我们感谢爱荷华大学的组织采购核心和 Kristen Coleman 博士提供患者肿瘤标本，并感谢妇产科的 Sofia Gabrilovich 博士协助生成 PDO 模型。我们还要感谢 Valerie Salvatico 博士（美国安捷伦）对手稿的批判性分析。我们感谢以下资金来源：NIH/NCI CA263783 和 DOD CDMRP CA220729P1 KWT;英国癌症研究中心、英国前列腺癌协会、前列腺癌基金会和医学研究委员会对 JSdB。资助者在实验的设计或分析或发表决定中没有任何作用。

用于患者来源的肿瘤类器官药物评估的自动动力学成像

<ol>
	<li>Drost, J., Clevers, H. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Organoids+in+cancer+research.">Organoids in cancer research.</a> Nat Rev Cancer. 18 (7), 407-418 (2018).</li><li>Lohmussaar, K., Boretto, M., Clevers, H. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Human-derived+model+systems+in+gynecological+cancer+research.">Human-derived model systems in gynecological cancer research.</a> Trends Cancer. 6 (12), 1031-1043 (2020).</li><li>Sachs, N., et al. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=A+living+biobank+of+breast+cancer+organoids+captures+disease+heterogeneity.">A living biobank of breast cancer organoids captures disease heterogeneity.</a> Cell. 172 (1-2), 373-386 (2018).</li><li>de Witte, C. J., et al. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Patient-derived+ovarian+cancer+organoids+mimic+clinical+response+and+exhibit+heterogeneous+inter-+and+intrapatient+drug+responses.">Patient-derived ovarian cancer organoids mimic clinical response and exhibit heterogeneous inter- and intrapatient drug responses.</a> Cell Rep. 31 (11), 107762 (2020).</li><li>Adan, A., Kiraz, Y., Baran, Y. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Cell+proliferation+and+cytotoxicity+assays.">Cell proliferation and cytotoxicity assays.</a> Curr Pharm Biotechnol. 17 (14), 1213-1221 (2016).</li><li>Driehuis, E., Kretzschmar, K., Clevers, H. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Establishment+of+patient-derived+cancer+organoids+for+drug-screening+applications.">Establishment of patient-derived cancer organoids for drug-screening applications.</a> Nat Protoc. 15 (10), 3380-3409 (2020).</li><li>Alzeeb, G., et al. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Gastric+cancer+cell+death+analyzed+by+live+cell+imaging+of+spheroids.">Gastric cancer cell death analyzed by live cell imaging of spheroids.</a> Sci Rep. 12 (1), 1488 (2022).</li><li>Deben, C., et al. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=OrBITS:+label-free+and+time-lapse+monitoring+of+patient+derived+organoids+for+advanced+drug+screening.">OrBITS: label-free and time-lapse monitoring of patient derived organoids for advanced drug screening.</a> Cell Oncol (Dordr). 46 (2), 299-314 (2023).</li><li>Tamura, H., et al. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Evaluation+of+anticancer+agents+using+patient-derived+tumor+organoids+characteristically+similar+to+source+tissues).">Evaluation of anticancer agents using patient-derived tumor organoids characteristically similar to source tissues).</a> Oncol Rep. 40 (2), 635-646 (2018).</li><li>Le Compte, M., et al. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Multiparametric+tumor+organoid+drug+screening+using+widefield+live-cell+imaging+for+bulk+and+single-organoid+analysis.">Multiparametric tumor organoid drug screening using widefield live-cell imaging for bulk and single-organoid analysis.</a> J Vis Exp. 190, 64434 (2022).</li><li>Hanson, K. M., Finkelstein, J. N. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=An+accessible+and+high-throughput+strategy+of+continuously+monitoring+apoptosis+by+fluorescent+detection+of+caspase+activation.">An accessible and high-throughput strategy of continuously monitoring apoptosis by fluorescent detection of caspase activation.</a> Anal Biochem. 564-565, 96-101 (2019).</li><li>Isherwood, B., et al. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Live+cell+in+vitro+and+in+vivo+imaging+applications:+accelerating+drug+discovery.">Live cell in vitro and in vivo imaging applications: accelerating drug discovery.