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临床前列腺癌骨转移中的骨细胞活性及其与肿瘤细胞雄激素受体活性的反向关系。

Bone Cell Activity in Clinical Prostate Cancer Bone Metastasis and Its Inverse Relation to Tumor Cell Androgen Receptor Activity.

机构信息

Department of Medical Biosciences, Pathology, Umea University, 901 85 Umea, Sweden.

Department of Surgical and Perioperative Sciences, Orthopaedics, Umea University, 901 85 Umea, Sweden.

出版信息

Int J Mol Sci. 2018 Apr 18;19(4):1223. doi: 10.3390/ijms19041223.

Abstract

Advanced prostate cancer frequently metastasizes to bone and induces a mixed osteoblastic/osteolytic bone response. Standard treatment for metastatic prostate cancer is androgen-deprivation therapy (ADT) that also affects bone biology. Treatment options for patients relapsing after ADT are limited, particularly in cases where castration-resistance does not depend on androgen receptor (AR) activity. Patients with non-AR driven metastases may, however, benefit from therapies targeting the tumor microenvironment. Therefore, the current study specifically investigated bone cell activity in clinical bone metastases in relation to tumor cell AR activity, in order to gain novel insight into biological heterogeneities of possible importance for patient stratification into bone-targeting therapies. Metastasis tissue obtained from treatment-naïve ( = 11) and castration-resistant ( = 28) patients was characterized using whole-genome expression analysis followed by multivariate modeling, functional enrichment analysis, and histological evaluation. Bone cell activity was analyzed by measuring expression levels of predefined marker genes representing osteoclasts (, , ), osteoblasts (, , ) and osteocytes (). Principal component analysis indicated a positive correlation between osteoblast and osteoclast activity and a high variability in bone cell activity between different metastases. Immunohistochemistry verified a positive correlation between runt-related transcription factor 2 (RUNX2) positive osteoblasts and tartrate-resistant acid phosphatase (TRAP, encoded by ) positive osteoclasts lining the metastatic bone surface. No difference in bone cell activity was seen between treatment-naïve and castration-resistant patients. Importantly, bone cell activity was inversely correlated to tumor cell AR activity (measured as , , , , , , , and expression) and to patient serum prostate-specific antigen (PSA) levels. Functional enrichment analysis indicated high bone morphogenetic protein (BMP) signaling in metastases with high bone cell activity and low tumor cell AR activity. This was confirmed by BMP4 immunoreactivity in tumor cells of metastases with ongoing bone formation, as determined by histological evaluation of van Gieson-stained sections. In conclusion, the inverse relation observed between bone cell activity and tumor cell AR activity in prostate cancer bone metastasis may be of importance for patient response to AR and/or bone targeting therapies, but needs to be evaluated in clinical settings in relation to serum markers for bone remodeling, radiography and patient response to therapy. The importance of BMP signaling in the development of sclerotic metastasis lesions deserves further exploration.

摘要

晚期前列腺癌常转移至骨骼并引起混合成骨/溶骨的骨反应。转移性前列腺癌的标准治疗方法是去势治疗(ADT),该治疗方法也会影响骨骼生物学。ADT 后复发的患者的治疗选择有限,特别是在去势抵抗不依赖雄激素受体(AR)活性的情况下。然而,非 AR 驱动的转移患者可能受益于针对肿瘤微环境的治疗。因此,目前的研究专门调查了临床骨转移中与肿瘤细胞 AR 活性相关的骨细胞活性,以期深入了解对患者分层进行骨靶向治疗可能具有重要意义的生物学异质性。使用全基因组表达分析,然后进行多元建模、功能富集分析和组织学评估,对来自治疗初治(= 11)和去势抵抗(= 28)患者的转移组织进行了表征。通过测量代表破骨细胞(、、)、成骨细胞(、、)和成骨细胞()的预定义标记基因的表达水平来分析骨细胞活性。主成分分析表明成骨细胞和破骨细胞活性之间存在正相关,并且不同转移之间的骨细胞活性变化很大。免疫组织化学证实了转移性骨表面排列的 runt 相关转录因子 2(RUNX2)阳性成骨细胞与抗酒石酸酸性磷酸酶(TRAP,由编码)阳性破骨细胞之间存在正相关。在治疗初治和去势抵抗患者之间,骨细胞活性没有差异。重要的是,骨细胞活性与肿瘤细胞 AR 活性(作为、、、、、、和表达测量)和患者血清前列腺特异性抗原(PSA)水平呈负相关。功能富集分析表明,在成骨细胞活性高和肿瘤细胞 AR 活性低的转移中存在高骨形态发生蛋白(BMP)信号。通过组织学评估 van Gieson 染色切片中正在进行骨形成的转移中肿瘤细胞的 BMP4 免疫反应证实了这一点。总之,在前列腺癌骨转移中观察到的骨细胞活性与肿瘤细胞 AR 活性之间的反比关系可能对 AR 和/或骨靶向治疗的患者反应很重要,但需要结合血清骨重塑标志物、射线照相和患者对治疗的反应在临床环境中进行评估。BMP 信号在硬化性转移病变发展中的重要性值得进一步探索。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c833/5979457/cb332fecf671/ijms-19-01223-g001.jpg

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