初发转移性去势敏感性前列腺癌与既往局部治疗后转移性复发之间的肿瘤基因表达谱差异
Differences in Tumor Gene Expression Profiles Between De Novo Metastatic Castration-sensitive Prostate Cancer and Metastatic Relapse After Prior Localized Therapy.
作者信息
Mathew Thomas Vinay, Sayegh Nicolas, Chigarira Beverly, Gebrael Georges, Tripathi Nishita, Nussenzveig Roberto, Jo Yeonjung, Dal Emre, Galarza Fortuna Gliceida, Li Haoran, Sahu Kamal Kant, Srivastava Ayana, Maughan Benjamin L, Agarwal Neeraj, Swami Umang
机构信息
Division of Medical Oncology, Department of Internal Medicine, Huntsman Cancer Institute, University of Utah, Salt Lake City, UT, USA.
Division of Medical Oncology, Department of Internal Medicine, Huntsman Cancer Institute, University of Utah, Salt Lake City, UT, USA; Department of Internal Medicine, University of Texas Southwestern Medical Center, Dallas, TX, USA.
出版信息
Eur Urol Oncol. 2024 Dec;7(6):1462-1468. doi: 10.1016/j.euo.2024.04.013. Epub 2024 May 11.
BACKGROUND AND OBJECTIVE
It has been reported that patients with de novo metastatic castration-sensitive prostate cancer (dn-mCSPC) have worse prognosis and outcomes than those whose cancer relapses after prior local therapy (PLT-mCSPC). Our aim was to interrogate and validate underlying differences in tumor gene expression profiles between dn-mCSPC and PLT-mCSPC.
METHODS
The inclusion criteria were histologically confirmed prostate adenocarcinoma and the availability of RNA sequencing data for treatment-naïve primary prostate tissue. RNA sequencing was performed by Tempus or Caris Life Sciences, both of which have Clinical Laboratory Improvement Amendments certification. The Tempus cohort was used for interrogation, while the Caris cohort was used for validation. Differential gene expression analysis between the cohorts was conducted using the DEseq2 pipeline. The resulting gene expression profiles were further analyzed using Gene Set Enrichment software to identify pathways with enrichment in each cohort.
KEY FINDINGS AND LIMITATIONS
Overall, 128 patients were eligible, of whom 78 were in the Tempus cohort (dn-mCSPC 37, PLT-mCSPC 41) and 50 were in the Caris cohort (dn-mCSPC 30, PLT-mCSPC 20). Tumor tissues from patients with dn-mCSPC had higher expression of genes associated with inflammation pathways, while tissues from patients with PLT-mCSPC had higher expression of genes involved in oxidative phosphorylation, fatty acid metabolism, and androgen response pathways.
CONCLUSIONS AND CLINICAL IMPLICATIONS
Our study revealed upregulation of distinct genomic pathways in dn-mCSPC in comparison to PLT-mCSPC. These hypothesis-generating data could guide personalized therapy for men with prostate cancer and explain different survival outcomes for dn-mCSPC and PLT-mCSPC.
PATIENT SUMMARY
We measured gene expression levels in tumors from patients with metastatic castration-sensitive prostate cancer. In patients with metastatic disease at first diagnosis, inflammatory pathways were upregulated. In patients whose metastasis occurred on relapse after treatment, androgen response pathways were upregulated. These findings could help in personalizing therapy for prostate cancer and explaining differences in survival.
背景与目的
据报道,初发转移性去势敏感性前列腺癌(dn-mCSPC)患者的预后和结局比那些在先前局部治疗(PLT-mCSPC)后癌症复发的患者更差。我们的目的是探究并验证dn-mCSPC与PLT-mCSPC之间肿瘤基因表达谱的潜在差异。
方法
纳入标准为组织学确诊的前列腺腺癌以及未经治疗的原发性前列腺组织的RNA测序数据。RNA测序由Tempus或Caris生命科学公司进行,这两家公司均具有临床实验室改进修正案认证。Tempus队列用于探究,而Caris队列用于验证。使用DEseq2管道对队列之间的差异基因表达进行分析。使用基因集富集软件对所得的基因表达谱进行进一步分析,以识别每个队列中富集的通路。
主要发现与局限性
总体而言,128例患者符合条件,其中78例在Tempus队列中(dn-mCSPC 37例,PLT-mCSPC 41例),50例在Caris队列中(dn-mCSPC 30例,PLT-mCSPC 20例)。dn-mCSPC患者的肿瘤组织中与炎症通路相关的基因表达较高,而PLT-mCSPC患者的组织中参与氧化磷酸化、脂肪酸代谢和雄激素反应通路的基因表达较高。
结论与临床意义
我们的研究表明,与PLT-mCSPC相比,dn-mCSPC中不同基因组通路上调。这些产生假设的数据可为前列腺癌男性患者的个性化治疗提供指导,并解释dn-mCSPC和PLT-mCSPC不同的生存结局。
患者总结
我们测量了转移性去势敏感性前列腺癌患者肿瘤中的基因表达水平。在初诊时患有转移性疾病患者中,炎症通路上调。在治疗后复发时发生转移的患者中,雄激素反应通路上调。这些发现有助于前列腺癌的个性化治疗并解释生存差异。
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