前列腺癌患者慢性前列腺炎症中的血清自身抗体
Serum Autoantibodies in Chronic Prostate Inflammation in Prostate Cancer Patients.
作者信息
Schlick Bettina, Massoner Petra, Lueking Angelika, Charoentong Pornpimol, Blattner Mirjam, Schaefer Georg, Marquart Klaus, Theek Carmen, Amersdorfer Peter, Zielinski Dirk, Kirchner Matthias, Trajanoski Zlatko, Rubin Mark A, Müllner Stefan, Schulz-Knappe Peter, Klocker Helmut
机构信息
Division of Experimental Urology, Dept. of Urology, Medical University of Innsbruck, Innsbruck, Austria.
ONCOTYROL, Center for Personalized Cancer Medicine, Innsbruck, Austria.
出版信息
PLoS One. 2016 Feb 10;11(2):e0147739. doi: 10.1371/journal.pone.0147739. eCollection 2016.
BACKGROUND
Chronic inflammation is frequently observed on histological analysis of malignant and non-malignant prostate specimens. It is a suspected supporting factor for prostate diseases and their progression and a main cause of false positive PSA tests in cancer screening. We hypothesized that inflammation induces autoantibodies, which may be useful biomarkers. We aimed to identify and validate prostate inflammation associated serum autoantibodies in prostate cancer patients and evaluate the expression of corresponding autoantigens.
METHODS
Radical prostatectomy specimens of prostate cancer patients (N = 70) were classified into high and low inflammation groups according to the amount of tissue infiltrating lymphocytes. The corresponding pre-surgery blood serum samples were scrutinized for autoantibodies using a low-density protein array. Selected autoantigens were identified in prostate tissue and their expression pattern analyzed by immunohistochemistry and qPCR. The identified autoantibody profile was cross-checked in an independent sample set (N = 63) using the Luminex-bead protein array technology.
RESULTS
Protein array screening identified 165 autoantibodies differentially abundant in the serum of high compared to low inflammation patients. The expression pattern of three corresponding antigens were established in benign and cancer tissue by immunohistochemistry and qPCR: SPAST (Spastin), STX18 (Syntaxin 18) and SPOP (speckle-type POZ protein). Of these, SPAST was significantly increased in prostate tissue with high inflammation. All three autoantigens were differentially expressed in primary and/or castration resistant prostate tumors when analyzed in an inflammation-independent tissue microarray. Cross-validation of the inflammation autoantibody profile on an independent sample set using a Luminex-bead protein array, retrieved 51 of the significantly discriminating autoantibodies. Three autoantibodies were significantly upregulated in both screens, MUT, RAB11B and CSRP2 (p>0.05), two, SPOP and ZNF671, close to statistical significance (p = 0.051 and 0.076).
CONCLUSIONS
We provide evidence of an inflammation-specific autoantibody profile and confirm the expression of corresponding autoantigens in prostate tissue. This supports evaluation of autoantibodies as non-invasive markers for prostate inflammation.
背景
在恶性和非恶性前列腺标本的组织学分析中经常观察到慢性炎症。它被怀疑是前列腺疾病及其进展的支持因素,也是癌症筛查中PSA检测假阳性的主要原因。我们假设炎症会诱导自身抗体,而自身抗体可能是有用的生物标志物。我们旨在识别和验证前列腺癌患者中与前列腺炎症相关的血清自身抗体,并评估相应自身抗原的表达。
方法
根据组织浸润淋巴细胞的数量,将前列腺癌患者(N = 70)的根治性前列腺切除术标本分为高炎症组和低炎症组。使用低密度蛋白质阵列对相应的术前血清样本进行自身抗体检查。在前列腺组织中鉴定出选定的自身抗原,并通过免疫组织化学和定量PCR分析其表达模式。使用Luminex微珠蛋白阵列技术在独立样本集(N = 63)中对鉴定出的自身抗体谱进行交叉检查。
结果
蛋白质阵列筛选确定了165种自身抗体,与低炎症患者相比,高炎症患者血清中的自身抗体丰度存在差异。通过免疫组织化学和定量PCR在良性和癌组织中确定了三种相应抗原的表达模式:SPAST(痉挛蛋白)、STX18( syntaxin 18)和SPOP(斑点型POZ蛋白)。其中,SPAST在高炎症的前列腺组织中显著增加。在独立于炎症的组织微阵列中分析时,所有三种自身抗原在原发性和/或去势抵抗性前列腺肿瘤中均有差异表达。使用Luminex微珠蛋白阵列在独立样本集上对炎症自身抗体谱进行交叉验证,找回了51种具有显著区分性的自身抗体。三种自身抗体在两次筛选中均显著上调,即MUT、RAB11B和CSRP2(p>0.05),两种自身抗体,即SPOP和ZNF671,接近统计学意义(p = 0.051和0.076)。
结论
我们提供了炎症特异性自身抗体谱的证据,并证实了相应自身抗原在前列腺组织中的表达。这支持将自身抗体评估为前列腺炎症的非侵入性标志物。
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