CD117

CD117
  • 文章类型: Journal Article
    当前的调查旨在研究在发育早期形成的胚胎真皮,并确定真皮的初始间质成分,这些成分可作为真皮组织发育的生物和结构支架。为了研究真皮结构,目前的研究使用形态学和免疫学技术。通过TEM鉴定的TC。他们有一个细胞体和独特的食宿和食宿。它们形成了遍布真皮的3D网络。它们之间建立了同质细胞接触,以及与其他细胞的异型细胞接触。使用TCssCD34、CD117和VEGF的特异性标志物的免疫组织化学技术证实了TC鉴定。TC代表真皮组织中的主要间质成分。他们建立了一个3D网络,封闭其他细胞和结构。TC表达VEGF促进血管生成。TC与发芽内皮细胞建立细胞接触。在细胞与TC连接的位置,确定并观察到细胞骨架细丝形成从内皮细胞突出的假足核。TC具有表达MMP-9、CD68和CD21的蛋白水解特性。蛋白水解活性有助于去除细胞外基质的成分和吞噬降解的残余物以创造空间以促进新的真皮结构的发展。总之,TC组织了未来真皮结构发展的支架,包括纤维成分和皮肤附件。研究皮肤TC将对开发用于治疗不同皮肤病症和疾病的治疗策略的可能性感兴趣。
    The current investigation aims to study the embryonic dermis formed in the early stages of development and identify the initial interstitial components of the dermis that serve as biological and structural scaffolds for the development of the dermal tissue. To investigate the dermal structure, the current study used morphological and immunological techniques. TCs identified by TEM. They had a cell body and unique podomeres and podoms. They formed a 3D network spread throughout the dermis. Homocellular contact established between them, as well as heterocellular contacts with other cells. Immunohistochemical techniques using specific markers for TCss CD34, CD117, and VEGF confirmed TC identification. TCs represent the major interstitial component in the dermal tissue. They established a 3D network, enclosing other cells and structures. Expression of VEGF by TC promotes angiogenesis. TCs establish cellular contact with sprouting endothelial cells. At the site of cell junction with TCs, cytoskeletal filaments identified and observed to form the pseudopodium core that projects from endothelial cells. TCs had proteolytic properties that expressed MMP-9, CD68, and CD21. Proteolytic activity aids in the removal of components of the extracellular matrix and the phagocytosis of degraded remnants to create spaces to facilitate the development of new dermal structures. In conclusion, TCs organized the scaffold for the development of future dermal structures, including fibrous components and skin appendages. Studying dermal TCs would be interested in the possibility of developing therapeutic strategies for treating different skin disorders and diseases.
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  • 文章类型: Journal Article
    c-KIT是唾液腺肿瘤的重要诊断标志物,在大多数腺样囊性癌中表达。组织学上相似的唾液腺肿瘤,c-KIT的免疫组织化学表达可变,这构成了挑战,并使诊断可靠性变得矛盾。PubMed在MEDLINE中进行了电子搜索,谷歌学者,Scopus,行程,科克伦图书馆,和EMBASE至2023年12月31日,无期限限制。包括研究唾液腺肿瘤中CD117或c-KIT的文章以供审查。灵敏度,特异性,得出c-KIT免疫组织化学表达的阳性和阴性预测值,并使用Sierra软件的OpenMeta分析软件进行荟萃分析。使用QUADAS-2工具分析了选定研究中的偏倚风险,并使用RevMan5.4输出结果。审查了43篇文章,分析2285例唾液腺病例。腺样囊性癌的总表达率为84.9%。在上皮上皮癌中发现了相似的表达(79.1%),淋巴上皮癌(75%),肌上皮癌(60.8%),单形性腺瘤(94.1%),多形性腺瘤(74.7%)。敏感性,特异性,c-KIT/CD117对腺样囊性癌合并其他涎腺肿瘤的阳性和阴性预测值为84.99%,69.09%,84.79%,和69.41%,分别。目前的证据表明c-KIT,尽管它很敏感,没有特异性,因此不能作为区分腺样囊性癌与其他唾液腺肿瘤的有用诊断标记。对表现出相当表达的其他唾液腺肿瘤的进一步研究对于验证c-KIT的诊断准确性是必要的。
    c-KIT is an important diagnostic marker in salivary gland tumours and is expressed in most adenoid cystic carcinomas. Histologically similar salivary gland tumours with variable immunohistochemical expression for c-KIT pose a challenge and make diagnostic reliability ambivalent. An electronic search was performed in MEDLINE by PubMed, Google Scholar, Scopus, Trip, Cochrane Library, and EMBASE up to 31 December 2023, without period restriction. The articles that investigated CD117 or c-KIT in salivary gland tumours