gall bladder cancer

胆囊癌
  • 文章类型: Journal Article
    胆囊癌(GBC)在某些地理区域的社会经济贫困人群中很常见。黄曲霉毒素是一种基因毒性的肝癌,它被认为在肝细胞癌的发病机制中起作用。然而,黄曲霉毒素在GBC发病机制中的作用尚不清楚。我们确定了血清AFB1-Lys白蛋白加合物(AAA)水平作为GBC患者黄曲霉毒素暴露的标志,并与无GBC患者进行了比较。评估了AAA水平与肿瘤的细胞遗传学(TP53突变和HER2/neu扩增)和放射学特征的关系。我们包括GBC病例(n=51)和非GBC对照(n=100)。GBC组(n=51)的平均血清AAA水平高于无GBC组(n=100)(26.1±12.2vs.13.1±11.9ng/mL;p<.001)。与不明确或阴性表达的人相比,HER2/neu表达与较高的AAA水平相关(43.9±3vs.28.6±10vs.19.3±7纳克/毫升;p<.001)。年龄较大(年龄>50岁)(比值比[OR]=3.2[CI:1.3-8.2];p=.013),幽门螺杆菌血清学阳性(OR=5.1[CI:1.4-17.8];p=0.012),GS的存在(OR=5[CI:1.5-16.9];p=.009)和可检测的AAA水平(OR=6.8[CI:1.3-35.7];p=.024)是所有研究受试者中GBC存在的独立危险因素.在携带GS的患者中,年龄较大(年龄>50岁)(OR=4.5[CI:1.3-14.9];p=0.015),女性(OR=3.8[CI:1.2-12.5];p=0.027),存在多重GS(OR=21.9[CI:4.8-100.4];p<.001)和高血清AAA水平(OR=5.3[CI:1.6-17.3];p=.006)是存在GBC的独立危险因素。年龄>50岁(OR=2.6[CI:1.3-5.2];p=.010)和经常食用花生(OR=2.3[CI:1.1-4.9];p=.030)是高血清AAA水平的独立危险因素。当前的研究对通过减少膳食黄曲霉毒素暴露来预防GBC具有意义。
    Gall bladder cancer (GBC) is common among the socioeconomically deprived populations of certain geographical regions. Aflatoxin is a genotoxic hepatocarcinogen, which is recognized to have a role in the pathogenesis of hepatocellular carcinoma. However, the role of aflatoxin in the pathogenesis of GBC is largely unknown. We determined serum AFB1-Lys albumin adduct (AAA) levels as a marker of aflatoxin exposure in the patients with GBC and compared to those without GBC. The relationship of AAA levels to cytogenetic (TP53mutation&HER2/neu amplification) and radiological characteristics of the tumor was assessed. We included GBC cases (n = 51) and non-GBC controls (n = 100). Mean serum AAA levels were higher in the GBC group (n = 51) than those without GBC (n = 100) (26.1 ± 12.2 vs. 13.1 ± 11.9 ng/mL; p < .001). HER2/neu expression was associated with higher AAA levels compared to those with equivocal or negative expression (43.9 ± 3 vs. 28.6 ± 10 vs. 19.3 ± 7 ng/mL; p < .001). Older age (age >50 years) (odds ratio [OR] = 3.2 [CI: 1.3-8.2]; p = .013), positive Helicobacter pylori serology (OR = 5.1 [CI: 1.4-17.8]; p = .012), presence of GS (OR = 5 [CI: 1.5-16.9]; p = .009) and detectable AAA levels (OR = 6.8 [CI: 1.3-35.7]; p = .024) were independent risk factors for the presence of the GBC among all study subjects. Among patients harboring GS, older age (age >50 years) (OR = 4.5 [CI: 1.3-14.9]; p = .015), female gender (OR = 3.8 [CI: 1.2-12.5]; p = .027), presence of multiple GS (OR = 21.9 [CI: 4.8-100.4]; p < .001) and high serum AAA levels (OR = 5.3 [CI: 1.6-17.3]; p = .006) were independent risk factors for the presence of the GBC. Elderly age >50 years (OR = 2.6 [CI: 1.3-5.2]; p = .010) and frequent peanut consumption (OR = 2.3 [CI: 1.1-4.9]; p = .030) were independent risk factors for high serum AAA levels. The current study has implications for the prevention of GBC through the reduction of dietary aflatoxin exposure.
