Unleashing the Impact of Exosomes Derived from Human Placental Mesenchymal Stem Cells (hPMSCs) on U-266 Myeloma Cell Line

Ayda Baghery Saghchy Khorasani, Mina Soufizomorrod, Davood Bashash
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Abstract

Multiple myeloma (MM) is a malignancy of plasma cells, terminally differentiated B cells, with complications like hypercalcemia, renal failure, anemia, and bone disease, which are also known as CRAB criteria. MM develops from monoclonal gammopathy of unknown significance (MGUS), a pre-malignant plasma cell dyscrasia. Over some time, MGUS has the potential to progress into smoldering multiple myeloma (SMM), which can evolve into MM. MM rarely progresses into plasma cell leukemia (PCL), a condition in which malignant plasma cells no longer stay in the bone marrow niche and circulate in the peripheral blood. In MM, various soluble factors play important roles, and interleukin-6 has different vital roles.  Interleukin-6, an inflammatory cytokine, has significant roles in the growth, survival, angiogenesis, metastasis, and apoptosis resistance in MM. Interleukin-6 is produced and secreted by both autocrine from myeloma cells and paracrine from bone marrow stromal cells. To tackle MM, various therapeutic approaches were applied over many years, and according to the results, most patients with MM can respond well to first-line treatment. However, the majority of patients may relapse as conventional treatment may not be curative. So, there is an urgent need for novel cell-based and cell-free therapeutic strategies, such as mesenchymal stem cell-based therapies and their products to offer new therapeutic strategies for MM. Materials and Methods: In the present study, we investigated the impacts of exosomes derived from human placental mesenchymal stem cells (hPMSCs) on apoptosis and interleukin-6 expression in a myeloma cell line, U-266, for the first time. hPMSCs were isolated from the human placenta and cultured in a DMEM medium. After characterizing the cells and acknowledging their identity, they underwent several passages and their supernatant was collected to harvest exosomes. The exosomes were isolated by ultracentrifugation and characterized by DLS and TEM, and their concentration was measured by BCA protein assay. U266 cells were treated with different concentrations of exosomes and then MTT and annexin/propidium iodide flow cytometry tests were performed to evaluate cell viability. Afterward, a real-time PCR test was performed to evaluate interleukin-6 gene expression. Results: According to our findings, treatment of U-266 cells with hPMSCS-derived exosomes led to the preservation of myeloma cells without changes in their cell cycle. Surprisingly, treatments did not hinder the expression of interleukin-6 in the myeloma cells. Conclusion: In MM patients, interleukin-6 plays different roles, and it is a desirable target to design new therapeutic strategies. To evaluate the effects of new therapeutic strategies, we designed and performed our study to estimate the effects of cell-free therapeutic strategy.  In the present study, the impacts of hPMSCS-derived exosomes on the viability of MM cells and interleukin-6 gene expression were evaluated. The results showed that hPMSCS-derived exosomes resulted in the perseverance of myeloma cells without changes in the cell cycle.  Furthermore, the interleukin-6 gene expression level showed no significant change.
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释放人胎盘间充质干细胞(hPMSCs)外泌体对 U-266 骨髓瘤细胞系的影响
多发性骨髓瘤(MM)是一种浆细胞(终末分化的 B 细胞)恶性肿瘤,具有高钙血症、肾功能衰竭、贫血和骨病等并发症,这也被称为 CRAB 标准。MM 是由意义不明的单克隆丙种球蛋白病(MGUS)发展而来的,MGUS 是一种恶性前浆细胞异常。经过一段时间后,MGUS 有可能发展为烟雾型多发性骨髓瘤(SMM),SMM 又可能发展为 MM。MM很少发展为浆细胞白血病(PCL),在这种情况下,恶性浆细胞不再停留在骨髓龛中,而是在外周血中循环。在 MM 中,各种可溶性因子发挥着重要作用,其中白细胞介素-6 发挥着不同的重要作用。 白细胞介素-6 是一种炎性细胞因子,在 MM 的生长、存活、血管生成、转移和抗凋亡中起着重要作用。白细胞介素-6通过骨髓瘤细胞的自分泌和骨髓基质细胞的旁分泌产生和分泌。针对骨髓瘤,多年来人们采用了多种治疗方法,结果表明,大多数骨髓瘤患者对一线治疗反应良好。不過,由於傳統治療未必能根治,大部分病人可能會復發。因此,迫切需要新型的细胞和无细胞治疗策略,如间充质干细胞疗法及其产品,为 MM 提供新的治疗策略。材料与方法:在本研究中,我们首次研究了从人胎盘间充质干细胞(hPMSCs)中提取的外泌体对骨髓瘤细胞系U-266的细胞凋亡和白细胞介素-6表达的影响。在确定细胞特征并确认其身份后,对其进行了多次传代,并收集其上清液以收获外泌体。通过超速离心法分离外泌体,用 DLS 和 TEM 对其进行表征,并用 BCA 蛋白检测法测定其浓度。用不同浓度的外泌体处理 U266 细胞,然后用 MTT 和附件素/碘化丙啶流式细胞术检测细胞活力。之后,进行实时 PCR 检测以评估白细胞介素-6 基因的表达。结果根据我们的研究结果,用源自 hPMSCS 的外泌体处理 U-266 细胞可保存骨髓瘤细胞,且细胞周期不会发生变化。令人惊讶的是,治疗并未阻碍骨髓瘤细胞中白细胞介素-6的表达。结论是在 MM 患者体内,白细胞介素-6 发挥着不同的作用,是设计新治疗策略的理想靶点。为了评估新治疗策略的效果,我们设计并开展了无细胞治疗策略的效果评估研究。 本研究评估了源自 hPMSCS 的外泌体对 MM 细胞活力和白细胞介素-6 基因表达的影响。结果表明,hPMSCS衍生的外泌体可使骨髓瘤细胞存活下来,而细胞周期不会发生变化。 此外,白细胞介素-6基因表达水平也没有发生显著变化。
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