smooth muscle actin

平滑肌肌动蛋白
  • 文章类型: Case Reports
    我们报告了一个独特的病例,该病例是一名66岁的男子,通过计算机断层扫描偶然发现胸腺区域有肿块。CT显示明确的1.6×1×0.9cm胸腺肿块,中等均匀增强。进行了胸腔镜胸腺切除术,病理诊断为胸腺原发性血管球瘤。没有异型性或恶性组织学特征,其他部位没有原发肿瘤.据我们所知,这是文献报道的首例原发性胸腺球瘤。
    We report a unique case of a 66-year-old man who was incidentally identified to have a mass in the thymus region by computerized tomography scan. CT revealed a well-defined 1.6 × 1 × 0.9 cm thymus mass with moderate uniform enhancement. Thoracoscopic thymectomy was performed, and the pathological diagnosis was primary glomus tumor of the thymus. There were no atypia or malignant histological features, and no primary tumors in other sites. To our knowledge, this is the first case of primary thymic glomus tumor reported in the literature.
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  • 文章类型: Review
    背景:性索性腺间质肿瘤占所有睾丸肿瘤的不到10%,并且由多种组织学亚型组成。2016年,世界卫生组织引入了一种新的亚型,肌样性腺间质瘤,由具有肌肉细胞免疫组织学特征的梭形细胞组成。迄今为止,只有少数病例报告。由于它的稀有性和最近才推出的,目前关于肌样性腺间质瘤的知识是有限的,尤其是,适当的临床管理仍然不明确.
    方法:一名47岁的高加索血统男子表现为非特异性阴囊不适。在左睾丸的颅骨区域检测到直径为8.5mm的圆形且边界清晰的低回声质量。血清肿瘤标志物水平在正常范围内。保留睾丸的手术显示出9毫米的白色,硬块有锋利的手术边缘。组织学上,肿瘤由微纤维组织和梭形细胞组成,这些细胞带有细长的核。免疫组织化学检查揭示了结蛋白的表达,小肌肉肌动蛋白,和S100蛋白为肿瘤细胞的生肌性质提供了证据。没有恶性肿瘤的迹象,无论是组织学还是临床。1年的随访是顺利的。
    结论:文献调查显示22例肌样性腺间质瘤。中位年龄为37岁,肿瘤的中位大小为20毫米,也没有优势.肌样性腺间质瘤与性腺间质瘤的其他亚型和睾丸宝石细胞瘤在年龄和侧性方面没有太大区别;然而,肌样性腺间质瘤的肿瘤大小小于生殖细胞肿瘤。虽然到目前为止很少表演,保留睾丸的手术可能是这种肿瘤的适当治疗方法。肌样性腺间质瘤代表了睾丸良性新生长的新兴实体,睾丸肿瘤患者的护理人员应注意。
    BACKGROUND: Sex cord gonadal stromal tumors compose less than 10% of all testicular neoplasms and consist of a variety of histological subtypes. In 2016, the World Health Organization introduced a novel subtype, the myoid gonadal stromal tumor, that consists of spindle-shaped cells with immunohistologic features of muscle cells. Only few cases have been reported to date. Due to its rarity and owing to its only recent introduction, the current knowledge about myoid gonadal stromal tumor is limited, and particularly, appropriate clinical management is still ill-defined.
    METHODS: A 47-year-old man of Caucasian descent presented with nonspecific scrotal discomfort. A roundish and well demarcated hypoechoic mass of 8.5 mm in diameter was detected in the cranial region of the left testis. Serum tumor marker levels were within normal ranges. Testis-sparing surgery revealed a 9-mm whitish, hard mass with sharp surgical margin. Histologically, the neoplasm consisted of microfibrillar tissue with spindle-shaped cells harboring elongated nuclei. Immunohistochemical work-up disclosed expression of desmin, small muscle actin, and S100 protein giving evidence for the myogenic nature of the neoplastic cells. There was no indication of malignancy, neither histologically nor clinically. Follow-up of 1 year was uneventful.
    CONCLUSIONS: A literature survey revealed 22 previous cases of myoid gonadal stromal tumor. The median age was 37 years, the median size of the neoplasm was 20 mm, and there was no side-preponderance. Myoid gonadal stromal tumor is not much different from other subtypes of gonadal stromal tumors nor from testicular gem cell tumors regarding age and laterality; however, tumor size is smaller in myoid gonadal stromal tumors than in germ cell tumors. Although rarely performed so far, testis-sparing surgery probably constitutes an appropriate treatment of this neoplasm. Myoid gonadal stromal tumor represents an emerging novel entity of benign testicular new growths that caregivers of patients with testicular tumors should be aware of.