</a> Pharmaceutics. 3 (2), 141-170 (2011).</li><li>Bi, J., et al. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Successful+patient-derived+organoid+culture+of+gynecologic+cancers+for+disease+modeling+and+drug+sensitivity+testing.">Successful patient-derived organoid culture of gynecologic cancers for disease modeling and drug sensitivity testing.</a> Cancers (Basel). 13 (12), 2901 (2021).</li><li>Binaschi, M., Zunino, F., Capranico, G. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Mechanism+of+action+of+DNA+topoisomerase+inhibitors.">Mechanism of action of DNA topoisomerase inhibitors.</a> Stem Cells. 13 (4), 369-379 (1995).</li><li>Park, Y. Y., Ahn, J. H., Cho, M. G., Lee, J. H. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=ATP+depletion+during+mitotic+arrest+induces+mitotic+slippage+and+APC/C(Cdh1)-dependent+cyclin+B1+degradation.">ATP depletion during mitotic arrest induces mitotic slippage and APC/C(Cdh1)-dependent cyclin B1 degradation.</a> Exp Mol Med. 50 (4), 1-14 (2018).</li><li>Lukonin, I., Zinner, M., Liberali, P. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Organoids+in+image-based+phenotypic+chemical+screens.">Organoids in image-based phenotypic chemical screens.</a> Exp Mol Med. 53 (10), 1495-1502 (2021).</li><li>Herpers, B., et al. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Functional+patient-derived+organoid+screenings+identify+MCLA-158+as+a+therapeutic+EGFR+x+LGR5+bispecific+antibody+with+efficacy+in+epithelial+tumors.">Functional patient-derived organoid screenings identify MCLA-158 as a therapeutic EGFR x LGR5 bispecific antibody with efficacy in epithelial tumors.</a> Nat Cancer. 3 (4), 418-436 (2022).</li><li>Ramm, S., et al. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=High-throughput+live+and+fixed+cell+imaging+method+to+screen+matrigel-embedded+organoids.">High-throughput live and fixed cell imaging method to screen matrigel-embedded organoids.</a> Organoids. 2 (1), 1-19 (2023).</li><li>Dekkers, J. F., et al. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=High-resolution+3D+imaging+of+fixed+and+cleared+organoids.">High-resolution 3D imaging of fixed and cleared organoids.</a> Nat Protoc. 14 (6), 1756-1771 (2019).</li><li>Van Hemelryk, A., et al. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Viability+analysis+and+high-content+live-cell+imaging+for+drug+testing+in+prostate+cancer+xenograft-derived+organoids.">Viability analysis and high-content live-cell imaging for drug testing in prostate cancer xenograft-derived organoids.</a> Cells. 12 (10), 1377 (2023).</li><li>Bi, J., et al. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Advantages+of+tyrosine+kinase+anti-angiogenic+cediranib+over+bevacizumab:+Cell+cycle+abrogation+and+synergy+with+chemotherapy.">Advantages of tyrosine kinase anti-angiogenic cediranib over bevacizumab: Cell cycle abrogation and synergy with chemotherapy.</a> Pharmaceuticals (Basel). 14 (7), 682 (2021).</li><li>Bi, J., et al. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=Blocking+autophagy+overcomes+resistance+to+dual+histone+deacetylase+and+proteasome+inhibition+in+gynecologic+cancer).">Blocking autophagy overcomes resistance to dual histone deacetylase and proteasome inhibition in gynecologic cancer).</a> Cell Death Dis. 13 (1), 59 (2022).</li><li>Guo, C., et al. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=B7-H3+as+a+Therapeutic+target+in+advanced+prostate+cancer.">B7-H3 as a Therapeutic target in advanced prostate cancer.</a> Eur Urol. 83 (3), 224-238 (2023).</li><li>Gil, V., et al. <a target="_blank" href="http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?db=PubMed&cmd=Search&doptcmdl=Citation&defaultField=Title+Word&term=HER3+is+an+actionable+target+in+advanced+prostate+cancer.">HER3 is an actionable target in advanced prostate cancer.</a> Cancer Res. 81 (24), 6207-6218 (2021).</li></ol>

