目的 探讨TAP水平与乳腺癌分子亚型及临床病理参数之间的相关性。方法 以2021年3月—2025年1月期间收治的150例乳腺癌病例为样本,采用静脉采血方式测定TAP凝聚物表面积指标,通过免疫组织化学EnVision双步染色技术,对雌激素受体(ER)、雄激素受体(AR)、孕激素受体(PR)、Ki-67及p53等表达水平进行分析,采用荧光原位杂交(FISH)对人表皮生长因子受体2(HER2)基因扩增状态进行检测。结果 150例患者中,TAP强阳性131例,TAP弱阳性15例,TAP阴性4例,TAP阳性率97.33%。免疫表型:ER阴性43例,ER阳性107例;AR阳性133例,AR阴性17例;PR阴性60例,PR阳性90例;p53阳性73例,p53阴性77例;HER2强阳性41例,HER2弱阳性89例,HER2阴性20例;Ki-67增殖指数≥20% 116例,Ki-67增殖指数<20% 34例。FISH对65例免疫组织化学检测结果为HER2(2+ )的乳腺癌病例进行基因扩增状态分析,其中阳性7例,阴性58例。Ki-67高增殖组TAP表达水平显著高于低增殖组(P<0.05);不同临床分期患者TAP表达水平存在差异(P<0.05);三阴型、HER2阳性型、Luminal A型和Luminal B型的患者之间的TAP表达水平存在差异(P<0.05),各分子分型(HER2阳性型、三阴型、Luminal A型和Luminal B型)与其对应非分型组的TAP表达均无统计学差异(均P>0.05)。结论 TAP在乳腺癌中广泛表达,且与Ki-67增殖指数、临床分期呈正相关。虽然不同分子分型间TAP表达存在总体差异,但具体亚型对比未显示显著性,后期需扩大样本量验证。
Objective To explore the relationship between tumor abnormal protein(TAP)level and molecular typing and clinicopathological features of breast cancer.Methods A total of 150 breast cancer cases admitted from March 2021 to January 2025 were enrolled in this study.The surface area of TAP condensates was measured using venous blood samples.The expression levels of estrogen receptor(ER),androgen receptor(AR),progesterone receptor(PR),Ki-67,and P53 were analyzed via immunohistochemistry(IHC)using the EnVision two-step staining technique.The amplification status of the human epidermal growth factor receptor 2(HER2+)gene was determined using fluorescence in situ hybridization(FISH).Results Among 150 patients,131 cases were strongly positive,15 cases were weakly positive and 4 cases were negative,with a positive rate of 97.33%.Immunophenotype:ER positive in 107 cases and ER negative in 43 cases,133 cases were positive for AR and 17 cases were negative,PR was positive in 90 cases and negative in 60 cases,73 cases were positive for p53 and 77 cases were negative.HER2 is strongly positive in 41 cases,weakly positive in 89 cases and negative in 20 cases.There were 116 cases with Ki-67 proliferation index ≥ 20% and 34 cases with Ki-67 proliferation index < 20%.Sixty-five cases of breast cancer HER2(2 )were detected in the later stage.by FISH,of which 7 cases were positive and 58 cases were negative.The expression level of TAP in patients with high Ki-67 proliferation index was higher than that in patients with low Ki-67 proliferation index(P<0.05).The expression level of TAP in patients with different clinical stages was different(P<0.05).There were differences in TAP expression levels among patients with triple negative type,HER2 positive type,Luminal A type and Luminal B type(P<0.05).There was no statistical difference in TAP expression between each molecular type(triple negative type,HER2 positive type,Luminal A type and Luminal B type)and its corresponding non-typing group(all P>0.05).Conclusions TAP is widely expressed in breast cancer,and it is positively correlated with Ki-67 proliferation index and clinical stage.Although there is a general difference in TAP expression among different molecular typing,the comparison of specific subtypes shows no significance,and it needs to be verified by expanding the sample size
目的 学习母细胞性浆细胞样树突细胞肿瘤(BPDCN)的临床病理及免疫表型特征,总结该少见肿瘤的病理诊断经验。方法 回顾分析2例BPDCN患者临床资料,通过苏木素-伊红(HE)染色分析肿瘤组织及细胞形态,通过免疫组织化学染色分析肿瘤免疫表型,通过流式细胞学检测骨髓有无肿瘤侵犯,并结合文献分析。结果 本报道中1例为97岁女性,临床以皮肤瘀斑结节为首发症状,肿瘤细胞真皮内弥漫浸润,不侵犯表皮,细胞中等大小,核形不规则,核仁不明显。另1例为69岁男性,临床以淋巴结肿大为首发症状,淋巴结结构完全破坏,肿瘤细胞弥漫浸润,细胞呈中等大小的母细胞样,核仁明显。2例免疫表型均表达CD123、CD4、CD56、TDT,不表达B系、T系淋巴细胞及髓系标志物,肿瘤均累及骨髓。结论 BPDCN是一种罕见的淋巴造血肿瘤,临床常以皮肤病变或淋巴结肿大为首发症状,临床过程具高度侵袭性,通常伴有骨髓侵犯。该肿瘤需与具有母细胞形态的淋巴系肿瘤和白血病相鉴别,诊断需结合临床信息、HE形态及免疫组化结果综合判断。
