Gastric Cancer

胃癌
  • 文章类型: Journal Article
    微创手术在局部晚期胃癌(LAGC)治疗中提供了一些临床优势,尽管对其应用标准的共识仍不清楚。手术仍然是老年患者的谨慎选择,经常表现脆弱的人,合并症,和其他致残疾病。这项研究旨在评估腹腔镜胃切除术在患有LAGC的老年患者中的可能优势。这项回顾性研究分析了2015年至2020年间接受LAGC根治性切除的老年患者(≥75岁)的单中心系列。进行了开腹与腹腔镜入路的比较分析,关注术后并发症,住院时间(LOS),和长期生存。共有62例患者通过开放或腹腔镜方法进行了胃切除术(每位31例)。研究人群在人口统计学上没有显示出统计学上的显着差异,手术风险,和新辅助化疗。腹腔镜组报告显着减少了总体并发症(45.2vs.71%,p=0.039)和肺部并发症(0vs.9.7%,p=0.038)以及较短的LOS(8vs.12天,p=0.007)。两组淋巴结收获相等,尽管腹腔镜胃切除术后的长期总生存率显着改善(p=0.048),在无病生存率和疾病特异性生存率方面没有相关差异。腹腔镜胃切除术对老年LAGC患者有效,提供实质性的短期和长期术后益处。
    Minimally invasive surgery has provided several clinical advantages in locally advanced gastric cancer (LAGC) care, although a consensus on its application criteria remains unclear. Surgery remains a careful choice in elderly patients, who frequently present with frailty, comorbidities, and other disabling diseases. This study aims to assess the possible advantages of laparoscopic gastric resections in elderly patients presenting with LAGC. This retrospective study analyzed a single-center series of elderly patients (≥75 years) undergoing curative resections for LAGC between 2015 and 2020. A comparative analysis of open versus laparoscopic approaches was conducted, focusing on postoperative complications, length of hospital stay (LOS), and long-term survival. A total of 62 patients underwent gastrectomy through an open or a laparoscopic approach (31 pts each). The study population did not show statistically significant differences in demographics, operative risk, and neoadjuvant chemotherapy. The laparoscopic group reported significantly minimized overall complications (45.2 vs. 71%, p = 0.039) and pulmonary complications (0 vs. 9.7%, p = 0.038) as well as a shorter LOS (8 vs. 12 days, p = 0.007). Lymph node harvest was equal between the groups, although long-term overall survival presented significantly better after laparoscopic gastrectomy (p = 0.048), without a relevant difference in terms of disease-free and disease-specific survivals. Laparoscopic gastrectomy proves effective in elderly LAGC patients, offering substantial short- and long-term postoperative benefits.
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  • 文章类型: Journal Article
    背景:胃癌根治术仍是胃癌的主要治疗手段,尽管死亡率很高。使用匹配学习算法,基于西班牙EURECCA注册数据库开发了胃癌手术后90天死亡率(90DM)风险的临床预测模型。我们基于来自国际多中心患者队列的数据对该模型进行了外部验证。
    方法:选择来自欧洲GASTRODATA数据库的一组患者。人口统计,临床,并比较原始队列和验证队列中的治疗变量.使用随机森林模型的曲线下面积(AUC)评估模型的性能。
    结果:验证队列包括来自24家欧洲医院的2546名患者。先进的临床T-和N-类,新辅助治疗,开放程序,全胃切除术率,在验证队列中,中心的平均体积显著较高.在验证队列中,90DM的发生率也较高(5.6%)。原始队列(3.7%)。验证模型中的AUC为0.716。
    结论:在临床实践中,用于预测接受有治愈性胃切除术的胃癌患者90DM风险的外部验证模型仍然与原始模型一样有用。
    BACKGROUND: Radical gastrectomy remains the main treatment for gastric cancer, despite its high mortality. A clinical predictive model of 90-day mortality (90DM) risk after gastric cancer surgery based on the Spanish EURECCA registry database was developed using a matching learning algorithm. We performed an external validation of this model based on data from an international multicenter cohort of patients.
