Retracing RAS signaling by correlating protein expression in different subtypes of neurofibromatosis 1-associated nerve sheath tumors.

IF 0.8 4区 医学 Q4 CLINICAL NEUROLOGY Clinical Neuropathology Pub Date : 2024-07-01 DOI:10.5414/NP301624
Christian Hagel, Louisa K N Nörnberg, Reinhard E Friedrich
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引用次数: 0

Abstract

Aims: Expression patterns of key proteins involved in RAS signaling and connected pathways were determined and correlated to possibly provide information for therapeutic application of RAS inhibitors in neurofibromatosis type 1 (NF1)-associated peripheral nerve sheath tumors (PNST).

Materials and methods: Clinical variables (age, sex), histological parameters (cell density, mitoses), and expression of immunohistochemically evaluated ligand and receptor proteins (neuregulin 1 (NRG1), ErbB2, ErbB3), RAS pathway proteins (mTor, Rho, phosphorylated MEK), transcription factors (Pax7, Sox9), and proliferation marker Ki-67, were correlated in cutaneous (CNF, n = 136), diffuse (DNF, n = 123)/diffuse plexiform (DPNF, n = 113), and plexiform neurofibroma (PNF, n = 126), and in malignant PNST (MPNST, n = 22).

Results: In CNF, NRG1 correlated with Ki-67 and Pax7. Further, mTOR correlated with ErbB3, Sox9, Pax7, and Ki-67. In DNF/DPNF, expression of NRG1 correlated with pMEK and Pax7. mTOR correlated with pMEK, Sox9, and Pax7. Noteworthy, pMEK was weakly expressed in some DNF but not in DPNF. ErbB3 correlated with mTor and Ki-67. Furthermore, Rho correlated with Pax7 and Ki-67. In PNF, ErbB3 expression was associated with Sox9, mTOR, pMEK, and Pax7 as well as mTOR with Sox9 and Pax7, Rho with pMEK and Pax7, and pMEK with Pax7 and Sox9. In MPNST, only few correlations were observed, ErbB2 correlated with Ki-67, and Rho with pMEK.

Conclusion: Signaling networks of the RAS pathway could be retraced by correlation analysis of protein expression in subgroups of NF1 associated benign PNST. In regard to treatment of PNST, MEK inhibitors, which are presently evaluated for PNF, may possibly also be effective to some extent in DNF.

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通过关联神经纤维瘤病 1 相关神经鞘瘤不同亚型中的蛋白质表达,重新追踪 RAS 信号转导。
目的:确定参与RAS信号转导及相关通路的关键蛋白的表达模式,并将其关联起来,以便为RAS抑制剂在神经纤维瘤病1型(NF1)相关周围神经鞘瘤(PNST)中的治疗应用提供信息:临床变量(年龄、性别)、组织学参数(细胞密度、有丝分裂)、免疫组化评估配体和受体蛋白(神经胶质蛋白 1 (NRG1)、ErbB2、ErbB3)、RAS 通路蛋白(mTor、Rho、磷酸化 MEK)的表达、在皮肤型(CNF,n = 136)、弥漫型(DNF,n = 123)/弥漫丛状型(DPNF,n = 113)和丛状型神经纤维瘤(PNF,n = 126)以及恶性 PNST(MPNST,n = 22)中,转录因子(Pax7、Sox9)和增殖标志物 Ki-67 均有相关性。结果在 CNF 中,NRG1 与 Ki-67 和 Pax7 相关。此外,mTOR 与 ErbB3、Sox9、Pax7 和 Ki-67 相关。在 DNF/DPNF 中,NRG1 的表达与 pMEK 和 Pax7 相关,mTOR 与 pMEK、Sox9 和 Pax7 相关。值得注意的是,pMEK在一些DNF中弱表达,但在DPNF中没有表达。ErbB3 与 mTor 和 Ki-67 相关。此外,Rho 与 Pax7 和 Ki-67 相关。在PNF中,ErbB3的表达与Sox9、mTOR、pMEK和Pax7相关,mTOR与Sox9和Pax7相关,Rho与pMEK和Pax7相关,pMEK与Pax7和Sox9相关。 在MPNST中,只观察到很少的相关性,ErbB2与Ki-67相关,Rho与pMEK相关:结论:通过对与 NF1 相关的良性 PNST 亚组中蛋白质表达的相关性分析,可以追溯 RAS 通路的信号网络。在治疗 PNST 方面,目前针对 PNF 进行评估的 MEK 抑制剂也可能在一定程度上对 DNF 有效。
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来源期刊
Clinical Neuropathology
Clinical Neuropathology 医学-病理学
CiteScore
1.60
自引率
0.00%
发文量
70
审稿时长
>12 weeks
期刊介绍: Clinical Neuropathology appears bi-monthly and publishes reviews and editorials, original papers, short communications and reports on recent advances in the entire field of clinical neuropathology. Papers on experimental neuropathologic subjects are accepted if they bear a close relationship to human diseases. Correspondence (letters to the editors) and current information including book announcements will also be published.
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