Objective To summarize the diagnostic experiences of blastic plasmacytoid dendritic cell neoplasm (BPDCN) based on the study of its clinicopathological features and immunophenotypes. Methods The clinical data of 2 patients with BPDCN were collected, the structure alteration and cell morphology were observed by HE staining, the immunophenotype of tumor cells were studied by immunohistochemistry staining and flow cytometry was adopted to confirm the bone marrow involvement. Results Two patients, one of whom was a 97 year-old female, presented with cutaneous ecchymosis nodules as the first symptom. The epidermis, but not the dermal, was diffusedly infiltrated by tumor cells, which were medium-sized with irregular nuclei without prominent nucleoli. The other case was a 69 year-old male with lymph node enlargement as the first symptom. The skin was normal, but the lymph nodes were invasively destroyed by tumor cells, which were medium-sized blast-like with prominent nucleoli. The immunophenotypes of the two patients were both positive for CD123, CD4, CD56 and TDT, but negative for B, T lymphocyte derived and myeloid origin markers, both of which involved bone marrow. Conclusions BPDCN is a rare form of hematological neoplasm, skin symptoms or lymph node enlargement may be presented as the initial symptom, the clinical course were highly aggressive with high frequency of bone marrow involvement. The blastic-like lymphoma and leukemia entities should be considered into account for differential diagnose. The precise diagnosis of BPDCN should be established by integrating histomorphology, immunophenotype and clinical presentation information comprehensively.
目的 探讨子宫内膜癌构成及临床病理特征。方法 以南平市第一医院2020年1月—2022年6月期间收治的82例子宫内膜癌患者为研究对象,收集其临床资料,通过免疫组织化学染色法检测4种错配修复蛋白表达,并分析错配修复蛋白表达与临床病理特征的关系。结果 82例患者中,70例(85.37%)为子宫内膜样癌,病理组织学类型以G1级30例(42.86%)为主,其他类型较为少见。错配修复蛋白表达总缺失率为35.71%,其中MUTL同源物1(MLH1)单独缺失率为2.86%,错配修复蛋白2抗体(MSH2)为4.29%,错配修复蛋白6抗体(MSH6)为14.29%,肿瘤错配修复基因PMS2抗体(PMS2)为14.29%;错配修复表达缺失(dMMR)组患者年龄50岁以上、伴脉管侵犯和淋巴结转移、组织学G3级和FIGO分期Ⅲ期占比高于错配修复表达正常(pMMR)组患者(P<0.05);MSH6蛋白表达缺失易发生在年龄50岁以上、有家族相关疾病史的患者(P<0.05);PMS2蛋白表达缺失易发生在组织学G2级、FIGO分期Ⅲ期、妊娠1次及以上、脉管内癌栓和淋巴结转移的患者(P<0.05)。结论 子宫内膜癌错配修复蛋白表达与其部分临床病理特征存在密切关联,可为患者后续治疗提供有价值的指导。
Objective To investigate the composition and clinicopathological features of endometrial carcinoma.Methods A total of 82 cases of endometrial carcinoma patients admitted to the First Hospital of Nanping City from January 2020 to June 2022 were studied.Epidemiological data were collected,and the expression of 4 mismatch repair proteins were detected by immunohistochemical staining,and their relationship with clinicopathological features was analyzed.Results Among 82 patients,70 cases(85.37%)were endometrioid carcinoma,and 30 cases(42.86%)were mainly G1 grade,other types were rare.The total deletion rate of mismatch repair proteins expression was 35.71%,in which MLH1 alone was 2.86%,MSH2 was 4.29%,MSH6 was14.29% and PMS2 was14.29%.The proportions of dMMR patients over 50 years old,with vascular invasion and lymph node metastasis,G3 grade histology and FIGO stage Ⅲ were significantly higher than those of the pMMR group(P<0.05).The loss of MSH6 protein expression was more likely to occur in patients over 50 years old with a family history of related diseases(P<0.05).The deletion of PMS2 protein expression was more likely to occur in patients with histological G2 grade,FIGO stage III,pregnancy of once or more and intravascular cancer thrombin and lymph node metastasis(P<0.05).Conclusions The expression of mismatch repair proteins in endometrial carcinoma is closely related to some clinicopathological features,which provides valuable guidance for follow-up treatment.
