Schick Volker, Majores Michael, Engels Gudrun, Spitoni Sylvia, Koch Arend, Elger Christian E, Simon Matthias, Knobbe Christiane, Blümcke Ingmar, Becker Albert J
Department of Neuropathology, University of Bonn Medical Center, Sigmund-Freud-Str. 25, 53105, Bonn, Germany.
Acta Neuropathol. 2006 Dec;112(6):715-25. doi: 10.1007/s00401-006-0128-y. Epub 2006 Sep 30.
Focal cortical dysplasias (FCD) with Taylor-type balloon cells (FCD(IIb)) are frequently observed in biopsy specimens of patients with pharmacoresistant focal epilepsies. The molecular pathogenesis of FCD(IIb), which lack familial inheritance, is only poorly understood. Due to their highly differentiated, malformative nature and glioneuronal phenotype, FCD(IIb) share neuropathological characteristics with lesions observed in familial disorders such as cortical tubers present in patients with autosomal dominant tuberous sclerosis complex (TSC), related to mutations in the TSC1 or TSC2 genes, and dysplastic gangliocytomas of the cerebellum found in Cowden disease. Current data have indicated distinct allelic variants of TSC1 to accumulate in FCD(IIb). TSC1 represents a tumor suppressor operating in the phosphatidylinositol 3-kinase (PI3K)/insulin pathway. The tumor-suppressor gene PTEN is mutated in Cowden disease. Like PTEN, also carboxyl-terminal modulator protein (CTMP) modulates PI3K-pathway signaling, both via inhibition of Akt/PKB, a kinase inactivating the TSC1/TSC2 complex. Here, we have analyzed alterations of Akt, PTEN and CTMP relevant for insulin signaling upstream of TSC1/TSC2 in FCD(IIb). Immunohistochemistry with antibodies against phosphorylated Akt (phospho-Akt; Ser 473) in FCD(IIb) (n=23) showed strong phospho-Akt expression in dysplastic FCD(IIb) components. We have further studied sequence alterations of PTEN (n=34 FCD(IIb)) and CTMP (n=20 FCD(IIb)) by laser microdissection/single-strand conformation polymorphism analysis. We observed a somatic mutation in an FCD(IIb), i.e., amino-acid exchange at nucleotide position 834 (PTEN cDNA, GenBank AH007803.1) in exon 8 with replacement of phenylalanine by leucine (F278L). We also found several silent polymorphisms of PTEN in exon 2 and exon 8 as well as silent and coding polymorphisms but no mutations in CTMP. No loss of heterozygosity in FCD(IIb) (n=6) at 10q23 was observed. To our knowledge, we here report on the first somatic mutation of a tumor-suppressor gene, i.e., PTEN, in FCD(IIb). However, our study also demonstrates that mutational alterations of PTEN and CTMP do not play major pathogenetic roles for activation of Akt in FCD(IIb). Future studies need to determine the origin of insulin pathway activation upstream of TSC1/TSC2 in FCD(IIb).
在药物难治性局灶性癫痫患者的活检标本中,常可观察到伴有泰勒型气球样细胞的局灶性皮质发育不良(FCD(IIb))。FCD(IIb)缺乏家族遗传性,其分子发病机制目前仍知之甚少。由于其高度分化、畸形的性质以及神经胶质神经元表型,FCD(IIb)与家族性疾病中观察到的病变具有神经病理学特征,如常染色体显性遗传性结节性硬化症(TSC)患者出现的皮质结节,这与TSC1或TSC2基因的突变有关,以及考登病中发现的小脑发育异常性神经节细胞瘤。目前的数据表明,TSC1的不同等位基因变体在FCD(IIb)中积累。TSC1是一种在磷脂酰肌醇3激酶(PI3K)/胰岛素途径中起作用的肿瘤抑制因子。肿瘤抑制基因PTEN在考登病中发生突变。与PTEN一样,羧基末端调节蛋白(CTMP)也通过抑制Akt/PKB(一种使TSC1/TSC2复合物失活的激酶)来调节PI3K途径信号传导。在此,我们分析了FCD(IIb)中TSC1/TSC2上游与胰岛素信号相关的Akt、PTEN和CTMP的改变。用抗磷酸化Akt(磷酸化Akt;Ser 473)抗体对FCD(IIb)(n = 23)进行免疫组织化学分析显示,在发育异常的FCD(IIb)成分中磷酸化Akt表达强烈。我们通过激光显微切割/单链构象多态性分析进一步研究了PTEN(n = 34例FCD(IIb))和CTMP(n = 20例FCD(IIb))的序列改变。我们在一个FCD(IIb)中观察到一个体细胞突变,即外显子8中核苷酸位置834(PTEN cDNA,GenBank AH007803.1)处的氨基酸交换,苯丙氨酸被亮氨酸取代(F278L)。我们还在PTEN的外显子2和外显子8中发现了几个沉默多态性以及沉默和编码多态性,但CTMP中未发现突变。在FCD(IIb)(n = 6)的10q23处未观察到杂合性缺失。据我们所知,我们在此首次报道了FCD(IIb)中肿瘤抑制基因PTEN的体细胞突变。然而,我们的研究也表明,PTEN和CTMP的突变改变在FCD(IIb)中Akt的激活中不发挥主要致病作用。未来的研究需要确定FCD(IIb)中TSC1/TSC2上游胰岛素途径激活的起源。
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