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  • 文章类型: Journal Article
    已经提出了P物质在肌肉骨骼纤维化中的作用,通过转化生长因子β(TGFβ)介导的作用。我们检查了P物质对增殖的体外作用,胶原蛋白分泌,在含10%胎牛血清的培养基中培养的大鼠原代真皮成纤维细胞中的胶原沉积,有或没有TGFβ。在六天文化中,P物质在0.0002至100nM的浓度下增加细胞增殖。TGFβ在0.0002至2pg/mL的浓度下增加增殖,虽然较高的浓度抑制增殖。单独使用浓度为100、0.2和0.00002nM的P物质处理不会增加每个细胞的胶原沉积,然而,当与TGFβ(5ng/mL)联合使用时,与单独的TGFβ治疗相比,胶原沉积增加。P物质处理(100nM)也在培养72小时时增加了平滑肌肌动蛋白(SMA)的表达,其水平与5ng/mLTGFβ相似;在培养48小时时,只有TGFβ增加了SMA。因此,当与TGFβ结合时,P物质可能在体内增强基质沉积中起作用,虽然这种增强可能取决于每个因素的浓度。靶向P物质的治疗可能是治疗其中P物质和TGFβ发挥作用的纤维化的可行策略。
    A role for substance P has been proposed in musculoskeletal fibrosis, with effects mediated through transforming growth factor beta (TGFβ). We examined the in vitro effects of substance P on proliferation, collagen secretion, and collagen deposition in rat primary dermal fibroblasts cultured in medium containing 10% fetal bovine serum, with or without TGFβ. In six-day cultures, substance P increased cell proliferation at concentrations from 0.0002 to 100 nM. TGFβ increased proliferation at concentrations from 0.0002 to 2 pg/mL, although higher concentrations inhibited proliferation. Substance P treatment alone at concentrations of 100, 0.2, and 0.00002 nM did not increase collagen deposition per cell, yet when combined with TGFβ (5 ng/mL), increased collagen deposition compared to TGFβ treatment alone. Substance P treatment (100 nM) also increased smooth muscle actin (SMA) expression at 72 h of culture at a level similar to 5 ng/mL of TGFβ; only TGFβ increased SMA at 48 h of culture. Thus, substance P may play a role in potentiating matrix deposition in vivo when combined with TGFβ, although this potentiation may be dependent on the concentration of each factor. Treatments targeting substance P may be a viable strategy for treating fibrosis where both substance P and TGFβ play roles.
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  • 文章类型: Journal Article
    目的:这项研究是在大鼠的下颌下腺(SSGs)中进行的,以证明与饮食中添加壳聚糖相比,生酮饮食(KD)的作用。
    方法:将18只白化病大鼠随机分为3组,每组6只。组I中的大鼠被饲喂均衡饮食并考虑为对照。同时,第二组和第三组的人被喂KD,高分子量壳聚糖的均衡饮食,分别。45天后,对大鼠实施安乐死,并仔细解剖SSGs,用苏木精和曙红(H&E)染色,α-平滑肌肌动蛋白(α-SMA)免疫组织化学染色,和刚果红特殊染色。α-SMA染色和刚果红染色的定量数据使用单向ANOVA进行统计分析,然后进行Tukey的多重比较事后检验。
    结果:关于刚果红和α-SMA染色,单因素方差分析显示三组之间存在显著差异.对于α-SMA染色和刚果红染色,II组的最高平均值分别为91.41±3.30和68.10±5.04,而第一组的最低值分别为56.13±3.96和16.87±2.19。第III组α-SMA的平均值为60.70±3.55,刚果红的平均值为19.50±1.78。Tukey的多重比较事后检验显示,I组和II组之间以及II组和III组之间存在显着差异(P<0.05)。同时,I组和III组之间无显著差异(P>0.05)。
    结论:无论我们使用什么测试,KD对大鼠SSG都有有害影响,和饮食中的壳聚糖补充剂改善了这些破坏性影响。
    OBJECTIVE: This study was carried out in the submandibular salivary glands (SSGs) of rats to demonstrate the effect of a ketogenic diet (KD) in comparison with dietary chitosan supplementation.
    METHODS: Eighteen albino rats were randomly divided into three equal groups of six animals each. Rats in Group I were fed a balanced diet and considered controls. Meanwhile, those of Groups II and III were fed a KD, a balanced diet with high molecular weight chitosan, respectively. After 45 days, rats were euthanized, and the SSGs were dissected carefully for staining with hematoxylin and eosin (H&E), alpha-smooth muscle actin (α-SMA) immunohistochemical staining, and Congo red special stain. Quantitative data from α-SMA staining and Congo red staining were statistically analyzed using one-way ANOVA followed by Tukey\'s multiple comparisons post hoc test.
