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从内镜超声引导下活检组织中培养胰腺癌类器官的策略见解。

Strategic insights into the cultivation of pancreatic cancer organoids from endoscopic ultrasonography-guided biopsy tissue.

机构信息

Institute of Hepatopancreatobiliary Surgery, Chongqing General Hospital, Chongqing University, Chongqing 401147, China.

出版信息

World J Gastroenterol. 2024 Nov 14;30(42):4532-4543. doi: 10.3748/wjg.v30.i42.4532.

Abstract

BACKGROUND

The frequent suboptimal efficacy of endoscopic ultrasound-guided fine-needle biopsy (EUS-FNB) to culture pancreatic cancer (PC) organoids (PCOs) poses a major challenge in the advancement of personalized medicine for advanced PC.

AIM

To explore how to obtain appropriate puncture tissues from EUS-FNB and optimize the strategy for efficiently constructing PCOs, providing an efficient tool for the advancement of personalized medicine.

METHODS

Patients who underwent EUS-FNB for the diagnosis of PC tissue were prospectively enrolled. We refined the endoscopic biopsy procedures and organoid cultivation techniques. All tissue specimens verified by on-site pathological assessment were cultured in a semi-suspended medium in a microfluidic environment. We assessed differences in PCOs cultured beyond and below five generations examining patient demographics, specimen and organoid attributes, and the sensitivity of organoids to a panel of clinical drugs through cell viability assays.

RESULTS

In this study, 16 patients with PC were recruited, one sample was excluded because onsite cytopathology showed no tumor cells. Successful organoid generation occurred in 93.3% (14 of 15) of the EUS-FNB specimens, with 60% (9 of 15) sustaining over five generations. Among these patients, those with a history of diabetes, familial cancer, or larger tumors exhibited enhanced PCO expandability. The key factors influencing long-term PCOs expansion included initial needle sample quality ( = 0.005), rapid initiation of organoid culture post-isolation ( ≤ 0.001), and high organoid activity ( = 0.031). Drug sensitivity analysis revealed a partial response in two patients following therapeutic intervention and surgery and stable disease in four patients, indicating a moderate correlation between organoid response and clinical outcomes.

CONCLUSION

Optimal initial needle sampling, rapid and precise biopsy sample processing, process isolated samples as soon as possible, and sufficient cellular material are crucial for successful cultivating PCOs. High organoid activity is an important factor in maintaining their long-term expansion, which is essential for shortening the time of drug sensitivity analysis and is the basis of PC research.

摘要

背景

经内镜超声引导下细针穿刺活检(EUS-FNB)培养胰腺癌细胞(PC)类器官(PCO)的疗效常不理想,这对推进晚期 PC 的个体化医学带来了重大挑战。

目的

探索如何从 EUS-FNB 获得合适的穿刺组织,并优化有效构建 PCO 的策略,为推进个体化医学提供有效的工具。

方法

前瞻性纳入因 PC 组织接受 EUS-FNB 诊断的患者。我们改进了内镜活检程序和类器官培养技术。所有经现场病理评估证实的组织标本均在微流控环境中的半悬浮培养基中培养。我们通过细胞活力测定评估了超过和低于五代培养的 PCO 之间的差异,考察了患者人口统计学特征、标本和类器官特征以及类器官对一组临床药物的敏感性。

结果

本研究共纳入 16 例 PC 患者,1 例样本因现场细胞学检查未见肿瘤细胞而被排除。EUS-FNB 标本中成功生成 PCO 的比例为 93.3%(14/15),其中 60%(9/15)能维持超过五代。在这些患者中,有糖尿病、家族性癌症或更大肿瘤史的患者,其 PCO 扩展性增强。影响长期 PCO 扩张的关键因素包括初始针样质量( = 0.005)、分离后快速启动类器官培养( ≤ 0.001)和高类器官活性( = 0.031)。药物敏感性分析显示,两名患者在接受治疗干预和手术后有部分缓解,四名患者病情稳定,表明类器官反应与临床结局之间存在中度相关性。

结论

优化初始针采样、快速准确的活检样本处理、尽快处理分离样本以及充足的细胞材料对于成功培养 PCO 至关重要。高类器官活性是维持其长期扩增的重要因素,这对于缩短药物敏感性分析时间和 PC 研究的基础至关重要。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7505/11572629/2778ac7f57a7/WJG-30-4532-g001.jpg

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