目的 探讨乳腺癌原发病灶超声声像图特点及病理分子分型与腋窝淋巴结转移的相关性。方法 回顾性分析106例接受乳腺超声检查及腋窝淋巴结活检,病理确诊为乳腺癌的患者资料。超声观察乳腺癌原发病灶的位置、大小、有无钙化、纵横比、内部血流、腋窝淋巴结声像图特点,结合临床病理学特点,分析与腋窝淋巴结转移相关的因素。结果 超声诊断未见明显异常的腋窝淋巴结75例,可疑的腋窝淋巴结31例;病理证实腋窝淋巴结未转移70例,转移36例。灵敏度66.7%、特异度90%、阳性预测值77.4%、阴性预测值84%。单因素分析显示原发肿块的位置、最大径、腋窝淋巴结淋巴门消失、ER表达与腋窝淋巴结转移有关(P<0.05 )。多因素分析显示原发肿块的位置、腋窝淋巴结淋巴门消失与腋窝淋巴结转移有关(P<0.05)。结论 腋窝淋巴结常规超声检查结合乳腺癌原发病灶超声声像图及病理分子分型有助于评估腋窝淋巴结状态。
Objective To analyse the ultrasonographic features and pathological molecular typing of the primary lesions and axillary lymph node (ALN) of breast cancer related to axillary lymph node metasta-sis(ALNM). Methods The Grey-scale and color Doppler ultrasound and axillary lymph node biopsy were performed in 106 patients with breastcarcinomas. The observed features included the position,the most dimen-sion,inner calcification,aspect ratio,the type of blood supply of the primary tumor and axillary lymph node image. Combining with the clinicopathological features, we analyzed the factors associated with axillary lymph node metastasis. Results Ultrasound found normal axillary lymphnodes in 70 patients and abnormal in 31 patients. Pathology confirmed axillary lymph node metastasis in 36 patients, and no metastasis in 70 patients.The sensitivity, specificity, positive predictive value, negative predictive value were 66.7%, 90%, 77.4% and 84% r-espectively.Univariate analysis showed that the location, maximum diameter, lymphnode with disappearance hilus and ER expression were related to axillary lymph node metastasis (P< 0.05). Multivariate analysis showed that the location of primary mass and lymph node with disappearance hilus were related to axillary lymph node metastasis (P< 0.05). Conclusion Axillary lymph node routine ultrasound examination combined with ultrasonographic and pathological molecular typing of primary breast cancer is helpful to evaluate axillary lymph node status.
目的 探讨子宫内膜微腺体癌的临床病理特征、诊断及鉴别诊断。方法 对1例首诊误诊为子宫颈微腺体增生的子宫内膜微腺体癌病例进行临床、病理组织学及免疫组织化学特征的观察及总结,同时进行相关文献复习。结果 本例患者年龄61岁,因绝经后阴道不规则流血1年就诊,B超提示子宫内膜不规则增厚,并行分段诊刮术,先后两次诊刮标本光镜下均见黏液性柱状上皮呈乳头状及网格状结构,细胞轻度异型,核分裂罕见,间质内大量中性粒细胞浸润伴腺上皮内“微脓肿”形成;免疫组化示:上皮成分P16弥漫强(+),CEA小灶(+),Vimentin弥漫(+),ER约90%(+,中-强),PR约90%(+,弱),Ki-67约3%(+),间质细胞CD10(+)、CD34(-)。结论 子宫内膜微腺体癌是一种极为罕见的子宫内膜黏液腺癌,其组织学形态与子宫颈良性病变微腺体增生十分相似,易于混淆,但通过免疫组化检查及详细地临床病史资料收集、分析,可以与其鉴别,从而做出正确地诊断。
Objective To investigate clinical and histopathological features, dignosis and differential diagnosis of the endometrial microglandular adenocarinoma (MGA). Methods The clinical and pathological features of microglandular adenocarinoma in a patient were observed. Immunohistochemical staining and literature review were also used. Results In the case, the age of patient was 61 years. Clinical manifestation was vaginal irregular bleeding for 1 year. Type-B ultrasound suggested endometrium was irregular thickening. Histologically, it was mainly composed of irregular shape, closely spaced small glands, and glandular cells was mild atypical. Mitosis was rarely observed. The endometrial stromata between gland were rare, but neutrophil were much observed with the formation of neutrophil microabscess in the glandular epithelium. Immunohistochemical study showed neoplastic cells were diffuse and strongly positivity for P16, diffuse positivity for vimentin, focally positive for CEA. ER and PR expression was found in approximately 90% tumor cells. The index of Ki-67 was about 3%. Interstitial cells were positivity for CD10, negativity for CD34. Conclusion The microglandular adenocarcinoma is a rare endometrial adenocarcinoma. It can be differentiated from cervical microglandular hyperplasia(MGH) and cervical mucinous adenocarcinoma by immunohistochemistry and morphological characteristics.