KWT 是 Immortagen Inc. 的共同所有人，CJD 是安捷伦的员工。JSdB曾在安进、阿斯利康、安斯泰来、拜耳、Bioxcel Therapeutics、勃林格殷格翰、Cellcentric、第一、卫材、基因泰克/罗氏、Genmab、葛兰素史克、鱼叉、ImCheck Therapeutics、Janssen、Merck Serono、Merck Sharp & Dohme、Menarini/Silicon Biosystems、Orion、Pfizer、Qiagen、Sanofi Aventis、Sierra Oncology、Taiho、Terumo和Vertex Pharmaceuticals等公司担任顾问委员会委员;是癌症研究所 （ICR） 的一名雇员，该研究所的研究工作已获得 AZ、安斯泰来、拜耳、Cellcentric、第一、基因泰克、Genmab、葛兰素史克、杨森、默沙东、美纳里尼/Silicon Biosystems、Orion、赛诺菲安万特、Sierra Oncology、Taiho、辉瑞和 Vertex 的资助或其他支持，并且在阿比特龙、PARP 抑制 DNA 修复缺陷癌症方面具有商业利益， 和PI3K/AKT通路抑制剂（无个人收入）;被指定为发明人，对Janssen提交的专利8 822 438没有经济利益，该专利涵盖了醋酸阿比特龙与皮质类固醇的使用;曾是许多行业赞助的临床试验的CI/PI;并且是美国国家卫生研究所 （NIHR） 高级研究员。没有其他作者有任何潜在的利益冲突需要披露。

PDO 培养物因其能够反映细胞反应和行为而成为越来越流行的体外模型系统2。PDO的产生、培养和扩增技术已经取得了重大进展，但分析治疗反应的方法却滞后了。市售的 3D 活力试剂盒是裂解终点测定，错过了潜在有价值的动力学响应数据，并限制了其他方法的后续分析8。新兴研究正在应用活细胞成像来评估PDO模型中的药物反应。在这里，我们提出了一种利用多...

患者来源的肿瘤类器官 （PDO） 正在迅速成为研究癌症发展和治疗反应的强大模型系统。PDO 是三维 （3D） 细胞培养系统，可概括原发肿瘤的复杂基因组图谱和结构 1,2。与永生化癌细胞系的传统二维 （2D） 培养不同，PDO 捕获并维持肿瘤内异质性 3,4，使其成为机制和转化研究的宝贵工具。尽管PDO正在成为一种越来越受欢迎的模型系统，但与PDO培养物相容的市售试剂和细胞效应分析方法仍然有限。
缺乏可靠的方法来分析治疗反应的细微变化阻碍了临床转化。3D 培养物中的金标准细胞健康试剂 CellTiter-Glo 3D 利用 ATP 水平作为细胞活力的决定因素 5,6。虽然该试剂可用于终点检测，但也有一些注意事项，最明显的是检测完成后无法将样品用于其他目的。
活细胞成像是一种复杂的动力学显微镜，当与荧光试剂结合使用时，能够量化 PDO 模型中的各种细胞健康读数，包括细胞凋亡7、8、9 和细胞毒性10。事实上，活细胞成像一直是2D平台中化合物高通量筛选不可或缺的一部分11,12。像Incucyte这样的系统使这项技术变得负担得起，因此可以在各种环境中为研究小组所使用。然而，这些系统在分析3D培养物中的应用仍处于起步阶段。
在此，我们描述了一种使用多重活细胞成像评估癌症PDO模型中药物反应的方法（图1）。通过对明场图像的分析，可以动力学地监测PDO大小和形态的变化。此外，随着时间的推移，可以使用荧光试剂同时定量细胞过程，例如用于细胞凋亡的膜联蛋白 V 红色染料和用于细胞毒性的 Cytotox Green 染料。所提出的方法针对 Cytation 5 活细胞成像系统进行了优化，但该协议可能适用于不同的活细胞成像平台。