    RESULTS: Regarding Congo red and α-SMA staining, one-way ANOVA revealed a significant difference between the three groups. For α-SMA staining and Congo red staining, Group II had the highest mean values of 91.41 ± 3.30 and 68.10 ± 5.04, respectively, while Group I had the lowest values of 56.13 ± 3.96 and 16.87 ± 2.19, respectively. Group III had mean values of 60.70 ± 3.55 for α-SMA and 19.50 ± 1.78 for Congo red. Tukey\'s multiple comparisons post hoc test revealed significant differences between groups I & II and between groups II & III (P < 0.05). Meanwhile, there was a nonsignificant difference between groups I and III (P > 0.05).
    CONCLUSIONS: A KD has a deleterious effect on rats\' SSG whatever the test we used, and dietary chitosan supplementation ameliorates these damaging effects.
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  • 文章类型: Journal Article
    暴露于颗粒物≤2.5μm(PM2.5)是许多肺部疾病的危险因素。尽管PM2.5对气道上皮的毒理学影响已得到很好的描述,PM2.5对肺成纤维细胞的影响研究较少。这里,我们试图研究PM2.5对成纤维细胞分化为肌成纤维细胞的影响.尽管成纤维细胞的单一处理不会导致胶原蛋白或肌成纤维细胞标志物α-SMA的变化,将成纤维细胞暴露于低浓度PM2.5的连续治疗会导致这些蛋白质的强劲增加。用核因子κB的抑制剂IMD0354治疗成纤维细胞,但不是用芳香烃受体的拮抗剂,消除了PM2.5诱导肌成纤维细胞分化的能力。这些数据表明PM2.5对成纤维细胞活化和纤维化的潜在影响,并支持利用低浓度和不同暴露方案进行毒理学研究的重要性。
    Exposure to particulate matter ≤ 2.5 µm (PM2.5) is a risk factor for many lung diseases. Although the toxicologic effects of PM2.5 on airway epithelium are well-described, the effects of PM2.5 on fibroblasts in the lung are less studied. Here, we sought to examine the effects of PM2.5 on the differentiation of fibroblasts into myofibroblasts. Although a single treatment of fibroblasts did not result in a change in collagen or the myofibroblast marker α-SMA, exposing fibroblasts to sequential treatments with PM2.5 at low concentrations caused a robust increase in these proteins. Treatment of fibroblasts with IMD0354, an inhibitor to nuclear factor κB, but not with an antagonist to aryl hydrocarbon receptor, abolished the ability of PM2.5 to induce myofibroblast differentiation. These data demonstrate that potential impact of PM2.5 to fibroblast activation and fibrosis and support the importance of utilizing low concentrations and varying exposure protocols to toxicologic studies.
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  • 文章类型: Journal Article
    背景:对膀胱癌中的多核巨细胞(MGCs)研究甚少。
    目的:为了描述功能,形态发生,保加利亚和法国患者膀胱尿路上皮癌(UC)中单核和MGCs的起源。
    方法:对2016-2020年膀胱尿路上皮癌(n=104)进行回顾性分析,采用免疫组织化学(IHC)和组织化学染色检查。35.6%的病例发现膀胱间质巨细胞,更常见的是高年级。
    结果:我们证实,膀胱UC粘膜中的MGCs对间充质和肌成纤维细胞标志物均呈阳性(波形蛋白,平滑肌肌动蛋白,Desmin,和CD34)和巨噬细胞标记CD68。此外,IHC研究揭示了这些细胞的以下特征:p16阳性;上皮阴性(CKAE1/AE3和GATA-3),血管(CD31),神经(PS100和C-KIT),形成层,blastic(CD34-blast和C-KIT),和免疫标记(IGG,免疫球蛋白G4和PD-L1);无增殖活性,没有特定的免疫功能,并且不能用于计算组合阳性评分量表。
    结论:结论:非肿瘤和肿瘤膀胱中的巨大间质细胞可以作为特征性和相对恒定的,虽然没有特异性,慢性膀胱损伤的组织学标志物,反映慢性刺激或炎症。同样,根据膀胱中单核和多核巨细胞的形态学和IHC,它们很可能代表能够使其形态适应器官病理的末端细胞。
    BACKGROUND: Multinucleated giant cells (MGCs) in bladder carcinomas are poorly studied.
    OBJECTIVE: To describe the function, morphogenesis, and origin of mononuclear and MGCs in urothelial carcinoma (UC) of the bladder in Bulgarian and French patients.