were included for review. Sensitivity, specificity, and positive and negative predictive values of c-KIT immunohistochemical expressions were derived and subjected to meta-analysis using Open Meta analyst for Sierra software. The risk of bias in selected studies was analysed using the QUADAS-2 tool, and RevMan 5.4 was used to output the result. Forty-three articles were reviewed, and 2285 salivary gland cases were analysed. Adenoid cystic carcinoma had an overall expression of 84.9%. A similar expression was found in epimyoepithelial carcinoma (79.1%), lymphoepithelial carcinoma (75%), myoepithelial carcinoma (60.8%), monomorphic adenoma (94.1%), and pleomorphic adenoma (74.7%). The sensitivity, specificity, and positive and negative predictive values of c-KIT/CD117 for adenoid cystic carcinoma with other salivary gland tumours were 84.99%, 69.09%, 84.79%, and 69.41%, respectively. Current evidence shows that c-KIT, despite its sensitivity, is not specific and therefore cannot be a useful diagnostic marker for distinguishing adenoid cystic carcinoma from other salivary gland tumours. Further research on other salivary gland tumours that exhibit comparable expression is necessary to validate the diagnostic accuracy of c-KIT.
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  • 文章类型: Case Reports
    胃肠道间质瘤(GIST)是由肠壁引起的肿瘤,最常见的是小肠的空肠回肠,但很少来自胃肠外的地方。GIST最常发生在年龄大于40岁的患者中,并且可呈现多种胃肠道症状。我们介绍了一例罕见的胃肠道外间质瘤(EGIST),导致一名34岁的西班牙裔男性腹痛和黑便。患者出现弥漫性腹痛,Melena,和严重的贫血。腹部计算机断层扫描显示小肠附近有一个大肿块。病人被送往手术,那里有肿块,它似乎来自网膜并侵入相邻的小肠,被完全切除,发现是梭形细胞GIST。切除边缘被确定为阴性,患者开始接受酪氨酸激酶抑制剂的维持治疗。患者继续在门诊基础上随访以进行监测。该病例代表罕见的疾病实体EGIST,该疾病在年轻患者的典型人口统计学特征之外出现,先前未发现遗传综合征。在这种情况下,肿块的总体检查也是非典型的,因为肿块植根于网膜并侵入小肠,这表明原发性肿瘤部位是胃肠道外的。该病例表明需要建立包括GIST的鉴别诊断,并且如果在临床过程中早期发现该疾病,则具有成功治疗该疾病的能力。
    Gastrointestinal stromal tumors (GISTs) are neoplasms arising from the bowel wall, most often in the jejunoileum of the small intestine, but rarely from extragastrointestinal locations. GISTs most often occur in patients older than 40 years of age and can present with a multitude of gastrointestinal symptoms. We present a rare case of an extragastrointestinal stromal tumor (EGIST) causing abdominal pain and melena in a 34-year-old Hispanic male. The patient presented with diffuse abdominal pain, melena, and severe anemia. Computed tomography of the abdomen revealed a large mass abutting the small bowel. The patient was taken to surgery where the mass, which appeared to be deriving from the omentum and invading the adjacent small bowel, was completely excised and found to be a spindle cell GIST. Excision margins were determined to be negative, and the patient was started on a tyrosine kinase inhibitor for maintenance therapy. The patient continues to follow up on an outpatient basis for surveillance. This case represents the rare disease entity EGIST presenting outside the typical demographics of the disease in a young patient with no identified previous genetic syndromes. Gross examination of the mass in this case was also atypical given the appearance that the mass was rooted in the omentum and invading the small bowel which would suggest the primary tumor site was extragastrointestinal. This case demonstrates the need to build a differential diagnosis that includes GIST and the ability to successfully treat this disease if it is identified early in the clinical course.
