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Cytoplasmic ADP-ribosylation levels correlate with markers of patient outcome in distinct human cancers

机译:细胞质ADP-核糖基化水平与不同人类癌症中患者结果的标志物相关

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ADP-ribosylation (ADPR) is a posttranslational modification whose importance in oncology keeps increasing due to frequent use of PARP inhibitors (PARPi) to treat different tumor types. Due to the lack of suitable tools to analyze cellular ADPR levels, ADPR's significance for cancer progression and patient outcome is unclear. In this study, we assessed ADPR levels by immunohistochemistry using a newly developed anti-ADP-ribose (ADPr) antibody, which is able to detect both mono- and poly-ADPR. Tissue microarrays containing brain (n = 103), breast (n = 1108), colon (n = 236), lung (n = 138), ovarian (n = 142), and prostate (n = 328) cancers were used to correlate ADPR staining intensities to clinico-pathological data, including patient overall survival (OS), tumor grade, tumor stage (pT), lymph node status (pN), and the presence of distant metastasis (pM). While nuclear ADPR was detected only in a minority of the samples, cytoplasmic ADPR (cyADPR) staining was observed in most tumor types. Strong cyADPR intensities were significantly associated with better overall survival in invasive ductal breast cancer (p < 0.0001), invasive lobular breast cancer (p < 0.005), and high grade serous ovarian cancer patients (p < 0.01). Furthermore, stronger cytoplasmic ADPR levels significantly correlated with early tumor stage in colorectal and in invasive ductal breast adenocarcinoma (p < 0.0001 and p < 0.01, respectively) and with the absence of regional lymph node metastasis in colorectal adenocarcinoma (p < 0.05). No correlation to cyADPR was found for prostate and lung cancer or brain tumors. In conclusion, our new anti-ADP-ribose antibody revealed heterogeneous ADPR staining patterns with predominant cytoplasmic ADPR staining in most tumor types. Different cyADPR staining patterns could help to better understand variable response rates to PARP inhibitors in the future.
机译:ADP-核糖基化(ADPR)是一种后期改性,其在肿瘤学中的重要性由于频繁使用PARP抑制剂(PARPI)来治疗不同的肿瘤类型。由于缺乏合适的分析细胞ADPR水平的工具,ADPR对癌症进展和患者结果的重要性尚不清楚。在这项研究中,我们通过新开发的抗ADP-核糖(ADPR)抗体来评估免疫组织化学的ADPR水平,该抗体能够检测单可以和Poly-ADPR。含有脑(n = 103),乳腺(n = 1108),结肠(n = 236),肺(n = 138),卵巢(n = 142)和前列腺(n = 328)癌症的组织微阵列用来相关ADPR染色到临床病理数据的强度,包括患者总存活(OS),肿瘤级,肿瘤阶段(PT),淋巴结状态(PN)以及远处转移(PM)的存在。虽然仅在少数群体中检测到核ADPR,但在大多数肿瘤类型中观察到细胞质ADPR(CYADPR)染色。强烈的睾丸强度与侵袭性导管乳腺癌(P <0.0001),侵袭性小叶乳腺癌(P <0.005)和高级浆液癌患者(P <0.01)有显着相关。此外,更强的细胞质ADPR水平与结直肠癌和侵袭性导管乳腺腺癌(P <0.0001和P <0.01分别)显着相关,并且在缺乏结肠直肠腺癌中的区域淋巴结转移(P <0.05)。对前列腺和肺癌或脑肿瘤发现与睾丸或脑肿瘤无关。总之,我们的新抗ADP-核糖抗体揭示了具有大多数肿瘤类型的主要细胞质ADPR染色的异质性ADPR染色模式。不同的Cyadpr染色模式可以帮助将来更好地了解可变响应率对PARP抑制剂。

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