这项工作得到了太平洋大学的 SAAG 和 SEED 资助的支持。我们感谢 William Chan 博士授予 Odyssey 红外成像 205 系统的访问权限，并感谢 John Livesey 博士授予 SpectraMax iD3 微孔板检测仪的访问权限。我们感谢 Melanie Felmlee 博士对动物协议的技术建议。

动物研究是在太平洋大学机构动物护理和使用委员会 （IACUC） 的批准下进行的（动物协议 19R10 和 22R10）。本研究使用 8 只 5-6 周龄的雄性无胸腺裸鼠，体重 20-25 克，用参考的啮齿动物饮食饲养并在无病原体 （SPF） 条件下饲养。笼子、垫料和饮用水被高压灭菌并定期更换。小鼠体内肿瘤接种的示意图如图 1 所示。有关本协议中使用的所有材料和仪器的详细信息，请参阅 材料表 。
1. A549-iRFP 细胞三维 MCS 的建立
<ol><li>在 37 °C 下用 5% CO2 的潮湿气氛孵育 A549-iRFP 细胞（人肺腺癌），并在含有 10% 胎牛血清、1% 青霉素-链霉素和 1 μg/mL 嘌呤霉素的完全生长培养基 DMEM 中培养它们。</li>
	<li>使用 100 μL 补充有 0.3% 胶原蛋白的完全生长培养基，以 4,000 个细胞/孔的接种密度将 A549-iRFP 细胞接种到 96 孔超低附着度圆底球状微孔板中。</li>
	<li>将微孔板在 4 °C 下以 300 × g 离心 7 分钟，以促进 MCS 形成。在显微镜下检查 MCS 形态，以确保离心后细胞聚集。</li>
	<li>48 小时后，向每个孔中加入 100 μL 完全生长培养基，以达到每孔 200 μL 生长培养基的总体积。</li>
	<li>每隔一天用新鲜的完全生长培养基替换每个孔中的 100 μL 生长培养基。</li>
</ol>2. A549-iRFP MCS 的表征
<ol><li>使用显微镜观察和成像 MCS 形态，并使用 MATLAB 中的参考软件根据相差显微镜图像通过仿真估计 MCS 体积。<ol><li>在 ImageJ 软件中打开一张 MCS 图像。</li>
		<li>使用 手绘选择 选择 MCS 的边缘并将其添加到 ROI 管理器中。</li>
		<li>单击 Edit |选择 |Create Mask （创建蒙版）。</li>
		<li>单击 Edit |反转。</li>
		<li>单击 File （文件） |另存为 |蒂夫。</li>
		<li>打开 ReViSP 软件。</li>
		<li>通过单击打开保存的 TIFF 图像 浏览.</li>
		<li>单击 Start 完成 MCS 模拟。</li>
	</ol></li>
	<li>使用 700 nm 通道的红外成像系统测量 iRFP 荧光信号，并使用软件（例如 Image Studio）量化荧光信号。<ol><li>打开 Image Studio 软件。</li>
		<li>在 Channels 选项卡中，选择 700 和 Intensity = 5。</li>
		<li>在 Scan Controls（扫描控制） 选项卡中，选择 84 μm、 Medium（中等）、0.0 mm（0.0 mm）和 Flip Image（翻转图像）。将其他所有内容保留为默认值。</li>
		<li>单击 Start 开始 开始扫描。</li>
	</ol></li>
	<li>根据供应商方案，使用 3D 细胞活力测定法评估和定量细胞活力。</li>
	<li>根据供应商方案，使用 BCA 检测试剂盒评估和定量细胞蛋白。</li>
</ol>3. 用于肿瘤接种的 MCS 选择
注意：将 MCS 接种到球状体微孔板中并在常规生长培养基交换下生长 2-3 周后，选择具有以下适当特性的 MCS 进行肿瘤接种。