    METHODS: A cohort of patients from the European GASTRODATA database was selected. Demographic, clinical, and treatment variables in the original and validation cohorts were compared. The performance of the model was evaluated using the area under the curve (AUC) for a random forest model.
    RESULTS: The validation cohort included 2546 patients from 24 European hospitals. The advanced clinical T- and N-category, neoadjuvant therapy, open procedures, total gastrectomy rates, and mean volume of the centers were significantly higher in the validation cohort. The 90DM rate was also higher in the validation cohort (5.6%) vs. the original cohort (3.7%). The AUC in the validation model was 0.716.
    CONCLUSIONS: The externally validated model for predicting the 90DM risk in gastric cancer patients undergoing gastrectomy with curative intent continues to be as useful as the original model in clinical practice.
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  • 文章类型: Journal Article
    胃癌(GC)幸存者可能更容易发展为骨质疏松症。然而,关于GC与骨质疏松症之间关系的研究很少在大量患者人群中进行。我们旨在通过使用韩国国家健康保险服务-国家样本队列(KNHIS-NSC)将患者与GC和匹配的对照进行比较来确定骨质疏松症的发生率并确定相关因素。这项研究包括9078例GC患者和36,312例对照(1:4倾向评分匹配性别,年龄,residence,和收入)。根据Charlson合并症指数(CCI)评分调整模型(调整后的HR=1.13),GC患者骨质疏松症的风险比(HR)明显高于对照组。Kaplan-Meier分析显示,从索引日期开始的随访期间,GC患者的骨质疏松症累积发生率明显高于对照组(p=0.0087)。在年龄<65岁的人群中,骨质疏松与GC呈正相关。男性,和那些与CCI分数=0。总之,研究结果表明,年龄<65岁的GC男性患骨质疏松症的风险增加。需要研究其他风险因素和最佳干预时机,以预防骨折并最大程度地减少GC幸存者的骨丢失。
    Gastric cancer (GC) survivors may be more likely to develop osteoporosis. However, few studies on the relationship between GC and osteoporosis have been conducted on large patient populations. We aimed to determine the incidence of osteoporosis and identify related factors by comparing patients with GC and matched controls using the Korean National Health Insurance Service-National Sample Cohort (KNHIS-NSC). This study included 9078 patients with GC and 36,312 controls (1:4 propensity score-matched for sex, age, residence, and income). The hazard ratio (HR) for osteoporosis was significantly greater for GC patients than for controls according to Charlson Comorbidity Index (CCI) score-adjusted models (adjusted HR = 1.13). Kaplan-Meier analysis revealed that the cumulative incidence of osteoporosis during the follow-up period commencing from the index date was significantly greater in GC patients than in the controls (p = 0.0087). A positive correlation of osteoporosis with GC was detected for those aged < 65 years, males, and those with CCI scores = 0. In conclusion, the study findings suggest that men with GC aged < 65 years may be at an increased risk for osteoporosis. Research into additional risk factors and the optimal timing of interventions are needed to prevent fractures and minimize bone loss in GC survivors.