<table border="1" fo:keep-together.within-page="1" fo:keep-with-next.within-page="always">
	<tbody>
		<tr>
			<td>1.5 mL microcentrfuge tube</td>
			<td>Dot Scientific Inc</td>
			<td>1008113</td>
			<td></td>
		</tr>
		<tr>
			<td>15 mL conical centrifuge tube</td>
			<td>Sarstedt</td>
			<td>62.554.100</td>
			<td></td>
		</tr>
		<tr>
			<td>554 NM LED Cube</td>
			<td>Agilent</td>
			<td>1225012</td>
			<td></td>
		</tr>
		<tr>
			<td>96-well plate</td>
			<td>Corning Costar</td>
			<td>3596</td>
			<td>Prewarmed to 37 &#176;C</td>
		</tr>
		<tr>
			<td>96-well plate</td>
			<td>Agilent</td>
			<td>204626-100</td>
			<td>Prewarmed to 37 &#176;C</td>
		</tr>
		<tr>
			<td>A83-01</td>
			<td>Tocris</td>
			<td>2939</td>
			<td>Final concentration is 500 nM (component of organoid culture media)</td>
		</tr>
		<tr>
			<td>Advanced DMEM/F-12</td>
			<td>Gibco</td>
			<td>12634-010</td>
			<td>component of organoid culture media</td>
		</tr>
		<tr>
			<td>B27 Supplement</td>
			<td>Gibco</td>
			<td>17504044</td>
			<td>Final concentration is 1x (component of organoid culture media)</td>
		</tr>
		<tr>
			<td>BioTek BioSpa 8 Automated Incubator</td>
			<td>Agilent</td>
			<td>BIOSPAG-SN</td>
			<td>Tabletop incubator; BioSpa OnDemand scheduling software comunicates with Gen5 to transfer plates between the BioSpa and the Cytation 5 for imaging (this protocol uses version 1.01.10)</td>
		</tr>
		<tr>
			<td>BioTek Cytation 5 Cell Imaging Multimode Reader</td>
			<td>Agilent</td>
			<td>CYT5PW-SN</td>
			<td>Plate reader; Gen5 software is used for this device (this protocol uses version 3.12.08)</td>
		</tr>
		<tr>
			<td>Cultrex UltiMatrix Reduced Growth Factor Basement Membrane Extract</td>
			<td>R&#38;D Systems</td>
			<td>BME001-10</td>
			<td></td>
		</tr>
		<tr>
			<td>Daunorubicin HCl</td>
			<td>Sigma-Aldrich</td>
			<td>S3035</td>
			<td>Reconstituted in DMSO</td>
		</tr>
		<tr>
			<td>Dimethyl sulfoxide</td>
			<td>Sigma-Aldrich</td>
			<td>D2438</td>
			<td></td>
		</tr>
		<tr>
			<td>EDTA (0.5 M)</td>
			<td>Thermo Fisher</td>
			<td>AM9260G</td>
			<td></td>
		</tr>
		<tr>
			<td>Forskolin</td>
			<td>Tocris</td>
			<td>1099</td>
			<td>Final concentration is 10 &#181;M (component of organoid culture media)</td>
		</tr>
		<tr>
			<td>Glutamax</td>
			<td>Gibco</td>
			<td>35050-061</td>
			<td>Final concentration is 1x (component of organoid culture media)</td>
		</tr>
		<tr>
			<td>HEPES</td>
			<td>Gibco</td>
			<td>15630-080</td>
			<td>Final concentration is 10 mM (component of organoid culture media)</td>
		</tr>
		<tr>
			<td>Human EGF, Animal-Free Recombinant Protein</td>
			<td>Gibco</td>
			<td>AF-100-15-1MG</td>
			<td>Final concentration is 0.5 ng/mL (component of organoid culture media)</td>
		</tr>
		<tr>
			<td>Human FGF-10 Recombinant Protein</td>
			<td>Gibco</td>
			<td>100-26-1MG</td>
			<td>Final concentration is 10 ng/mL (component of organoid culture media)</td>