<ol><li>在显微镜下观察 MCS 形态，并选择具有圆形、整体光滑边缘但有 5-10 个粗糙芽（ 图 2F 中的箭头）且直径在 700-800 μm 范围内的 MCS。</li>
	<li>测量 iRFP 荧光（参见步骤 2.2）并选择荧光信号在平均值一个标准差内的 MCS。</li>
</ol>4. 肺内 MCS 接种
注意：在处理动物之前，使用 70% 异丙醇喷雾剂清洁手术台和工具。
<ol><li>用 80 mg/kg 氯胺酮和 12 mg/kg 甲苯噻嗪的 IP 注射麻醉每只小鼠;用镊子捏住小鼠脚，以确保完全麻醉。</li>
	<li>皮下注射 10 μL 盐酸丁丙诺啡 （0.3 mg/mL） 以减轻疼痛。</li>
	<li>在眼睛上涂抹眼药膏以防止干燥。</li>
	<li>将鼠标置于背侧姿势，并用胶带将四肢固定在伸展位置。</li>
	<li>用碘和酒精棉签棒对背部皮肤进行消毒。</li>
	<li>使用手术剪刀在左后侧切出 0.5-1 厘米的切口（图 1B）。小心地使用镊子分离肌肉和脂肪组织，直到可以看到胸壁和肺部运动。</li>
	<li>使用移液管将一个选定的 MCS 从微孔板转移到含有冰冷 PBS 的玻璃培养皿中。</li>
	<li>将 20 G 针头连接到 100 μL 玻璃注射器上，在冰上预冷，然后吸取 20 μL 预冷的 PBS 和 Matrigel 混合物 （1：1 v/v）。</li>
	<li>使用注射器从培养皿中快速吸出最小体积的 PBS-Matrigel 混合物中的一个 MCS，将 MCS 保持在针头的金属部分。 注意：紧紧握住注射器和柱塞，以防止 MCS 从针头中滑出。</li>
	<li>轻轻地将针头垂直插入两根肋骨之间至 ~3 mm 深，然后缓慢注入所有含有 MCS 的 20 μL PBS 和 Matrigel 混合物。 注意： 插入过程中避免用力过大，以防止损伤肺、脉管系统或心脏。</li>
	<li>小心地取下针头并在伤口上涂抹三联抗生素软膏。</li>
	<li>用手术夹密封切口，2 周后取下。 注意：不要缝合切口，因为缝合线可能会干扰荧光成像。裸鼠在手术后能够自然愈合。</li>
	<li>将动物放在红外线加热垫上，并用实验室湿巾覆盖以保持体温。监测动物至少 30-60 分钟，直到它醒来并正常移动。</li>
	<li>在最初的 48 小时内，每天 3 次皮下注射 10 μL 盐酸丁丙诺啡 （0.3 mg/mL） 以减轻疼痛。</li>
</ol>5. 术后监测
<ol><li>每 3-4 天测量一次体重。</li>
	<li>在小动物成像系统上以 700 nm 通道以四种姿势测量来自 iRFP 异种移植物的 iRFP 荧光信号：左、右、背侧和腹侧，同时通过吸入异氟醚（流速：1.5-2 L/min 氧气，含有 1.5% 异氟醚）在 2-3 分钟内保持小鼠处于麻醉状态。</li>
	<li>使用软件（例如，Image Studio）量化 体内 异种移植癌的净荧光强度。<ol><li>使用固定矩形（A1,200 x 125 像素）作为小鼠胸部区域的采样窗口。</li>
		<li>使用徒手功能在矩形 （A1） 内追踪小鼠的形状，并测量区域 A1 中的荧光强度 （F1）。</li>
		<li>使用另一个较小的矩形（A2,25 x 40 像素）测量小鼠在大腿区域的背景荧光 （F2）。</li>
		<li>使用公式 （1） 计算每只小鼠中异种移植癌的净荧光强度： <img alt="Equation 1" src="/files/ftp_upload/66787/66787eq01.jpg" style="margin: auto;">（1）</li>
	</ol></li>
</ol>

