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首页> 外文期刊>Medicine. >Clinical, histopathologic, subtype, and immunohistochemical analysis of jaw phosphaturic mesenchymal tumors
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Clinical, histopathologic, subtype, and immunohistochemical analysis of jaw phosphaturic mesenchymal tumors

机译:颌骨间充质肿瘤的临床,组织病理学,亚型和免疫组化分析

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Jaw phosphaturic mesenchymal tumors (PMTs) are a rare neoplasm with uncertain histogenesis. This study aimed to clarify the clinical and pathological features of jaw PMTs. We reviewed the clinical records of 39 patients diagnosed with PMTs in the jaws, and investigated clinical and morphologic characteristics, histologic subtypes, and immunophenotypes of all cases. Microscopic analyses revealed 2 major histologic tumor subtypes: “ phosphaturic mesenchymal tumors of mixed epithelial and connective tissue” (PMTMECT), and “ phosphaturic mesenchymal tumors of mixed connective tissue” (PMTMCT). PMTMECTs and PMTMCTs accounted for 29 and 10 cases of PMTs, respectively. Most PMTMECT diagnoses were made predominantly in males aged 45 years, and the incidence was similar in both the mandible and maxilla. In contrast, patients with PMTMCTs are predominantly females aged ≥45 years, and all tumors were in the mandible. Histologically, PMTMECT had lower cellularity and a more elongated and spindled mesenchymal component with less elaborate intrinsic microvasculature than PMTMCT. Immunohistochemically, the epithelia of all PMTMECTs was immunoreactive for AE1/AE3. Other immunohistochemical staining of PMTMECTs revealed positive expression of vimentin, SATB2, ERG, CD99, Bcl-2, CD56, S-100, D2-40, CD68, SMA, and CD34 in either one or both components. Immunohistochemical staining of PMTMCTs was diffusely positive for vimentin and a varied ratio of positivity for SATB2, ERG, CD99, Bcl-2, CD56, S-100, D2-40, CD68, SMA, and CD34, but negative for AE1/AE3. Most patients were cured by complete resection, except 2 patients who had repeated recurrences, one of which also had multiple metastasis. Jaw PMT can be divided into 2 major histological subtypes. PMTMECTs are more common than are PMTMCTs, and can transform into malignant PMTMCTs during the progression. PMTMECTs were more commonly observed in males and the incidence was similar in both the maxilla and mandible. PMTMCTs were almost always observed in the mandible of females. Compared with PMTMCTs, PMTMECTs have an admixture of epithelial components with less prominent vasculature and lower cellularity. There were no statistically significant differences in the expression of immunohistochemical markers except AE1/AE3 between PMTMECTs and PMTMCTs. However, immunohistochemical markers have great significance for differentiating other mesenchymal tumors.
机译:下颚磷酸性间充质肿瘤(PMTS)是一种罕见的肿瘤,具有不确定的组织发生。本研究旨在阐明JAW PMTS的临床和病理特征。我们审查了患有钳口中PMTS的39名患者的临床记录,并研究了所有病例的临床和形态学特征,组织学亚型和免疫咽部。微观分析显示出2个主要组织学肿瘤亚型:“混合上皮和结缔组织的磷酸性间充质肿瘤(PMTMECT)和”混合结缔组织的磷酸性间充质肿瘤“(PMTMCT)。 PMTMects和PMTMCT分别占PMT的29例和10例。大多数PMTMECT诊断主要是在<45岁的男性中,发病率在下颌和上颌中相似。相比之下,患有PMTMCT的患者主要是≥45岁的女性,所有肿瘤都在下颌骨。组织学上,PMTMECT具有较低的细胞性,并且具有比PMTMCT更少细化的内在微血管结构的细胞间和更细长的和纺锤形的间充质成分。免疫组织化学,所有PMT22的上皮细胞对AE1 / AE3的免疫反应。 PMT2的其他免疫组织化学染色揭示了一种或两种组分中的Vimentin,SATB2,ERG,CD99,BCL-2,CD56,S-100,D2-40,CD68,SMA和CD34的正表达。 PMTMCTS的免疫组织化学染色是Vimentin的阳性阳性和SATB2,ERG,CD99,BCL-2,CD56,S-100,D2-40,CD68,SMA和CD34的变化比例,但是AE1 / AE3的阴性。大多数患者通过完全切除治愈,除了2名重复复发的患者外,其中还具有多种转移。钳口PMT可分为2个主要组织学亚型。 PMTMects比PMTMCTS更常见,并且可以在进展期间转换为恶性PMTMCT。在麦利中更常见的PMTMECTS在颌骨和下颌骨中的发病率相似。在女性的下颌骨上几乎总是观察到的PMTMCT。与PMTMCT相比,PMTMECTS对上皮组分的混合物具有较小突出的脉管系统和较低的细胞性。除了PMT2和PMTMCTS之间的AE1 / AE3之外的免疫组织化学标记表达没有统计学上显着的差异。然而,免疫组织化学标志物对区分其他间充质肿瘤具有重要意义。

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