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  • 文章类型: Journal Article
    目的:胆囊癌(GBC)由于其侵袭性和有限的治疗选择,在肿瘤学中提出了重大挑战。缺乏用于早期检测和预后的有效生物标志物加剧了GBC患者的预后。肿瘤出芽(TB)和肿瘤浸润淋巴细胞(TIL)已成为各种癌症的潜在预后指标。反映肿瘤-宿主免疫相互作用和肿瘤侵袭性。由于可用的文献有限,对GBC中TB和TILs的研究尤其重要。
    方法:这项回顾性观察性研究旨在评估GBC患者中TB和TILs与临床病理参数的相关性。临床病理数据是从接受手术切除的经组织学证实的GBC患者中收集的。使用标准化方法评估切片的TB和TIL。进行统计分析以评估这些参数与临床病理变量之间的关联。
    结果:肿瘤分期和分级与TB和TILs显著相关,表明它们作为预后标志物的潜力。高TB与晚期肿瘤分期和更高等级相关,而高TIL浸润与肿瘤早期分期和低分级有关。此外,TIL表现出与淋巴管浸润的显着关联。有趣的是,在TB和TIL之间观察到负相关,强调肿瘤侵袭性和宿主免疫反应之间的动态相互作用。
    结论:TB和TILs在GBC中具有预后意义,提供对其发病机制和潜在治疗靶点的见解。未来的研究探索GBC中肿瘤-宿主免疫相互作用的机制基础对于将这些发现转化为临床应用和改善患者预后至关重要。
    OBJECTIVE: Gallbladder carcinoma (GBC) poses significant challenges in oncology due to its aggressive nature and limited treatment options. The lack of effective biomarkers for early detection and prognosis exacerbates the prognosis for GBC patients. Tumor budding (TB) and tumor infiltrating lymphocytes (TILs) have emerged as potential prognostic indicators in various cancers, reflecting tumor-host immune interactions and tumor aggressiveness. The study of TB and TILs in GBC is particularly important due to the limited literature available.
    METHODS: This retrospective observational study aimed to evaluate the association of TB and TILs with clinicopathological parameters in GBC patients. Clinicopathological data were collected from patients with histologically confirmed GBC who underwent surgical resection. The sections were evaluated for TB and TILs using standardized methods. Statistical analysis was performed to assess associations between these parameters and clinicopathological variables.
    RESULTS: Tumor stage and grade showed significant associations with TB and TILs, indicating their potential as prognostic markers. High TB correlated with advanced tumor stage and higher grade, while high TIL infiltration was associated with early tumor stage and lower grade. Additionally, TILs exhibited a significant association with lymphovascular invasion. Interestingly, an inverse association was observed between TB and TILs, highlighting the dynamic interplay between tumor aggressiveness and host immune response.
    CONCLUSIONS: TB and TILs hold prognostic significance in GBC, offering insights into its pathogenesis and potential therapeutic targets. Future research exploring the mechanistic underpinnings of tumor-host immune interactions in GBC is crucial for translating these findings into clinical applications and improving outcomes for patients.
