间(TOF)下降,差异均有统计学意义(t=8.084,t=8.639,t=7.945;P<0.05)。LuminalA型组患者Ki-67及AR阳性检出率低于LuminalB型组,差异有统计学意义(x^(2)=4.224,x^(2)=4.262;P<0.05)。90例Luminal型乳腺癌患者PI与Ki-67和AR表达水平均呈正相关(r=0.159,r=0.657;P<0.05);TTP、TOF与Ki-67和AR表达水平均呈负相关(r=-0.537,r=-0.407;r=-0.503,r=-0.023;P<0.05)。结论:超声造影定量参数对Luminal型乳腺癌的临床诊断价值较高,并与AR、Ki-67具有一定的相关性,可用于对Luminal型乳腺癌状况变化的诊断评估。

肿瘤相关碳水化合物抗原的适配体研究

肿瘤细胞异常的糖基化模式是癌症的标志,在恶性转化和癌症进展中起着至关重要的作用。不同机制导致的肿瘤相关碳水化合物抗原(tumor-associated carbohydrate antigens,TACAs)不仅是临床肿瘤学诊断中公认的生物标志物,也为治疗干预提供了特定的靶点。适配体作为抗体或凝集素的有力替代品,近年来在碳水化合物的识别中展现了潜在的应用价值。本文聚焦于癌症中异常的糖基化改变,综述了目前TACAs识别适配体的开发进展。依据适配体筛选程序中的靶标来源,阐述了针对3种类型靶标,包括糖类分子、蛋白质聚糖表位,以及血清糖类抗原的筛选策略。从筛选方法、性能指标及相关应用性方面对适配体进行了总结,并讨论了当前研究中存在的问题和未来发展方向。

应用肿瘤相关抗原P53、IMPDH、LAMR1和ENO1的肽抗原检测非小细胞肺癌患者的自身抗体

目的本研究主要探讨肿瘤相关抗原(TAAs)P53、IMPDH、LAMR1和ENO1的自身抗体及其组合在非小细胞肺癌(NSCLC)检测中的潜在价值。方法应用免疫信息学数据库和免疫学软件设计并用固相合成法合成P53、IMPDH、LAMR1和ENO1的肽抗原(hAgs)。收集221名NSCLC患者和243名健康人的血标本,应用酶联免疫吸附试验(ELISA)方法检测NSCLC患者和健康人血清中P53、IMPDH、LAMR1和ENO1自身抗体的水平,对不同病理类型及分期的NSCLC自身抗体的水平进行分析。结果NSCLC患者血清中P53、IMPDH、LAMR1和ENO1自身抗体水平均显著上调(P<0.001),在NSCLC腺癌患者血清中的水平明显高于鳞癌(P<0.05);Ⅰ期NSCLC患者的P53、IMPDH、LAMR1和ENO1的自身抗体水平明显高于健康对照组(P<0.001)。结论肿瘤相关抗原P53、IMPDH、LAMR1和ENO1自身抗体,具有NSCLC的诊断潜能,同时显示出早期NSCLC筛查的潜能。