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  • 文章类型: Journal Article
    子宫内膜癌是发展中国家最常见的妇科肿瘤类型之一。研究表明,肿瘤干细胞在子宫内膜癌的发生发展中起重要作用。这些是高度致瘤细胞的子集,具有与正常干细胞相似的特征(无限增殖,多潜能分化,自我更新,侵略性,入侵,复发,和化学和内分泌治疗抵抗)。Wnt/β-catenin,Hedghog,和Notch1是子宫内膜癌干细胞中最常见的激活途径。癌症干细胞的存在与由不同机制引起的对化学疗法的抗性有关。各种标记,已经在这些细胞的表面上鉴定了CD24、CD40、CD44、CD9、CD133和CD166。此类标志物的较高表达转化为增强的致瘤性。然而,没有强有力的证据表明这些鉴定的标志物可以用作子宫内膜癌干细胞的通用标志物。来自基因组和蛋白质组学分析的不断增长的数据为理解人类癌症的分子基础和癌症干细胞的作用提供了一些启示。然而,还有很多事情要发现。因此,需要更多的研究来充分揭示它们的功能机制,以防止癌症的发展和复发,以及提高治疗效果。
    Endometrial cancer is one of most common types of gynaecological tumours in developing countries. It has been suggested that cancer stem cells play an important role in the development of endometrial cancer. These are a subset of highly tumorigenic cells with similar features to normal stem cells (unlimited proliferation, multi-potential differentiation, self-renewal, aggressiveness, invasion, recurrence, and chemo- and endocrine therapy resistance). Wnt/β-catenin, Hedghog, and Notch1 are the most frequently activated pathways in endometrial cancer stem cells. The presence of cancer stem cells is associated with the resistance to chemotherapy caused by different mechanisms. Various markers, including CD24, CD40, CD44, CD9, CD133, and CD 166, have been identified on the surface of these cells. A higher expression of such markers translates into enhanced tumorigenicity. However, there is no strong evidence showing that any of these identified markers can be used as the universal marker for endometrial cancer stem cells. Growing data from genomic and proteomic profiling shed some light on the understanding of the molecular basis of cancers in humans and the role of cancer stem cells. However, there is much left to discover. Therefore, more studies are needed to fully uncover their functional mechanisms in order to prevent the development and recurrence of cancer, as well as to enhance treatment effectiveness.
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  • 文章类型: Case Reports
    我们确定了一名年轻女性患者因怀疑肾脏恶性肿瘤而入院。影像学评估和讨论后进行部分肾切除术。术后活检病理提示多发低度嗜酸性肾肿瘤(LOT)伴血管平滑肌脂肪瘤生长。在查看了数据之后,我们发现LOT主要是孤立的,发生在中老年患者中。这种情况是独一无二的,我们分享它以提高对这种疾病的理解。
    We identified a young female patient admitted for suspected renal malignancy. Partial nephrectomy was performed after imaging evaluation and discussion. Postoperative biopsy pathology reported multiple low-grade eosinophilic renal tumors (LOTs) with angiomyolipoma growth. After reviewing the data, we found that LOT was mostly solitary and occurred in middle-aged and elderly patients. This case is unique and we share it to improve the understanding of this disease.