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  • 文章类型: Journal Article
    背景:胆道溢出(BS)是胆囊癌(GBC)初次胆囊切除术后的常见并发症。很少有研究探讨BS作为长期预后因素的重要性。我们对BS与GBC生存率之间的关系进行了荟萃分析。
    方法:于2023年2月进行了系统的文献检索。纳入了评估BS发生率及其与初次腹腔镜或开腹胆囊切除术患者长期预后的关系的研究。总生存期(OS),无病生存率(DFS),腹膜癌病(RPC)的发生率是主要终点。森林地块分析用于计算OS的合并风险比(HR),DFS,和RPC。元回归用于评估BS与围手术期危险因素之间的研究水平关联。
    结果:在已发表的181篇文章中,11例符合纳入标准,样本量为1116例。BS的发生率介于9%和67%之间。在汇总分析中,BS与OS较差相关(HR=1.68,95%置信区间[CI]=1.32-2.14),DFS(合并HR=2.19,95%CI=1.30-3.68),和更高的RPC(比值比=9.37,95%CI=3.49-25.2)。BS的发生率与较高的T分期无关,淋巴结转移,更高等级,正边距状态,再切除,或转化率。
    结论:我们的荟萃分析显示,BS是GBC中腹膜复发率较高和生存率较差的预测因子。BS与肿瘤特征或转化率无关。需要进一步的研究来确定BS的其他潜在危险因素,并研究理想的治疗方案以提高生存率。
    BACKGROUND: Biliary spillage (BS) is a common complication following initial cholecystectomy for gall bladder cancer (GBC). Few studies have explored the importance of BS as a long-term prognostic factor. We perform a meta-analysis of the association between BS and survival in GBC.
    METHODS: A systematic literature search was performed in February 2023. Studies evaluating the incidence of BS and its association with long-term outcomes in patients undergoing initial laparoscopic or open cholecystectomy for either incidental or resectable GBC were included. Overall survival (OS), disease-free survival (DFS), and rate of peritoneal carcinomatosis (RPC) were the primary end points. Forest plot analyses were used to calculate the pooled hazard ratios (HRs) of OS, DFS, and RPC. Metaregression was used to evaluate study-level association between BS and perioperative risk factors.
    RESULTS: Of 181 published articles, 11 met inclusion criteria with a sample size of 1116 patients. The rate of BS ranged between 9% and 67%. On pooled analysis, BS was associated with worse OS (HR = 1.68, 95% confidence interval [CI] = 1.32-2.14), DFS (pooled HR= 2.19, 95% CI = 1.30-3.68), and higher RPC (odds ratio = 9.37, 95% CI = 3.49-25.2). The rate of BS was not associated with higher T stage, lymph node metastasis, higher grade, positive margin status, reresection, or conversion rates.
    CONCLUSIONS: Our meta-analysis shows that BS is a predictor of higher peritoneal recurrence and poor survival in GBC. BS was not associated with tumor characteristics or conversion rates. Further research is needed to identify other potential risk factors for BS and investigate the ideal treatment schedule to improve survival.
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  • 文章类型: Journal Article
    黄色肉芽肿性胆囊炎(XGC)是慢性胆囊炎的罕见变种之一,其特征是胆囊炎伴急性和慢性炎症细胞浸润。富含脂质的巨噬细胞在GB壁中的壁内积累是该疾病的标志。XGC导致胆囊(GB)与周围结构紧密粘附,像十二指肠一样,结肠,和胃。强烈的GB炎症导致胆囊穿孔和胆囊与周围结构之间的瘘管连通的发展。这也可能导致形成接近模拟胆囊恶性肿瘤的炎性肿块。通常很难根据临床表现,甚至根据术中和放射学发现与GB癌(CaGB)区分,该问题只能在最终组织病理学(HPE)上解决。我们回顾了患者的介绍和调查,讨论我们在处理XGC此类病例时管理困境的方法,并回顾文献。
    Xanthogranulomatous cholecystitis (XGC) is one of the rare variants of chronic cholecystitis which is characterized by inflammation of gall bladder along with infiltration by acute and chronic inflammatory cells. Intramural accumulation of lipid laden macrophages in GB wall is the hallmark of the disease. XGC results in dense adhesion of gall bladder (GB) to surrounding structures, like duodenum, colon, and stomach. The intense GB inflammation results in gall bladder perforation and development of fistulous communication between gall bladder and surrounding structures. This may also lead to formation of inflammatory mass which closely mimic gall bladder malignancy. Often differentiation from carcinoma of GB (Ca GB) on the basis of clinical presentation and even on intra-operative and radiological findings is difficult, and the issue could only be resolved on final Histopathology (HPE). We review presentation and investigation of a patient, discuss our approach in managing dilemma in treating such cases of XGC, and review the literature.