		</tr>
		<tr>
			<td>Human R-Spondin 1 Recombinant Protein</td>
			<td>Gibco</td>
			<td>120-38-5UG</td>
			<td>Final concentration is 250 ng/mL (component of organoid culture media)</td>
		</tr>
		<tr>
			<td>Hydrocortisone Stock Solution</td>
			<td>StemCell Technologies</td>
			<td>7926</td>
			<td>Final concentration is 500 ng/mL (component of organoid culture media)</td>
		</tr>
		<tr>
			<td>Imaging Filter Cube- GFP</td>
			<td>Agilent</td>
			<td>1225101</td>
			<td></td>
		</tr>
		<tr>
			<td>Imaging Filter Cube- TRITC</td>
			<td>Agilent</td>
			<td>1225125</td>
			<td></td>
		</tr>
		<tr>
			<td>Imaging LED GFP/CFP</td>
			<td>Agilent</td>
			<td>1225001</td>
			<td></td>
		</tr>
		<tr>
			<td>Incucyte Annexin V Red Dye</td>
			<td>Sartorius</td>
			<td>4641</td>
			<td>Reconstituted in organoid culture media</td>
		</tr>
		<tr>
			<td>Incucyte Cytotox Green Dye</td>
			<td>Sartorius</td>
			<td>4633</td>
			<td>DMSO solution</td>
		</tr>
		<tr>
			<td>N-Acetyl-L-cysteine</td>
			<td>Sigma-Aldrich</td>
			<td>A7250</td>
			<td>Final concentration is 1.25 mM (component of organoid culture media)</td>
		</tr>
		<tr>
			<td>Nexcelom Bioscience ViaStain AOPI Staining Solution</td>
			<td>Fisher-Scientific</td>
			<td>13366169</td>
			<td>Add 1:50 volume</td>
		</tr>
		<tr>
			<td>Nicotinamide</td>
			<td>Sigma-Aldrich</td>
			<td>N0636</td>
			<td>Final concentration is 10 mM (component of organoid culture media)</td>
		</tr>
		<tr>
			<td>Noggin</td>
			<td>R&#38;D Systems</td>
			<td>6057-NG</td>
			<td>Final concentration is 100 ng/mL (component of organoid culture media)</td>
		</tr>
		<tr>
			<td>Penicillin-Streptomycin</td>
			<td>Gibco</td>
			<td>15140122</td>
			<td>Final concentration is 10 units/mL (component of organoid culture media)</td>
		</tr>
		<tr>
			<td>Phosphate Buffered Saline (1x)</td>
			<td>Gibco</td>
			<td>14190-144</td>
			<td></td>
		</tr>
		<tr>
			<td>Primocin</td>
			<td>InvivoGen</td>
			<td>ant-pm-05</td>
			<td>Final concentration is 100 &#181;g/mL (component of organoid culture media)</td>
		</tr>
		<tr>
			<td>Recombinant Human Heregulin&#946;-1</td>
			<td>Pepro Tech</td>
			<td>100-03</td>
			<td>Final concentration is 37.5 ng/mL (component of organoid culture media)</td>
		</tr>
		<tr>
			<td>Staurosporine solution from Streptomyces sp.</td>
			<td>Sigma-Aldrich</td>
			<td>S6942</td>
			<td></td>
		</tr>
		<tr>
			<td>TrypLE Express</td>
			<td>Life Technologies</td>
			<td>12604013</td>
			<td></td>
		</tr>
		<tr>
			<td>Y-27632, CAS 331752-47-7</td>
			<td>Sigma-Aldrich</td>
			<td>688000</td>
			<td>Final concentration is 5 &#181;M (component of organoid culture media)</td>
		</tr>
		<tr>
			<td>&#946;-Estradiol</td>
			<td>Sigma-Aldrich</td>
			<td>E2758</td>
			<td>Final concentration is 100 nM (component of organoid culture media)</td>
		</tr>
	</tbody>
</table>