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  • 文章类型: Journal Article
    背景:肥大细胞与各种膀胱疾病的病理学有关。然而,尽管肥大细胞的患病率相对明确,但肥大细胞在膀胱组织中的分布仍不确定.使用小鼠组织模型,这项研究旨在描述肥大细胞在整个膀胱中的流行和分布。
    方法:从6只C57BL/6J雌性小鼠收集膀胱组织。肥大细胞患病率通过流式细胞术进行定量,基于以下特征性标记物的表达:CD45,CD117和FcºRIα。甲苯胺蓝染色评估肥大细胞分布,尺寸,靠近脉管系统。重复测量单向ANOVA用于评估膀胱离散层之间的肥大细胞密度,和普通的单向方差分析用于评估膀胱壁肥大细胞大小之间的潜在差异。
    结果:确定了肥大细胞占膀胱中所有活白细胞的不到4%。还发现它们在固有层和逼尿肌层中更为突出,与尿路上皮和外膜相比。此外,20.89%的肥大细胞位于脉管系统附近,这可能是考虑到它们的功能和可能导致各种膀胱病变的重要因素,如膀胱炎或膀胱过度活动症。
    结论:这些发现提供了对肥大细胞在整个膀胱中的患病率和分布的基线理解。
    BACKGROUND: Mast cells have been implicated in the pathology of various urinary bladder disorders. However, the distribution of mast cells throughout urinary bladder tissue remains uncertain despite mast cell prevalence being relatively well-defined. Using a mouse tissue model, this study aims to characterise the prevalence and distribution of mast cells throughout the urinary bladder.
    METHODS: Bladder tissues were collected from six C57BL/6J female mice. Mast cell prevalence was quantified by flow cytometry, based on the expression of the following characteristic markers: CD45, CD117 and FcɛRIα. The toluidine blue stain assessed mast cell distribution, size, and proximity to vasculature. A repeated measures one-way ANOVA was used to evaluate the density of mast cells between the discrete layers of the urinary bladder, and an ordinary one-way ANOVA was used to assess potential differences between mast cell size across the urinary bladder wall.
    RESULTS: It was determined that mast cells compose less than 4% of all live leukocytes in the urinary bladder. They were also found to be more prominent in the lamina propria and detrusor muscle layers, compared to the urothelium and adventitia. In addition, 20.89% of mast cells were located near vasculature, which may be an important factor in consideration of their function and potential to contribute to various bladder pathologies, such as cystitis or overactive bladder.
    CONCLUSIONS: These findings provide a baseline understanding of mast cell prevalence and distribution throughout the urinary bladder.
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  • 文章类型: Case Reports
    该病例报告详细介绍了一名76岁女性患者的空肠穿孔胃肠道间质瘤(GIST)的罕见情况。患者出现急性腹痛和腹胀,排便习惯没有任何改变或恶心和呕吐发作。初始诊断,包括腹部平片和超声检查,没有定论;然而,计算机断层扫描(CT)扫描显示气腹和不规则的液体收集提示小肠穿孔。手术干预发现了一个35毫米的空肠GIST,穿孔10毫米。组织病理学检查证实混合细胞型GIST具有高恶性潜能,免疫组织化学标记CD117,DOG1和波形蛋白进一步证实。分子分析阐明了关键癌基因的作用,主要是KIT和PDGFRA突变,强调分子诊断在GIST管理中的重要性。尽管演讲的严重性,患者术后恢复良好,强调及时手术和多学科方法在管理复杂GIST病例中的有效性。
    This case report details a rare instance of a perforated jejunal gastrointestinal stromal tumor (GIST) in a 76-year-old female patient. The patient presented with acute abdominal pain and distension without any changes in bowel habits or episodes of nausea and vomiting. Initial diagnostics, including abdominal plain radiography and ultrasonography, were inconclusive; however, a computed tomography (CT) scan revealed pneumoperitoneum and an irregular fluid collection suggestive of small intestine perforations. Surgical intervention uncovered a 35 mm jejunal GIST with a 10 mm perforation. Histopathological examination confirmed a mixed cell type GIST with high malignancy potential, further substantiated by immunohistochemistry markers CD117, DOG1, and vimentin. Molecular analysis illuminated the role of key oncogenes, primarily KIT and PDGFRA mutations, emphasizing the importance of molecular diagnostics in GIST management. Despite the severity of the presentation, the patient\'s postoperative recovery was favorable, highlighting the effectiveness of prompt surgical and multidisciplinary approaches in managing complex GIST cases.