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  • 文章类型: Journal Article
    在印度,胆囊癌(GBC)正在成为一种非常具有破坏性的肝胆肿瘤。印度每年GBC的新病例都很高。尽管最近有先进的多模态治疗方案,GBC患者的生存率很低。如果疾病在晚期诊断(有局部淋巴结转移或远处转移)或手术切除不可手术,这些患者的预后很差。所以,正在采取靶向治疗的观点。靶向治疗包括激素治疗,蛋白酶体抑制剂,信号转导和凋亡抑制剂,血管生成抑制剂,和免疫治疗剂。一种这样的信号转导抑制剂是特异性短干扰RNA(siRNA)或短发夹RNA(shRNA)。为了开发siRNA介导的治疗shRNA,尽管已经使用胆囊细胞进行了一些临床前研究来评估这些关键分子的功效,需要更多的临床试验。迄今为止,已经鉴定出许多这样的基因。这篇综述将讨论最近鉴定的与GBC相关的基因,以及那些在siRNA或shRNA治疗中具有意义的基因。
    Gall bladder cancer (GBC) is becoming a very devastating form of hepatobiliary cancer in India. Every year new cases of GBC are quite high in India. Despite recent advanced multimodality treatment options, the survival of GBC patients is very low. If the disease is diagnosed at the advanced stage (with local nodal metastasis or distant metastasis) or surgical resection is inoperable, the prognosis of those patients is very poor. So, perspectives of targeted therapy are being taken. Targeted therapy includes hormone therapy, proteasome inhibitors, signal transduction and apoptosis inhibitors, angiogenesis inhibitors, and immunotherapeutic agents. One such signal transduction inhibitor is the specific short interfering RNA (siRNA) or short hairpin RNA (shRNA). For developing siRNA-mediated therapy shRNA, although several preclinical studies to evaluate the efficacy of these key molecules have been performed using gall bladder cells, many more clinical trials are required. To date, many such genes have been identified. This review will discuss the recently identified genes associated with GBC and those that have implications in its treatment by siRNA or shRNA.
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  • 文章类型: Case Reports
    腹腔镜胆囊切除术是一种相当常见的手术,目前被认为是胆囊切除术的金标准。然而,在存在胆囊癌(GBC)的情况下进行腹腔镜手术与端口部位转移(PSM)的风险相关.此外,在少数情况下,即使在术后组织病理学上,GBC仍然隐匿,并且远程出现PSM。这里,我们描述了2例出现PSM的隐匿性原发性GBC病例,并定义了氟-18氟脱氧葡萄糖正电子发射断层扫描-计算机断层扫描在处理此类病例中的作用.
    Laparoscopic cholecystectomy is a fairly common procedure and is currently considered the gold standard for cholecystectomy. However, the laparoscopic procedure in the presence of gall bladder cancer (GBC) is associated with the risk of port-site metastasis (PSM). Furthermore, in few cases, GBC remains occult even on postoperative histopathology and presents with PSM remotely. Here, we describe two such cases of GBC with occult primary who presented with PSM and also defined the role of fluorine-18 fluorodeoxyglucose positron emission tomography-computed tomography in the management of such cases.