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  • 文章类型: Journal Article
    评估胃癌(n=68)和食管癌(n=43)患者的血清中IgG的蛋白水解片段。20名健康供体的血清样品用作对照。我们分析了止血指标(凝血酶原时间,纤维蛋白原,纤溶酶原活性,a2-抗纤溶酶活性,蛋白C活性)在血浆中和血清中总IgG的水平。健康供者的IgG-LysK中位数低于食管癌和胃癌患者。ROC分析显示食管癌组的敏感性(91%)和特异性(85%)高,但68%和85%,分别,胃癌患者。对癌症患者的假阴性IgG-LysK的分析表明,大多数患者患有晚期癌症并伴有转移。IgG-LysK值假阴性患者血浆中的总IgG比阳性样品低30%,而α2-抗纤溶酶水平升高,凝血酶原时间缩短。血液稳态的这些变化可能是IgG-LysK系数的假阴性值比例增加的原因。循环IgG-LysK水平在胃癌和食道癌等癌症的早期阶段增加。因此,当与其他更具体的这些病理标记一起用于面板时,这一指标可以显著增加癌症的早期发现。
    Blood serum of patients with gastric (n = 68) and esophageal (n = 43) cancer was assessed for proteolytic fragments of IgG. Serum samples of 20 healthy donors were used as a control. We analyzed indicators of hemostasis (prothrombin time, fibrinogen, plasminogen activity, a2-antiplasmin activity, protein C activity) in blood plasma and the level of total IgG in the blood serum. The median IgG-LysK of healthy donors was lower than in esophageal cancer and in patients with gastric cancer. ROC-analysis showed high sensitivity (91%) and specificity (85%) in the group with esophageal cancer but 68% and 85%, respectively, in patients with gastric cancer. Analysis of false negatives IgG-LysK in cancer patients showed that most patients had an advanced stage of cancer accompanied by metastases. Total IgG in the plasma of patients with false-negative IgG-LysK values was 30% lower than in samples with positive values, while the level of a2-antiplasmin was increased and the prothrombin time was shorter. These changes in blood homeostasis may be the reason for an increase in the proportion of false-negative values of the IgG-LysK coefficient. Circulatory IgG-LysK levels increase in the early stages of such cancers as gastric and esophageal cancers. Thus, when used in a panel with other more specific markers for these pathologies, this indicator can significantly increase the early detection of cancer.
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  • 文章类型: Journal Article
    由于其高侵袭性和多克隆肿瘤状态,胃癌被认为是严重的健康问题。在这项研究中,我们分析了Her2和Ki67与患者数据相关的预后因素的可能性.该研究包括在五年内接受手术治疗的48例胃肿瘤。位于胃中部区域的肠型腺癌的百分比具有统计学意义(p=0.05);在弥漫性亚型中,没有Her2阳性样本,在混合亚型中,三个样本中只有一个是Her2阳性。我们的结果证实了现有的数据,我们可以得出结论,这种联系可以被认为是进展和治疗有效性的预后因素。
    Due to its high aggressiveness and polyclonal tumor state, stomach cancer is considered a severe health problem. In this study, we analyzed Her2 and Ki67 in correlation with patient data for the possibility of prognostic factors. The study included 48 cases of gastric tumors that had been surgically treated in a period of five years. The percentage was statistically significant for intestinal-type adenocarcinomas located in the medio-gastric region (p = 0.05); in the diffuse subtype, there were no Her2 positive samples, and in the mixed subtype only one out of three samples was Her2 positive. Our results confirm the existing data, and we can conclude that this link can be considered a prognostic factor in the progression and treatment effectiveness.
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  • 文章类型: Journal Article
    胃癌是世界上第五大常见疾病和第四大最常见的死亡原因。它是通过食管胃十二指肠镜检查和活检诊断的;然而,早期发现病变存在局限性.最近,已经积极进行了使用液体活检来诊断各种癌症的研究,包括胃癌.来自癌症的各种物质反映在血液中。通过分析这些物质,预计不仅可以诊断癌症的存在或不存在,而且可以诊断癌症的类型。然而,这些物质的量非常小,甚至这些变量取决于个体的特征或癌症的特征。为了克服这些,我们使用MeDIP收集甲基化DNA片段,并将其与正常血浆进行比较,以确定胃癌组织或患者血浆的特征.我们试图利用通过癌组织和患者血浆反映在血液中的癌症特征来诊断胃癌。因此,我们证实了组织和血浆之间常见甲基化片段的一致性约为41.2%,我们发现通过SFR和5'端基序分析,使用片段的特征诊断和表征癌症的可能性.
