健康供体和急性移植物抗宿主疾病患者 T 细胞反应的比较评估:定制免疫监测平台

Mohini Mendiratta, Meenakshi Mendiratta, Sandeep Rai, Ritu Gupta, Sameer Bakhshi, Mukul Aggarwal, Aditya Kumar Gupta, Hridayesh Prakash, Sujata Mohanty, Ranjit K Sahoo
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CD3+ T-cell were isolated and stimulated with varying concentrations of PHA (1-10μg/ml) and IL-2 (50-500 IU/ml). Cell proliferation was assessed using MTS and CFSE assays, while apoptosis was evaluated with Annexin V/7-AAD staining. Results: We observed enhanced proliferation of healthy individuals at higher PHA concentrations (5-10μg/ml), whereas aGVHD patients exhibited heightened proliferation at lower PHA concentrations (1-2.5μg/ml) at 48 hours. Prolonged exposure to PHA led to decreased proliferation in aGVHD patients, while healthy individuals continued to show increased proliferation at 72 hours with optimal PHA concentrations of 5.0-7.5μg/ml. The CFSE assay confirmed these findings, showing a higher proliferation rate in healthy individuals at elevated PHA concentrations and in aGVHD patients at lower concentrations. 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引用次数: 0

摘要

背景:T细胞的活化和增殖对于了解健康和病理情况下的免疫反应(如急性移植物抗宿主病(aGVHD))至关重要。植物血凝素(PHA)和白细胞介素-2(IL-2)常用于研究T细胞动态的体外试验。我们的研究旨在确定 PHA 和 IL-2 促进 T 细胞增殖和存活的最佳浓度,并评估这些条件如何影响健康人与 AGVHD 患者的 T 细胞反应:收集年龄和性别匹配的健康人(10 人)和 aGVHD 患者(10 人)的外周血样本。分离 CD3+ T 细胞并用不同浓度的 PHA(1-10μg/ml)和 IL-2(50-500 IU/ml)刺激。用 MTS 和 CFSE 检测法评估细胞增殖,用 Annexin V/7-AAD 染色法评估细胞凋亡。结果我们观察到健康人在较高 PHA 浓度(5-10μg/ml)下细胞增殖增强,而 aGVHD 患者在较低 PHA 浓度(1-2.5μg/ml)下 48 小时细胞增殖增强。长时间暴露于 PHA 会导致 aGVHD 患者的增殖减少,而健康人在最佳 PHA 浓度为 5.0-7.5μg/ml 时,增殖在 72 小时内继续增加。CFSE 检测证实了这些发现,在 PHA 浓度较高时,健康人的增殖率较高,而在 PHA 浓度较低时,aGVHD 患者的增殖率较低。IL-2补充剂(50 IU/ml)能显著提高T细胞的增殖和存活率,最佳浓度能在较长的培养期内支持T细胞的稳健增殖:我们的研究确定了体外 T 细胞研究中 PHA 和 IL-2 的最佳浓度,7.5μg/ml PHA 和 50IU/ml IL-2 可使健康人的 T 细胞稳健增殖。相比之下,AGVHD 患者的 T 细胞在较低 PHA 浓度(1.0μg/ml)和相似的 IL-2 要求下增殖更好。这些结果突出表明,需要根据患者的情况定制实验条件,以有效研究T细胞的行为,并改进治疗策略,解决aGVHD和其他疾病中T细胞失调的问题。
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A Comparative assessment of T-Cell response of Healthy donors and Acute Graft-versus-Host-Disease Patients: Customizing immune monitoring platform
Background: T-cell activation and proliferation are critical for understanding immune responses in both healthy and pathological conditions such as acute graft-versus-host disease (aGVHD). Phytohemagglutinin (PHA) and interleukin-2 (IL-2) are commonly used in in vitro assays to study T-cell dynamics. Our study aimed to determine the optimal concentrations of PHA and IL-2 for promoting T-cell proliferation and survival and to evaluate how these conditions impact T-cell responses in healthy individuals versus aGVHD patients. Methods: Peripheral blood samples were collected from age- and sex-matched healthy individuals (n=10) and aGVHD patients (n=10). CD3+ T-cell were isolated and stimulated with varying concentrations of PHA (1-10μg/ml) and IL-2 (50-500 IU/ml). Cell proliferation was assessed using MTS and CFSE assays, while apoptosis was evaluated with Annexin V/7-AAD staining. Results: We observed enhanced proliferation of healthy individuals at higher PHA concentrations (5-10μg/ml), whereas aGVHD patients exhibited heightened proliferation at lower PHA concentrations (1-2.5μg/ml) at 48 hours. Prolonged exposure to PHA led to decreased proliferation in aGVHD patients, while healthy individuals continued to show increased proliferation at 72 hours with optimal PHA concentrations of 5.0-7.5μg/ml. The CFSE assay confirmed these findings, showing a higher proliferation rate in healthy individuals at elevated PHA concentrations and in aGVHD patients at lower concentrations. IL-2 supplementation (50 IU/ml) significantly enhanced T-cell proliferation and survival, with the optimal concentration supporting robust proliferation over extended culture periods. Conclusion: Our study identifies optimal PHA and IL-2 concentrations for in vitro T-cell studies, with 7.5μg/ml of PHA and 50IU/ml of IL-2 providing robust T-cell proliferation in healthy individuals. In contrast, aGVHD patients' T-cells showed better proliferation at lower PHA concentrations (1.0μg/ml) and similar IL-2 requirements. These results underscore the need for tailored experimental conditions based on patient profiles to effectively study T-cell behavior and improve therapeutic strategies for T-cell dysregulation in aGVHD and other conditions.
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