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  • 文章类型: Journal Article
    胆囊癌(GBC)的特点是具有高侵袭性和不良预后,腺癌是主要的组织学亚型。根据统计数据,诊断为晚期GBC的患者5年生存率低于5%。尽管有新颖的治疗技术,不能令人满意的结果可能与肿瘤细胞的潜在生物学特性和对化疗的耐药性有关。早期诊断比临床治疗更重要,因为它有助于确定癌症的病理阶段并有助于选择合适的药物。因此,了解GBC的确切发病机制和发现潜在的新型生物标志物对GBC的早期诊断具有重要意义。非编码RNA,比如microRNA,长链非编码RNA,和环状RNA,已经发现影响与癌症相关的靶基因的转录调节,直接或间接。microRNA是一组小的,非编码,内源性表达的单链RNA。miRNA在各种基本细胞过程中发挥重要作用。因此,miRNA具有作为GBC的有价值的生物标志物和治疗靶标的潜力。
    Gallbladder cancer (GBC) is characterized by a highly invasive nature and a poor prognosis, with adenocarcinoma being the main histological subtype. According to statistical data, patients diagnosed with advanced GBC have a survival rate of less than 5% for 5 years. Despite the novel therapeutic techniques, the unsatisfactory results could be related to the underlying biology of tumor cells and resistance to chemotherapy. Early diagnosis is more important than clinical therapy as it assists in determining the pathological stage of cancer and facilitates the selection of appropriate medication. Hence, it is very important to understand the precise pathogenesis of GBC and to discover potential novel biomarkers for early diagnosis of GBC. Non-coding RNAs, such as microRNAs, long non-coding RNAs, and circular RNAs, have been found to influence the transcriptional regulation of target genes associated with cancer, either directly or indirectly. microRNAs are a group of small, non-coding, single-stranded RNAs that are expressed endogenously. miRNAs play significant roles in various fundamental cellular processes. Therefore, miRNAs have the potential to serve as valuable biomarkers and therapeutic targets for GBC.
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  • 文章类型: Journal Article
    大多数患有胆囊癌(GBCa)的患者处于晚期阶段并且具有较差的存活率。目的是回顾性研究指导FNA在超级专业机构中在GBCa诊断中的作用,并描述北印度人群胆囊(GB)病变的细胞形态谱。
    包括2017年至2019年从原发性GB肿块或转移性肝占位性病变接受引导FNA的所有GBCa疑似病例。由两名细胞病理学家分别检索并分析了抽吸物涂片的细胞形态学特征。肿瘤病变根据WHO2019分类进行分类。
    在489例中,细针穿刺细胞学(FNAC)诊断463例(94.6%),其中417例(90.1%)为恶性肿瘤阳性,35(7.5%)为炎性,11例(2.4%)的恶性肿瘤尚无定论。未指明的腺癌(NOS)是330例(79.1%)中最常见的类型,而87例(20.9%)是异常变异。这些包括乳头状腺癌(22,5.2%),黏液腺癌(12,2.8%),印戒癌(2.0.4%),腺鳞癌(8,1.9%),鳞状细胞癌(10,2.4%),神经内分泌肿瘤(7,1.7%),未分化癌(24,5.7%)和非霍奇金淋巴瘤(2,0.4%),分别。细胞块上的免疫组织化学尽可能地证实了诊断。33例中有5例组织病理学不一致。
    指导FNAC是一项敏感的研究,在确认晚期GBCa患者的诊断和决定进一步的治疗方案中起着至关重要的作用。GBCa的不常见变体可以在细胞学上可靠地分类。
    UNASSIGNED: A majority of the patients with gall bladder cancer (GBCa) present at an advanced stage and have poor survival. The aim is to retrospectively study the role of guided FNA in the diagnosis of GBCa in a superspecialty institute and to describe the cytomorphologic spectrum of gall bladder (GB) lesions in the North Indian population.
    UNASSIGNED: All suspected cases of GBCa who underwent guided FNA from the primary GB mass or metastatic liver space-occupying lesion from 2017 to 2019 were included. The aspirate smears were retrieved and analyzed for cytomorphological features independently by two cytopathologists. The neoplastic lesions were classified according to the WHO 2019 classification.