    Gastric cancer is the fifth most common disease in the world and the fourth most common cause of death. It is diagnosed through esophagogastroduodenoscopy with biopsy; however, there are limitations in finding lesions in the early stages. Recently, research has been actively conducted to use liquid biopsy to diagnose various cancers, including gastric cancer. Various substances derived from cancer are reflected in the blood. By analyzing these substances, it was expected that not only the presence or absence of cancer but also the type of cancer can be diagnosed. However, the amount of these substances is extremely small, and even these have various variables depending on the characteristics of the individual or the characteristics of the cancer. To overcome these, we collected methylated DNA fragments using MeDIP and compared them with normal plasma to characterize gastric cancer tissue or patients\' plasma. We attempted to diagnose gastric cancer using the characteristics of cancer reflected in the blood through the cancer tissue and patients\' plasma. As a result, we confirmed that the consistency of common methylated fragments between tissue and plasma was approximately 41.2% and we found the possibility of diagnosing and characterizing cancer using the characteristics of the fragments through SFR and 5\'end-motif analysis.
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  • 文章类型: Journal Article
    自身免疫性萎缩性胃炎是一种免疫介导的疾病,导致专门的产酸胃壁细胞的自身免疫破坏。因此,在自身免疫性萎缩性胃炎中,胃酸分泌不可逆受损,而由此产生的低盐酸会导致主要的临床表现,并且是有联系的,直接或间接,这种疾病的长期肿瘤性并发症。在过去的几年里,自身免疫性萎缩性胃炎引起了人们越来越多的兴趣,从而获得了有关该疾病不同方面的新知识。尽管可靠的血清学生物标志物是可用的,并且胃肠内窥镜检查技术已经有了实质性的发展,自身免疫性萎缩性胃炎的诊断仍然受到相当大的延迟的影响,并且依赖于胃活检的组织病理学评估。诊断延迟的原因之一是引起临床怀疑的自身免疫性萎缩性胃炎的临床表现非常不同,范围从血液学到神经-精神病,再到胃肠道,很少见到妇产科症状或体征。因此,患有自身免疫性萎缩性胃炎的患者通常会向胃肠病学家以外的其他医学专业的医生寻求建议,因此强调需要在广泛的医学和科学界提高对这种疾病的认识。
    Autoimmune atrophic gastritis is an immune-mediated disease resulting in autoimmune destruction of the specialized acid-producing gastric parietal cells. As a consequence, in autoimmune atrophic gastritis, gastric acid secretion is irreversibly impaired, and the resulting hypochlorhydria leads to the main clinical manifestations and is linked, directly or indirectly, to the long-term neoplastic complications of this disease. In the last few years, autoimmune atrophic gastritis has gained growing interest leading to the acquisition of new knowledge on different aspects of this disorder. Although reliable serological biomarkers are available and gastrointestinal endoscopy techniques have substantially evolved, the diagnosis of autoimmune atrophic gastritis is still affected by a considerable delay and relies on histopathological assessment of gastric biopsies. One of the reasons for the diagnostic delay is that the clinical presentations of autoimmune atrophic gastritis giving rise to clinical suspicion are very different, ranging from hematological to neurological-psychiatric up to gastrointestinal and less commonly to gynecological-obstetric symptoms or signs. Therefore, patients with autoimmune atrophic gastritis often seek advice from physicians of other medical specialties than gastroenterologists, thus underlining the need for increased awareness of this disease in a broad medical and scientific community.
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  • 文章类型: Letter
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  • 文章类型: Journal Article
    编码NUAK家族激酶1(NUAK1)的基因经常被扩增,其表达上调,在各种癌症中激活致癌信号。然而,对其在胃癌(GC)中的作用知之甚少。我们调查了NUAK1、刺猬信号、和GC的肿瘤发生。NUAK1过表达在本地和公共GC队列中得到验证。患者来源的异种移植和转基因小鼠模型证明NUAK1消耗或抑制显著改善胃肿瘤发生。NUAK1通过激活STAT5介导的转录和稳定GLI1蛋白上调GLI1表达。NUAK1消耗或抑制损害癌细胞扩增,肿瘤形成,和体外和体内模型中的化疗抗性。临床病理分析证实,NUAK1表达上调与人GC预后不良和化疗耐药相关。我们的发现表明信号轴NUAK1/STAT5/GLI1促进癌细胞扩增和肿瘤发生,并表明NUAK1是GC中一个有吸引力的治疗靶标和预后因素。
    The gene encoding the NUAK family kinase 1 (NUAK1) is frequently amplified and its expression is upregulated, activating oncogenic signaling in various cancers. However, little is known about its role in gastric cancer (GC). We investigate the mechanistic links among NUAK1, Hedgehog signaling, and tumorigenesis in GC. NUAK1 overexpression is validated in local and public GC cohorts. Patient-derived xenograft and transgenic mouse models demonstrate that NUAK1 depletion or inhibition dramatically ameliorates gastric tumorigenesis. NUAK1 upregulates GLI1 expression by activating STAT5-mediated transcription and stabilizing GLI1 protein. NUAK1 depletion or inhibition impairs cancer cell expansion, tumor formation, and chemotherapy resistance in in vitro and in vivo models. Clinicopathological analysis confirms that upregulated NUAK1 expression correlates with poor prognosis and chemotherapy resistance in human GC. Our findings demonstrate that the signaling axis NUAK1/STAT5/GLI1 promotes cancer cell expansion and tumorigenesis and indicate that NUAK1 is an attractive therapeutic target and prognostic factor in GC.