multiplexed live-cell imaging for drug responses in patient-derived organoid models of cancer

患者来源的癌症类器官 （PDO） 模型是一种多功能研究系统，与癌细胞系相比，它更好地概括了人类疾病。PDO模型可以通过在细胞外基底膜提取物（BME）中培养患者肿瘤细胞并将其铺成三维圆顶来生成。然而，针对单层培养物中的表型测定进行了优化的市售试剂通常与 BME 不兼容。在此，我们描述了一种使用自动活细胞成像系统对PDO模型进行板化和评估药物效果的方法。此外，我们应用与动力学测量兼容的荧光染料来同时量化细胞健康和细胞凋亡。图像捕获可以自定义为在几天内以固定的时间间隔进行。用户可以在单个 Z 平面图像或来自多个焦平面的连续图像的 Z 投影中分析药物效应。 使用掩蔽，计算感兴趣的特定参数，例如PDO数，面积和荧光强度。我们提供概念验证数据，证明细胞毒性药物对细胞健康、细胞凋亡和活力的影响。这种自动化动力学成像平台可以扩展到其他表型读数，以了解癌症PDO模型中的各种治疗效果。

Patient-derived tumor organoids (PDOs) are rapidly emerging as a robust model system to study cancer development and therapeutic responses. PDOs are three-dimensional (3D) cell culture systems that recapitulate the complex genomic profile and architecture of the primary tumor1,2. Unlike traditional two-dimensional (2D) cultures of immortalized cancer cell lines, PDOs capture and maintain intratumoral heterogeneity3,4, making them a valuable tool for both mechanistic and translational research. Although PDOs are becoming an increasingly popular model system, commercially available reagents and analysis methods for cellular effects that are compatible with PDO cultures are limited.
The lack of robust methods to analyze subtle changes in treatment response hinders clinical translation. The gold standard cell health reagent in 3D cultures, CellTiter-Glo 3D, utilizes ATP levels as a determinant of cell viability5,6. While this reagent is useful for endpoint assays, there are several caveats, most notably the inability to use samples for other purposes after completion of the assay.
Live-cell imaging is a sophisticated form of kinetic microscopy that, when combined with fluorescent reagents, has the capacity to quantify a variety of cell health readouts within PDO models, including apoptosis7,8,9 and cytotoxicity10. Indeed, live-cell imaging has been integral to high throughput screening of compounds in 2D platforms11,12. Systems such as the Incucyte have made the technology affordable and thus accessible to research groups in a variety of settings. However, the application of these systems to analyze 3D cultures is still in its infancy.
Herein, we describe a method to assess drug response in PDO models of cancer using multiplexed live-cell imaging (Figure 1). Through analysis of bright field images, changes in PDO&#160;size and morphology can be kinetically monitored. Furthermore, cellular processes can be simultaneously quantified over time using fluorescent reagents, such as Annexin V Red Dye for apoptosis and Cytotox Green Dye for cytotoxicity. The methods presented are optimized for the Cytation 5 live-cell imaging system, but this protocol may be adapted across different live-cell imaging platforms.

作者聚焦：为基于类器官的药物反应分析开发多重动力学分析

多重活细胞成像在患者来源的癌症类器官模型中用于药物反应

We apply patient derived organoid models, which are created from actual patient tumor specimens to examine how the tumors respond to drugs. We can also define the molecular characteristics that correlate with response. These results are then used to prioritize the best new therapies to advance in the clinical trials in the future.One of the main challenges in using patient derived organoid models is that they are a finite resource. In addition, there are very few off the shelf kits to assess drug response in organoid models that preserve the sample in a format that allows for other downstream analyses, such as transcriptomic profiling. We developed a multiplexed approach to kinetically monitor therapeutic response in organoid models.We use fluorescent dyes that are specific to different cellular processes, which provides insight into the mechanism of drug activity in each organoid model. In a single experiment we collect both functional and time course data and the samples are available for other assays. This method can be applied to assess response to a broad range of therapeutic modalities beyond small molecule inhibitors, including radiation sensitivity.We are also continuing to innovate by developing tools for other cellular phenotypes that can be kinetically measured, such as senescence.

我们的目的是证明使用多重活细胞成像来评估PDO治疗反应的可行性。在两个独立的子宫内膜癌PDO模型中进行了概念验证实验：ONC-10817和ONC-10811（ONC-10811数据见 补充图1 和 补充图2 ）。细胞凋亡（膜联蛋白 V 染色）和细胞毒性（Cytotox Green 摄取）对细胞凋亡诱导剂星形孢菌素进行动力学监测。具体而言，将PDO接种在96孔板中，用Annexin V Red和Cytotox Green染料处理，并置于37°C培?...