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  • 文章类型: Case Reports
    尤因肉瘤中的KIT基因突变很少;然而,它们在其他肿瘤中更常见,即肥大细胞增多症。我们描述了一个成年男性的情况下,有一年的时间反复发作的疼痛,肿胀,右手第三根手指的近端指骨发红。核心活检提示可能存在肥大细胞增多症。经过四年的反复发作和症状恶化,切开活检显示尤因肉瘤有KIT基因突变(M541L,在外显子10上)。在2.6%的尤因肉瘤中发现了具有功能获得的KIT基因突变。在这种情况下,在先前的肥大细胞增殖部位发展的尤因肉瘤中检测到KIT突变,提出了原始病变可能肉瘤演变的假设.据我们所知,目前的文献中没有描述类似的病例。这也是描述尤文肉瘤中KITM541L突变(外显子10)的第一份报告。
    KIT gene mutations in Ewing sarcomas are rare; however, they are much more frequent in other neoplasms, namely mastocytosis. We describe a case of an adult male with a one-year duration of recurrent episodes of pain, swelling, and redness on the proximal phalanx of the third finger of his right hand. A core biopsy suggested a possible mastocytosis. After four years of recurrent episodes and worsening symptoms, an incisional biopsy revealed an Ewing sarcoma with a KIT gene mutation (M541L, on exon 10). KIT gene mutations with gain-of-function were identified in 2.6% of Ewing sarcomas. In this case, the detection of a KIT mutation in an Ewing sarcoma developed at the site of previous mast cell proliferation raises the hypothesis of a possible sarcomatous evolution of the original lesion. To the best of our knowledge, similar cases are not described in the current literature. This is also the first report describing the KIT M541L mutation (exon 10) in Ewing sarcoma.
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  • 文章类型: Journal Article
    卵巢癌是最致命的妇科癌症和第八常见的女性癌症。尽管技术有了重大发展,但卵巢癌的早期诊断仍然是临床问题。近70%的卵巢癌患者被诊断为III-IV期转移性疾病。目前缺乏可靠的诊断和预后生物标志物。卵巢癌复发和对化疗的耐药性带来了严重的问题,并转化为不良的预后。癌症干细胞似乎是由化学治疗抗性导致的肿瘤复发的原因。由于自我更新的能力,这些细胞对于肿瘤的启动也至关重要,区分,避免免疫破坏,促进炎症和血管生成。研究证实了CSC的发生与化疗耐药之间的关系,随后的转移,和癌症复发。因此,消除CSC对于克服耐药性和改善预后似乎很重要。本文对卵巢CSC标志物的表达进行综述,包括CD133,CD44,CD24,CD117和醛脱氢酶1,显示出潜在的预后意义。在CSC表面表达的一些标志物与临床特征相关,可用于卵巢癌的诊断和预后。然而,由于CSC的异质性和可塑性,特定CSC表型的测定是困难的。
    Ovarian cancer is the most lethal gynaecological cancer and the eighth most common female cancer. The early diagnosis of ovarian cancer remains a clinical problem despite the significant development of technology. Nearly 70% of patients with ovarian cancer are diagnosed with stages III-IV metastatic disease. Reliable diagnostic and prognostic biomarkers are currently lacking. Ovarian cancer recurrence and resistance to chemotherapy pose vital problems and translate into poor outcomes. Cancer stem cells appear to be responsible for tumour recurrence resulting from chemotherapeutic resistance. These cells are also crucial for tumour initiation due to the ability to self-renew, differentiate, avoid immune destruction, and promote inflammation and angiogenesis. Studies have confirmed an association between CSC occurrence and resistance to chemotherapy, subsequent metastases, and cancer relapses. Therefore, the elimination of CSCs appears important for overcoming drug resistance and improving prognoses. This review focuses on the expression of selected ovarian CSC markers, including CD133, CD44, CD24, CD117, and aldehyde dehydrogenase 1, which show potential prognostic significance. Some markers expressed on the surface of CSCs correlate with clinical features and can be used for the diagnosis and prognosis of ovarian cancer. However, due to the heterogeneity and plasticity of CSCs, the determination of specific CSC phenotypes is difficult.
