Marietheres Evers, Thorsten Stühmer, Martin Schreder, Torsten Steinbrunn, Martina Rudelius, Franziska Jundt, Regina Ebert, Tanja Nicole Hartmann, Ralf Christian Bargou, Andreas Rosenwald, Ellen Leich
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Furthermore, <i>ADAM8</i>/<i>15</i> expression increased with MM progression and in relapsed/refractory MM compared to untreated patient samples. RNA sequencing and gene set enrichment analysis comparing <i>ADAM8</i>/<i>9</i>/<i>15</i><sup>high/low</sup> patient samples revealed an upregulation of proliferation markers and proliferation-associated gene sets in <i>ADAM8</i>/<i>9</i>/<i>15</i><sup>high</sup> patient samples. High <i>ADAM8</i>/<i>9</i>/<i>15</i> expression correlated with high Ki67 and high <i>ADAM8</i>/<i>15</i> expression with high MYC protein expression in immunohistochemical stainings of patient tissue. Conversely, siRNA-mediated knockdown of <i>ADAM8</i>/<i>9</i>/<i>15</i> in HMCL downregulated proliferation-related gene sets. Western blotting revealed that <i>ADAM8</i> knockdown regulated IGF1R/AKT signaling and <i>ADAM9</i> knockdown decreased mTOR activation. 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引用次数: 0
摘要
多发性骨髓瘤(MM)是一种血液系统恶性肿瘤,患者的复发和耐药性极大地影响了其治愈率。我们以前曾提出,ADAM8、ADAM9 和 ADAM15(分解蛋白和金属蛋白酶 8/9/15)的高表达是 MM 的不良预后标志物。本研究利用两个患者队列和七个人类 MM 细胞系(HMCL),重点研究了 ADAM8/9/15 在 MM 中的作用。ADAM8/9/15的高表达与高危细胞遗传学异常和髓外疾病有关。此外,与未经治疗的患者样本相比,ADAM8/15的表达随MM的进展而增加,在复发/难治性MM中也是如此。通过对ADAM8/9/15高/低患者样本进行RNA测序和基因组富集分析,发现在ADAM8/9/15高的患者样本中,增殖标志物和增殖相关基因组上调。在患者组织的免疫组化染色中,ADAM8/9/15高表达与Ki67高表达相关,ADAM8/15高表达与MYC蛋白高表达相关。相反,siRNA介导的HMCL中ADAM8/9/15的敲除会降低与增殖相关的基因集。Western blotting显示,ADAM8敲除可调节IGF1R/AKT信号转导,而ADAM9敲除可减少mTOR激活。最后,ADAM8/9/15的高表达水平被证实是独立于Ki67/MYC表达和/或高危异常的预后标志物。总之,这些研究结果表明,ADAM8/9/15在MM进展和增殖信号转导中发挥作用。
Association of ADAM family members with proliferation signaling and disease progression in multiple myeloma
Multiple myeloma (MM) is a hematological malignancy whose curability is greatly challenged by recurrent patient relapses and therapy resistance. We have previously proposed the high expression of ADAM8, ADAM9 and ADAM15 (A Disintegrin And Metalloproteinase 8/9/15) as adverse prognostic markers in MM. This study focused on the so far scarcely researched role of ADAM8/9/15 in MM using two patient cohorts and seven human MM cell lines (HMCL). High ADAM8/9/15 expression was associated with high-risk cytogenetic abnormalities and extramedullary disease. Furthermore, ADAM8/15 expression increased with MM progression and in relapsed/refractory MM compared to untreated patient samples. RNA sequencing and gene set enrichment analysis comparing ADAM8/9/15high/low patient samples revealed an upregulation of proliferation markers and proliferation-associated gene sets in ADAM8/9/15high patient samples. High ADAM8/9/15 expression correlated with high Ki67 and high ADAM8/15 expression with high MYC protein expression in immunohistochemical stainings of patient tissue. Conversely, siRNA-mediated knockdown of ADAM8/9/15 in HMCL downregulated proliferation-related gene sets. Western blotting revealed that ADAM8 knockdown regulated IGF1R/AKT signaling and ADAM9 knockdown decreased mTOR activation. Lastly, high ADAM8/9/15 expression levels were verified as prognostic markers independent of Ki67/MYC expression and/or high-risk abnormalities. Overall, these findings suggest that ADAM8/9/15 play a role in MM progression and proliferation signaling.
期刊介绍:
Blood Cancer Journal is dedicated to publishing high-quality articles related to hematologic malignancies and related disorders. The journal welcomes submissions of original research, reviews, guidelines, and letters that are deemed to have a significant impact in the field. While the journal covers a wide range of topics, it particularly focuses on areas such as:
Preclinical studies of new compounds, especially those that provide mechanistic insights
Clinical trials and observations
Reviews related to new drugs and current management of hematologic malignancies
Novel observations related to new mutations, molecular pathways, and tumor genomics
Blood Cancer Journal offers a forum for expedited publication of novel observations regarding new mutations or altered pathways.