    UNASSIGNED: Of 489 cases, fine needle aspiration cytology (FNAC) was diagnostic in 463 cases (94.6%), of which 417 (90.1%) were positive for malignancy, 35 (7.5%) were inflammatory, and 11 (2.4%) were inconclusive for malignancy. Adenocarcinoma not otherwise specified (NOS) was the most common type seen in 330 cases (79.1%) and 87 (20.9%) were unusual variants. These included papillary adenocarcinoma (22, 5.2%), mucinous adenocarcinoma (12, 2.8%), signet ring carcinoma (2,0.4%), adenosquamous carcinoma (8, 1.9%), squamous cell carcinoma (10, 2.4%), neuroendocrine neoplasms (7, 1.7%), undifferentiated carcinoma (24, 5.7%) and non-Hodgkin lymphoma (2,0.4%), respectively. Immunohistochemistry on the cell block confirmed the diagnosis wherever possible. Histopathology was discordant in 5 out of 33 cases.
    UNASSIGNED: Guided FNAC is a sensitive investigation that plays a crucial role in confirming the diagnosis and deciding the further treatment options in advanced-stage GBCa patients. The uncommon variants of GBCa can be reliably categorized on cytology.
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  • 文章类型: Journal Article
    未经证实:胆道癌(BTC)与预后不良有关,部分原因是它通常被诊断为晚期,强调对诊断性生物标志物的需求。该项目的目的是鉴定和验证可以区分BTC患者与非癌症对照的多蛋白特征。
    未经批准:在这项研究中,我们包括未接受BTC治疗的患者,健康的控制,以及良性疾病包括良性胆道疾病的患者。参与者分为三个不重叠的队列:基于病例对照的发现队列(BTC=186,对照=249);基于病例对照的验证队列(验证队列1:BTC=113,对照=241);以及基于队列研究的验证队列,其中包括参与者(BTC=8,对照=132),用于疑似癌症的诊断检查(验证队列2)。使用邻近延伸测定(Olink蛋白质组学)在血清和血浆中测量免疫肿瘤学(I-O)相关蛋白。套索和里奇回归用于在发现队列中产生I-O相关蛋白质和碳水化合物抗原19-9(CA19-9)的蛋白质特征。
    未经证实:十六个蛋白质特征,包括2到82种蛋白质,产生了。所有特征包括CA19-9和趋化因子C-C基序配体20。BTC患者与BTC患者之间的区别特征controls,发现队列的AUC范围为0.95至0.99,验证队列1的AUC范围为0.94至0.97。在验证队列2中,AUC范围为0.84至0.94。在验证队列2中,9个签名实现82%至84%的特异性,同时保持100%的灵敏度。所有特征表现优于CA19-9,并且包括>15种蛋白质的特征表现出最佳性能。
    UNASSIGNED:该研究表明,有可能产生可以成功区分BTC患者与非癌症对照的蛋白质特征。
    UNASSIGNED:我们试图寻找基于血液样本的蛋白质谱,以区分患有胆道癌的患者和没有癌症的患者。在不同组的患者中发现并测试了几种概况。这些资料成功地识别了大多数胆道癌患者,指出多蛋白签名在这种情况下的实用性。
    UNASSIGNED: Biliary tract cancer (BTC) is associated with a dismal prognosis, partly because it is typically diagnosed late, highlighting the need for diagnostic biomarkers. The purpose of this project was to identify and validate multiprotein signatures that could differentiate patients with BTC from non-cancer controls.
    UNASSIGNED: In this study, we included treatment-naïve patients with BTC, healthy controls, and patients with benign conditions including benign biliary tract disease. Participants were divided into three non-overlapping cohorts: a case-control-based discovery cohort (BTC = 186, controls = 249); a case-control-based validation cohort (validation cohort 1: BTC = 113, controls = 241); and a cohort study-based validation cohort including participants (BTC = 8, controls = 132) referred for diagnostic work-up for suspected cancer (validation cohort 2). Immuno-Oncology (I-O)-related proteins were measured in serum and plasma using a proximity extension assay (Olink Proteomics). Lasso and Ridge regressions were used to generate protein signatures of I-O-related proteins and carbohydrate antigen 19-9 (CA19-9) in the discovery cohort.