多细胞球体的肺内接种以模拟原位 NSCLC

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作者没有需要声明的利益冲突。

A549-iRFP MCS 的构建是一种简单且高度可重复的实验室程序，可以转化为多种细胞系的 MCS 形成。在离心和胶原蛋白的帮助下生成的 MCS 在 3-4 天内表现出更完整的实体瘤样结构。这种方法可确保形成坚固的球体，这些球体可以长时间保持其整体结构，通常为 2-3 周甚至更长时间，直到小芽开始出现。通过采用离心和胶原蛋白，我们对 MCS 的形成进行了标准化，确保了它们在我们的实验模型中的一致性?...

在所有肿瘤疾病中，肺癌不仅造成的生命损失最高，而且在美国每年的新患者人数也位居第二1。这种毁灭性的恶性肿瘤是现代医疗保健的主要障碍，敦促人们更深入地了解其错综复杂的生物学和更有效的治疗方式2。非小细胞肺癌 （NSCLC） 占肺癌的 85%，并倾向于发展为实体瘤3。肺癌面临的主要挑战之一是动态和异质性的肿瘤微环境，它深刻影响癌症的进展和对治疗干预的反应 4,5,6。在 NSCLC 的不同阶段，更深入地了解癌细胞与其微环境之间的相互作用，需要精细的病理模型来概括 NSCLC 进展的组织学特征。
在这方面，原位动物模型成为 NSCLC 研究的一个有前途的途径。与常用的皮下异种移植模型7 不同，原位模型的特点是癌细胞直接接种到起源器官中。对于肺癌，这意味着将癌细胞直接植入肺组织 8,9。因此，肺癌的原位模型更好地模拟了天然肿瘤微环境，包括邻近的组织、血管和免疫成分，从而提高了它们的生理和临床相关性。
三维多细胞球体 （MCS） 代表了另一种有前途的概括肿瘤环境特征的方法。大多数癌症的特征是其复杂的肿瘤微环境，包括各种细胞间相互作用、细胞外基质以及氧气和营养物质的梯度10,11。传统的 2D 细胞培养缺乏空间和结构复杂性，无法概括这些肿瘤特异性特征12。相比之下，适当大小的 MCS 具有异质结构，具有缺氧和坏死的核心，这不仅概括了肿瘤内微环境，还概括了防止药物渗透的生理屏障，这是抗癌治疗中耐药性的主要机制 13,14,15。
利用原位动物模型和 MCS 培养技术，MCS 已接种到免疫功能低下的小鼠中，以成功构建乳腺癌和前列腺癌的原位模型16,17。在此，我们报告了构建和表征肺癌小鼠原位异种移植模型的详细方法。该方法采用源自荧光人肺癌细胞 （A549-iRFP） 的 3D MCS 的肺内接种18。该模型提供了一个绝佳的机会来观察肺癌在与 NSCLC 的四个临床分期密切相关的阶段的体内进展。此外，该模型的异种移植癌对临床确定的抗肺癌药物顺铂有反应。

<table border="1" fo:keep-together.within-page="1" fo:keep-with-next.within-page="always">
	<tbody>
		<tr>
			<td>100 &#181;L Glass Syringe</td>
			<td>Hamilton</td>
			<td>Part/REF #80601</td>
			<td></td>
		</tr>
		<tr>
			<td>20 G Needle</td>
			<td>Thermo Fisher Scientific Inc.</td>
			<td>14 826D</td>
			<td></td>
		</tr>
		<tr>
			<td>96-well Ultra-Low-Attachment Spheroid Microplate&#160;</td>
			<td>Corning</td>
			<td>15-100-173</td>
			<td></td>
		</tr>
		<tr>
			<td>A549-iRFP</td>
			<td>Imanis Life Sciences&#160;</td>
			<td>CL082-STAN</td>
			<td></td>
		</tr>
		<tr>
			<td>AIN-93M Mature Rodent Diet&#160;</td>
			<td>Research Diets, Inc.</td>
			<td>D10012M</td>
			<td></td>
		</tr>
		<tr>
			<td>Athymic Nude Mouse</td>
			<td>Charles River Laboratories, Inc.</td>
			<td>Strain Code: 490; homozygous</td>
			<td></td>
		</tr>
		<tr>
			<td>BCA</td>
			<td>Pierce</td>
			<td>23227</td>
			<td></td>
		</tr>
		<tr>
			<td>Buprenorphine Hydrochloride</td>
			<td>Patterson Veterinary</td>
			<td>NDC Number: 42023-179-05</td>
			<td></td>
		</tr>
		<tr>
			<td>CellTiter-Glo 3D Cell Viability Assay</td>
			<td>Promega</td>
			<td>G9683</td>
			<td></td>
		</tr>
		<tr>
			<td>Collagen</td>
			<td>Gibco</td>
			<td>A1064401&#160;</td>
			<td></td>
		</tr>
		<tr>
			<td>DMEM</td>
			<td>Corning</td>
			<td>MT10013CV</td>
			<td></td>
		</tr>
		<tr>
			<td>Fetal Bovine Serum (FBS)</td>
			<td>Cytiva HyClone</td>
			<td>SH3039603</td>
			<td></td>
		</tr>
		<tr>
			<td>ImageJ</td>
			<td>Open source tool (https://imagej.net/ij/)</td>
			<td>N/A</td>
			<td></td>
		</tr>
		<tr>
			<td>Image Studio&#160;</td>
			<td>LI-COR</td>
			<td>Version 5.2</td>
			<td></td>
		</tr>
		<tr>
			<td>Isoflurane</td>
			<td>Patterson Veterinary</td>
			<td>NDC Number: 17033-0091-25</td>
			<td></td>
		</tr>
		<tr>
			<td>Ketamine</td>
			<td>Patterson Veterinary</td>
			<td>NDC Number: 50989-0161-06</td>
			<td></td>
		</tr>
		<tr>
			<td>Microscope&#160;</td>
			<td>Keyence</td>
			<td>Model number: BZ-X710</td>
			<td></td>
		</tr>
		<tr>
			<td>Matrigel</td>
			<td>Corning</td>
			<td>CB-40234</td>
			<td></td>
		</tr>
		<tr>
			<td>Odyssey Infrared Imaging 205 System&#160;</td>
			<td>LI-COR</td>
			<td>Model number: 9140</td>
			<td></td>
		</tr>
		<tr>
			<td>PBS</td>
			<td>Corning</td>
			<td>MT21040CV</td>
			<td></td>
		</tr>
		<tr>
			<td>Pearl Trilogy small animal imaging system&#160;</td>
			<td>LI-COR</td>
			<td>Model number: 9430</td>
			<td></td>
		</tr>
		<tr>
			<td>Penicillin-Streptomycin&#160;</td>
			<td>Corning</td>
			<td>MT30002CI</td>
			<td></td>
		</tr>
		<tr>
			<td>Puromycin</td>
			<td>Thermo Fisher Scientific Inc.</td>
			<td>AAJ67236XF</td>
			<td></td>
		</tr>
		<tr>
			<td>ReViSP software from MATLAB&#160;</td>
			<td>Open source tool on Sourceforge (https://sourceforge.net/projects/revisp/)</td>
			<td>N/A</td>
			<td></td>
		</tr>
		<tr>
			<td>Surgical Clips--AutoClip System</td>
			<td>Fine Science Tools</td>
			<td>12020-00</td>
			<td></td>
		</tr>
		<tr>
			<td>Xylazine</td>
			<td>Patterson Veterinary</td>
			<td>NDC Number: 61133-6017-01</td>
			<td></td>
		</tr>
	</tbody>
</table>