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  • 文章类型: Journal Article
    背景:胃癌(GC)的死亡率很高,和强大的诊断生物标志物目前缺乏。然而,环状RNA(circularRNAs,circRNAs)作为GC生物标志物的临床相关性在很大程度上仍未被研究.
    目的:评估新型circRNAcirc_0004592在GC早期筛查和预后中的潜力。
    方法:进行circRNAs的高通量测序以筛选潜在的靶分子。在GC组织中检查Circ_0004592表达,细胞,和等离子体。从健康受试者中收集血浆样本,以及良性病变患者,癌前病变,和GC,此后评估了circ_0004592的诊断准确性。进一步分析血浆中circ_0004592水平与GC患者临床病理资料的相关性。
    结果:Circ_0004592在GC患者的组织和血浆中均上调。Further,癌前病变患者的circ_0004592表达高于健康对照组,而GC患者的表达最高。同一个病人,术后血浆circ_0004592水平低于术前水平。此外,circ_0004592水平与肿瘤分化显著相关,肿瘤深度,淋巴结转移。血浆circ_0004592的曲线下面积(AUC)表现出区分患有GC的患者与健康供体的高灵敏度和特异性。基于circ_0004592,癌胚抗原,和癌抗原199取得了优越的AUC和高度敏感。
    结论:血浆circ_0004592可能是GC患者的一种潜在的非侵入性辅助诊断生物标志物。
    BACKGROUND: Gastric cancer (GC) has a high mortality rate, and robust diagnostic biomarkers are currently lacking. However, the clinical relevance of circular RNAs (circRNAs) as GC biomarkers remains largely unexplored.
    OBJECTIVE: To evaluate the potential of novel circRNA circ_0004592 in the early screening and prognosis of GC.
    METHODS: High-throughput sequencing of circRNAs was performed to screen for potential target molecules. Circ_0004592 expression was examined in GC tissues, cells, and plasma. Plasma samples were collected from healthy subjects\' patients, as well as from patients with benign lesions, precancerous lesions, and GC, whereafter the diagnostic accuracy of circ_0004592 was evaluated. The correlation between circ_0004592 levels in plasma and clinicopathological data of patients with GC was further analyzed.
    RESULTS: Circ_0004592 was upregulated in both the tissue and plasma of patients with GC. Further, circ_0004592 expression was higher in patients with precancerous lesions than in healthy controls while being highest in patients with GC. In the same patient, the postoperative plasma level of circ_0004592 was lower than that in the preoperative period. Moreover, circ_0004592 level was significantly correlated with tumor differentiation, tumor depth, and lymph node metastasis. The area under the curve (AUC) of plasma circ_0004592 exhibited high sensitivity and specificity for differentiating patients with GC from healthy donors. Diagnosis based on circ_0004592, carcinoembryonic antigen, and cancer antigen 199 achieved a superior AUC and was highly sensitive.
    CONCLUSIONS: Plasma circ_0004592 may represent a potential non-invasive auxiliary diagnostic biomarker for patients with GC.
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