    UNASSIGNED: Sixteen protein signatures, including 2 to 82 proteins, were generated. All signatures included CA19-9 and chemokine C-C motif ligand 20. Signatures discriminated between patients with BTC vs. controls, with AUCs ranging from 0.95 to 0.99 in the discovery cohort and 0.94 to 0.97 in validation cohort 1. In validation cohort 2, AUCs ranged from 0.84 to 0.94. Nine signatures achieved a specificity of 82% to 84% while keeping a sensitivity of 100% in validation cohort 2. All signatures performed better than CA19-9, and signatures including >15 proteins showed the best performance.
    UNASSIGNED: The study demonstrated that it is possible to generate protein signatures that can successfully differentiate patients with BTC from non-cancer controls.
    UNASSIGNED: We attempted to find blood sample-based protein profiles that could differentiate patients with biliary tract cancer from those without cancer. Several profiles were found and tested in different groups of patients. The profiles were successful at identifying most patients with biliary tract cancer, pointing towards the utility of multiprotein signatures in this context.
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  • 文章类型: Journal Article
    未经证实:上皮-间质转化(EMT)是侵袭的心脏。与癌症进展和转移相关的EMT被称为III型EMT。β-catenin,E-cadherin,EMT和MMP9标记通常用于诊断目的。
    UNASSIGNED:我们使用这些标记通过免疫组织化学(IHC)研究胆囊癌(GBC)中肿瘤浸润深度的EMT,临床结果,和无病生存。
    未经评估:这是一项前瞻性病例对照研究。
    UNASSIGNED:包括70个胆囊(50GBC和20CC)。经过详细的组织学检查,根据表达的百分比和强度研究了免疫表达。
    UNASSIGNED:通过Studentt检验和方差分析比较CC和GBC之间的表达。Kaplan-Meier用于生存分析,并计算了协议范围(“Kappa”)。
    UNASSIGNED:GBC的发病年龄为49.40(11.6)岁,女性为主(F:M=4:1)。在88%(44/50)的GBC中,眼底参与其中。中分化腺癌最常见[54%;27/50]。在GBC中观察到E-cadherin(P=0.022)和β-catenin(P<0.001)的显着下调和MMP9的上调(P<0.001),它们之间存在显着关联。MMP9表达与较高的肿瘤分期显着相关,但与化疗反应相关。我们的结果表明,上皮-间质转化III型在GBC侵袭中起作用。MMP9过表达和膜β-连环蛋白的丢失可能被认为是不良临床结果和晚期疾病的标志物。
    UNASSIGNED: Epithelial-mesenchymal transition (EMT) is the heart of invasion. EMT associated with cancer progression and metastasis is known as type III EMT. Beta-catenin, E-cadherin, and MMP9 markers of EMT are routinely employed for diagnostic purposes.
    UNASSIGNED: We employed these markers to study EMT by immunohistochemistry (IHC) in gall bladder cancer (GBC) with respect to depth of tumor invasion, clinical outcome, and disease-free survival.
    UNASSIGNED: This was a prospective case-control study.
    UNASSIGNED: Seventy gall bladders were included (50 GBC and 20 CC). After detailed histology, immunoexpression was studied in terms of percentage and strength of expression.
    UNASSIGNED: Expression was compared between CC and GBC by Student t test and analysis of variance. Kaplan-Meier was used for survival analysis, and the extent of agreement (\"Kappa\") was calculated.
    UNASSIGNED: The age of incidence of GBC was 49.40 (+11.6) years with female predominance (F:M = 4:1). In 88% (44/50) of GBC, the fundus was involved. Moderately differentiated adenocarcinoma was most frequent [54%; 27/50]. Significant downregulation of E-cadherin (P = 0.022) and beta-catenin (P < 0.001) and upregulation in MMP9 (P < 0.001) were seen in GBC with respect to CC with significant association among them. MMP9 expression was significantly associated with higher tumor stage but with chemotherapeutic response. Our results display that epithelial-mesenchymal transition type III plays a role in GBC invasion. MMP9 overexpression and loss of membranous beta-catenin may be considered a marker for poor clinical outcomes and advanced disease.
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