construction of an orthotopic xenograft model of non-small cell lung cancer mimicking disease progression and predicting drug activities

非小细胞肺癌 （NSCLC） 是一种高度致命的疾病，具有复杂且异质性的肿瘤微环境。目前，基于癌细胞悬液皮下接种的常见动物模型并不能概括 NSCLC 中的肿瘤微环境。在此，我们描述了一种小鼠原位肺癌异种移植模型，该模型采用三维多细胞球 （MCS） 的肺内接种。具体来说，荧光人 NSCLC 细胞 （A549-iRFP） 在含有胶原蛋白的低附着 96 孔微孔板中培养 3 周以形成 MCS，然后将其肋间接种到无胸腺裸鼠的左肺中，以建立原位肺癌模型。
与原始 A549 细胞系相比，A549-iRFP 细胞系的 MCS 对抗癌药物的反应相似。A549-iRFP 细胞的长波长荧光信号与癌细胞生长的常见标志物（包括球体体积、细胞活力和细胞蛋白水平）密切相关，因此可以通过荧光成像动态监测 体内 癌症生长。接种到小鼠体内后，A549-iRFP MCS 异种移植物可靠地经历了与 NSCLC 临床阶段非常相似的阶段，包括原发肿瘤的扩增、邻近继发性肿瘤的出现以及癌细胞向对侧右肺和远端器官的转移。此外，该模型对基准抗肺癌药物顺铂的反应具有预期的毒性和较慢的癌症进展。因此，这种 NSCLC 的小鼠原位异种移植模型将作为一个平台来概括疾病的进展并促进潜在抗癌药物的开发。