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  • 文章类型: Journal Article
    肥大细胞瘤(MCT)是犬常见的皮肤癌,具有广泛的临床行为。这项研究的目的是开发一种新型的多色流式细胞术(FC)小组,该小组将能够在手术切除肿瘤之前对细针抽吸物(FNA)样品中的候选预后标志物(Ki-67和pKIT)进行定量。使用犬MCT和NI-1细胞系的FNA来开发包括生存力染料的FC面板(FVS620,BDBiosciences;7-AAD,Invitrogen)和以下主要缀合抗体:CD117-PE(ACK45,BDBiosciences),pKIT-A647(多克隆bs-3242R,BIOSS)和Ki-67-FITC(20Raj1,eBioscience;MIB-1,DAKO)。共收集了9个犬MCT的FNA样本,七个,产生足够的细胞用于FC分析。Ki-67抗体克隆20Raj1在应用于血液白细胞时产生阳性信号,但未能提供肿瘤肥大细胞的稳健标记。Ki-67抗体克隆MIB-1在NI-1细胞和原代MCT细胞中均提供了优异的染色质量。CD117-PE信号在固定和透化后以及在7-AAD的组合中是足够的。pKIT产生非特异性染色,不适合这种多色FC组。总之,犬MCT的FNA样品通常可以产生足够的细胞数量用于FC分析,并开发了多色FC面板,可以检测犬肥大细胞中的Ki-67。这将允许进一步研究该小组用于犬皮肤和皮下MCT预测目的的潜在用途。
    Mast cell tumor (MCT) is a common skin cancer in dogs that has a wide range of clinical behaviors. The purpose of this study was to develop a novel multicolor flow cytometry (FC) panel that will enable the quantification of candidate prognostic markers (Ki-67 and pKIT) in fine needle aspirate (FNA) samples prior to surgical removal of the tumors. FNA of canine MCTs and the NI-1 cell line were utilized to develop a FC panel that includes a viability dye (FVS620, BD Biosciences; 7-AAD, Invitrogen) and the following primary conjugated antibodies: CD117-PE (ACK45, BD Biosciences), pKIT-A647 (polyclonal bs-3242R, BIOSS) and Ki-67-FITC (20Raj1, eBioscience; MIB-1, DAKO). A total of nine FNA samples of canine MCTs were collected, seven out which produced sufficient cells for FC analysis. The Ki-67 antibody clone 20Raj1 produced a positive signal when applied to blood leukocytes but failed to provide robust labeling of neoplastic mast cells. The Ki-67 antibody clone MIB-1 delivered a superior staining quality in both the NI-1 cells and primary MCT cells. CD117-PE signal was adequate post fixation and permeabilization and in the combination of 7-AAD. pKIT produced non-specific staining and was not suitable for this multicolor FC panel. In conclusion, FNA samples of canine MCTs can often yield adequate cell numbers for FC analysis, and a multicolor FC panel was developed that can detect Ki-67 in canine mast cells. This would permit further studies into the potential use of this panel for canine cutaneous and subcutaneous MCT prognostication purposes.
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