Watch this Scientific Journal Video about Multiplexed Live-Cell Imaging for Drug Responses in Patient-Derived Organoid Models of Cancer at JoVE.com

患者来源的肿瘤类器官是用于基础和转化研究的复杂模型系统。本文详细介绍了使用多重荧光活细胞成像对不同类器官表型进行同步动力学评估。

Patient-derived organoid (PDO) models of cancer are a multifunctional research system that better recapitulates human disease as compared to cancer cell ...

我们应用患者来源的类器官模型，这些模型是从实际的患者肿瘤标本创建的，以检查肿瘤对药物的反应。我们还可以定义与响应相关的分子特征。然后，这些结果将用于优先考虑最佳新疗法，以在未来的临床试验中取得进展。使用患者来源的类器官模型的主要挑战之一是它们是一种有限的资源。此外，很少有现成的试剂盒可以评估类器官模型中的药物反应，这些模型以允许其他下游分析（例如转录组学分析）的形式保存样本。我们开发了一种多路复用方法，用于动力学监测类器官模型中的治疗反应。我们使用特定于不同细胞过程的荧光染料，这提供了对每个类器官模型中药物活性机制的深入了解。在单个实验中，我们收集功能和时程数据，样品可用于其他检测。该方法可用于评估对小分子抑制剂以外的各种治疗方式的反应，包括辐射敏感性。我们还通过开发其他细胞表型（如衰老）的工具继续创新。

multiplexed-live-cell-imaging-for-drug-responses-patient-derived

Research

JoVE Journal

Cancer Research

Multiplexed Live-Cell Imaging for Drug Responses in Patient-Derived Organoid Models of Cancer

786 次观看.  University of Iowa. 我们应用患者来源的类器官模型，这些模型是从实际的患者肿瘤标本创建的，以检查肿瘤对药物的反应。我们还可以定义与响应相关的分子特征。然后，这些结果将用于优先考虑最佳新疗法，以在未来的临床试验中取得进展。使用患者来源的类器官模型的主要挑战之一是它们是一种有限的资源。此外，很少有现成的试剂盒可以评估类器官模型中的药物反应，这些模型以?...

视频: 作者聚焦：为基于类器官的药物反应分析开发多重动力学分析

Patient-derived organoid (PDO) models of cancer are a multifunctional research system that better recapitulates human disease as compared to cancer cell lines. PDO models can be generated by culturing patient tumor cells in extracellular basement membrane extracts (BME) and plating them as three-dimensional domes. However, commercially available reagents that have been optimized for phenotypic assays in monolayer cultures often are not compatible with BME. Herein, we describe a method to plate PDO models and assess drug effects using an automated live-cell imaging system. In addition, we apply fluorescent dyes that are compatible with kinetic measurements to quantify cell health and apoptosis simultaneously. Image capture can be customized to occur at regular time intervals over several days. Users can analyze drug effects in individual Z-plane images or a Z Projection of serial images from multiple focal planes. Using masking, specific parameters of interest are calculated, such as PDO number, area, and fluorescence intensity. We provide proof-of-concept data demonstrating the effect of cytotoxic agents on cell health, apoptosis, and viability. This automated kinetic imaging platform can be expanded to other phenotypic readouts to understand diverse therapeutic effects in PDO models of cancer.

Patient-derived tumor organoids are a sophisticated model system for basic and translational research. This methods article details the use of multiplexed fluorescent live-cell imaging for simultaneous kinetic assessment of different organoid phenotypes.