Among all oncological disorders, lung cancer not only inflicts the highest life loss but also claims the second-highest number of new patients every year in the US1. This devastating malignancy stands as a major obstacle in modern healthcare, urging for a deeper understanding of its intricate biology and more efficacious therapeutic modalities2. Non-small cell lung cancer (NSCLC) accounts for 85% of lung cancer and tends to develop into solid tumors3. One of the foremost challenges in lung cancer is the dynamic and heterogeneous tumor microenvironment, which profoundly influences the cancer&#39;s progression and responses to therapeutic interventions4,5,6. A deeper understanding of the interplay between cancer cells and their microenvironment at different stages of NSCLC calls for refined pathological models that recapitulate the histological features of NSCLC progression.
In this regard, orthotopic animal models emerge as a promising avenue for NSCLC research. Unlike commonly employed subcutaneous xenograft models7, orthotopic models feature cancer cells that are directly inoculated into the organ of origin. For lung cancer, this means implanting cancer cells directly into the lung tissue8,9. Consequently, orthotopic models of lung cancer better mimic the native tumor microenvironment, including the neighboring tissues, vessels, and immune components, thus improving their physiological and clinical relevance.
Three-dimensional multicellular spheroids (MCS) represent another promising approach to recapitulating features of the tumor environment. Most cancers are characterized by their complex tumor microenvironment, including the various cell-cell interactions, the extracellular matrix, and the gradients in oxygen and nutrients10,11. Traditional 2D cell cultures lack the spatial and structural complexity to recapitulate these tumor-specific features12. In contrast, MCS of appropriate size feature a heterogeneous structure with a hypoxic and necrotic core, which recapitulates not only the intratumoral microenvironment but also the physiological barrier against drug penetration, which is a major mechanism of drug resistance in anticancer therapy13,14,15.
Taking advantage of both the orthotopic animal models and the MCS culturing techniques, MCS have been inoculated to immune-compromised mice to successfully construct orthotopic models of breast cancer and prostate cancer16,17. Herein, we report the detailed methodology to construct and characterize a murine orthotopic xenograft model of lung cancer. This method employs the intrapulmonary inoculation of 3D MCS derived from fluorescent human lung cancer cells (A549-iRFP)18. This model offers an exceptional opportunity to observe the in vivo progression of lung cancer through stages that closely parallel the four clinical stages of NSCLC. Furthermore, the xenograft cancer of this model responded to the clinically established antilung cancer drug, cisplatin.

作者聚焦：建立小鼠非小细胞肺癌模型以开发抗癌药物纳米制剂

模拟疾病进展和预测药物活性的非小细胞肺癌原位异种移植模型的构建

Our research focused on developing nanoformulations of anticancer drugs. In order to evaluate anticancer activities, we established this murine non-small cell lung cancer model by inoculation of multicellular spheroids. We aim to validate this model's ability to replicate clinical stages, drug tumor progression, reflux imaging, and response to therapeutic treatments.We aim to establish a more clinically relevant model of non-small cell lung cancer. Traditional model using subcutaneous inoculation of 2D cell suspension lack the fidelity to a tumor microenvironment and disease progression. By utilizing multicellular spheroids and orthotopic inoculation, we bridge this gap, better mimicking non-small cell lung cancer complexity and therapy response.With this orthotopic animal model, we have opened avenues to investigate non-small cell lung cancer tumor microenvironment and screen normal molecule for anticancer activity. Our finding paved the way for deeper exploration into tumor biology and the developments of anticancer therapies.

A549-iRFP MCS 的表征 在胶原蛋白和离心的帮助下，A549-iRFP MCS 在球状微孔板中成功培养。当 MCS 在 1 周后达到约 500 μm 的直径时，A549 和 A549-iRFP MCS 都暴露于各种抗癌药物和制剂 3 天，然后在无药物生长培养基中再维持 4 天。A549-iRFP MCS 表现出与亲本 A549 细胞非常相似的反应模式。A549 和 A549-iRFP MCS 显示出与顺铂相似的剂量反应曲线和 IC50 值，顺铂是抗肺癌的一线抗癌药物之一<s...

Read this Scientific Article Protocol about Construction of An Orthotopic Xenograft Model of Non-small Cell Lung Cancer Mimicking Disease Progression and Predicting Drug Activities at JoVE.com

本研究提出了一种基于荧光 A549-iRFP 细胞多细胞球体肺内接种的原位非小细胞肺癌 （NSCLC） 模型。该模型根据长波长荧光的 动态体内 监测，概括了临床 NSCLC 分期和对顺铂的反应。

Non-small cell lung cancer (NSCLC) is a highly lethal disease with a complex and heterogeneous tumor microenvironment. Currently, common animal models ...

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Research

JoVE Journal

Cancer Research

Construction of An Orthotopic Xenograft Model of Non-Small Cell Lung Cancer Mimicking Disease Progression and Predicting Drug Activities

577 次观看.  University of the Pacific. 我们的研究重点是开发抗癌药物的纳米制剂。为了评估抗癌活性，我们通过接种多细胞球体建立了这种小鼠非小细胞肺癌模型。我们旨在验证该模型复制临床分期、药物肿瘤进展、反流成像和对治疗反应的能力。我们的目标是建立一个更具临床相关性的非小细胞肺癌模型。使用皮下接种 2D 细胞悬液的传统模型缺乏对肿瘤微环境和疾病进展的保?...