科研

癌症研究

Plating Intact Patient-Derived Organoids and Setting Up Imaging Parameters for Multiplexed Live-Cell Imaging

To begin, take a tube with patient-derived organoids or PDO suspension in an equal amount of basement membrane extracts, or BME. Using a 20 microliter pipette, seed five microliter domes into the center of each well of a pre-warmed 96 well plate. After seeding all the wells, place the lid on the plate and gently invert it.Incubate the inverted plate at 37 degrees Celsius for 20 minutes in the tissue culture incubator to allow the domes to solidify. Flip the plate over so that the lid is facing upwards. Then incubate again.After adding fluorescent dyes and drugs to the plates containing the PDOs. Place the plate in citation five. Start the Gen5 software and in the task manager window, select imager manual mode and click capture now.In the settings, specify the objective, filter, microplate format, and vessel type, select use lid and use slower carrier speed and click okay. Then choose a well of interest. Select the brightfield channel, click on auto expose and adjust the settings as required.Next to set up the Z stack, expand the imaging mode tab, select Z stack, and adjust the focus using the course adjustment arrows until all PDOs are out of focus. Establish this point as the bottom of the Z stack and repeat in reverse to set the top. Afterward, set up the fluorescent channels by opening the edit imaging step.Under channels, select the desired number of channels, designate one channel for the brightfield and additional channels for each fluorescent channel. Close the window by clicking okay, change the dropdown menu to the GFP to set the exposure for the first fluorescent channel, click auto expose and adjust the exposure settings under the exposure tab to reduce the background signal. To copy exposure settings to the image mode tab, click the copy icon and then click edit imaging step to open a new window.In the GFP channel, click the clipboard icon in the exposure line to add settings for illumination, integration time, and camera gain to the channel. Now click on the camera icon and choose image pre-processing under add processing step. On the brightfield tab, uncheck the apply image pre-processing option.For each fluorescent channel tab, ensure apply image pre-processing is checked. Deselect, use same options as channel one, and then click okay to close the window. Now click on Z projection under the add processing step, adjust the slice range if necessary, and close the window by clicking okay.To set up the protocol for kinetic imaging, in the toolbar click image set, and from the dropdown menu, choose create experiment from this image set. Click on options under the other heading and check the discontinuous kinetic procedure box. Under estimated total time, enter the runtime for the experiment.Close the window by clicking okay. Additionally, set plate layout and temperature gradient at this time. Validate the data reduction steps by clicking through the windows.Then navigate to file and click save protocol as in the toolbar. Select a save location. Enter a file name and click save.To begin kinetic imaging, load the protocol into the bio spa on demand scheduling software and choose an available slot. In the procedure info tab, select user from the menu. Next to the protocol slot, click select and choose add a new entry.Now click select next to the protocol slot. Click open to navigate and import the protocol into the scheduling software. Enter the required imaging time for the plate and click okay to close the window.Under interval, input the desired frequency of imaging, select schedule, plate, or vessel to initiate the plate validation sequence, click yes to accept this schedule.

电镀完整的患者来源的类器官并设置用于多重活细胞成像的成像参数

Image Analysis in Gen5 Software to Analyze Drug Response in Patient-Derived Organoids Using Multiplexed Live-Cell Imaging

To begin, image the fluorescently-labeled PDOs using the Cytation 5 live cell imaging system. Then, launch the Gen5 software. Navigate to Experiments and click Open in the Task Manager.Open the desired experiment and select Plate, followed by View in the toolbar. Then, switch the data dropdown menu to Z Projection. Double-click on a chosen well.Select Analyze. Click, I want to set up a new image analysis data reduction step, and click OK.In Analysis settings, set type to Cellular Analysis and detection channel to Z Projection transformed TSF Brightfield. Click Options to open the primary mask and count page.Check Auto in the threshold box, and click OK to close the popup window. Under Object Selection, define minimum and maximum object sizes to filter out cellular debris or single cells, and select other features as desired. Next, click Apply and the masked objects will be highlighted.To set up a subpopulation analysis in the cellular analysis toolbar, click on Calculated Metrics. Then, click Select or create object level metrics of interest at the bottom-right corner. From available object metrics, choose desired metrics, such as Circularity, and click Insert.Click OK to confirm. Next, select Subpopulation Analysis in the cellular analysis toolbar, and click Add to create a new subpopulation. Enter a name for the subpopulation.In the object metrics, click Add Condition to add a chosen metric. Input desired parameters in the Edit Condition window, and click OK.Select the desired results in the table at the bottom of the window and click OK, followed by Apply. Under Object Details, select the designated subpopulation to view masking.If satisfied, click OK in the Cellular Analysis window, and click Add Step to apply the analysis to all wells.