    METHODS: Urothelial bladder carcinomas (n = 104) from 2016-2020 were analyzed retrospectively using immunohistochemical (IHC) and histochemical stain examination. Giant cells in the bladder stroma were found in 35.6% of cases, more often in high-grades.
    RESULTS: We confirm that MGCs in the mucosa in UC of the bladder were positive for both mesenchymal and myofibroblast markers (vimentin, smooth muscle actin, Desmin, and CD34) and the macrophage marker CD68. Furthermore, IHC studies revealed the following profile of these cells: Positive for p16; negative for epithelial (CK AE1/AE3 and GATA-3), vascular (CD31), neural (PS100 and C-KIT), cambial, blastic (CD34-blasts and C-KIT), and immune markers (IG G, immunoglobulin G4, and PD-L1); no proliferative activity, possess no specific immune function, and cannot be used to calculate the Combined Positive Score scale.
    CONCLUSIONS: In conclusion, the giant stromal cells in non-tumor and tumor bladder can be used as a characteristic and relatively constant, although nonspecific, histological marker for chronic bladder damage, reflecting the chronic irritation or inflammation. Likewise, according to the morphological and IHC of the mono- and multinucleated giant cells in the bladder, they are most likely represent telocytes capable of adapting their morphology to the pathology of the organ.
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  • 文章类型: Case Reports
    血管球瘤并不常见,良性病变通常位于手部手指上,在诊断上具有挑战性。这是因为血管瘤或神经节囊肿在这些位置更常见。我们的病例报告强调了血管球瘤的诊断挑战和免疫组织化学染色的重要性。
    Glomus tumors are uncommon, benign lesions commonly located on the digits of the hands and are diagnostically challenging. This is because hemangiomas or ganglion cysts are more commonly identified in those locations. Our case report underlines the diagnostic challenge of a glomus tumor and the importance of immunohistochemical staining.
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  • 文章类型: Journal Article
    暴露于缺氧,由于高海拔或慢性肺病,导致肺血管壁的结构变化,包括肺动脉平滑肌细胞(PASMCs)的增生和迁移。先前的研究表明,缺氧会上调Na/H交换亚型1(NHE1)的表达,并且NHE1的抑制或丢失会阻止缺氧诱导的PASMC迁移和增殖。尚未完全描述NHE1控制PASMC功能的确切机制。在成纤维细胞中,NHE1已被证明是肌动蛋白丝的膜锚,通过衔接蛋白的结合,ezrin.因此,在这项研究中,我们测试了ezrin和NHE1/肌动蛋白相互作用在控制PASMC功能中的作用。使用暴露于体外低氧(4%O2,24h)的大鼠PASMC,我们发现低氧暴露会增加ezrin的磷酸化(激活),并通过免疫沉淀和共定位测量,促进了NHE1,磷酸化的ezrin和平滑肌特异性α-肌动蛋白(SMA)之间的相互作用。在没有缺氧的情况下,野生型人NHE1的过表达足以诱导PASMC迁移和增殖,而用NSC668394抑制ezrin磷酸化抑制NHE1/SMA在低氧PASMC中的共定位和迁移。最后,尽管表现出正常的Na/H交换活性,但过表达人类NHE1版本的氨基酸突变以防止NHE1/ezrin/SMA相互作用无法增加PASMC迁移和增殖。从这些结果来看,我们得出结论,低氧暴露会增加PASMC中的ezrin磷酸化,导致ezrin/NHE1/SMA相互作用增强。我们进一步推测,这些相互作用促进肌动蛋白细胞骨架与膜的锚定,以促进迁移和增殖所需的细胞运动和形状的变化。
    Exposure to hypoxia, due to high altitude or chronic lung disease, leads to structural changes in the pulmonary vascular wall, including hyperplasia and migration of pulmonary arterial smooth muscle cells (PASMCs). Previous studies showed that hypoxia upregulates the expression of Na+/H+ exchanger isoform 1 (NHE1) and that inhibition or loss of NHE1 prevents hypoxia-induced PASMC migration and proliferation. The exact mechanism by which NHE1 controls PASMC function has not been fully delineated. In fibroblasts, NHE1 has been shown to act as a membrane anchor for actin filaments, via binding of the adaptor protein, ezrin. Thus, in this study, we tested the role of ezrin and NHE1/actin interactions in controlling PASMC function. Using rat PASMCs exposed to in vitro hypoxia (4% O2, 24 h) we found that hypoxic exposure increased phosphorylation (activation) of ezrin, and promoted interactions between NHE1, phosphorylated ezrin and smooth muscle specific α-actin (SMA) as measured via immunoprecipitation and co-localization. Overexpression of wild-type human NHE1 in the absence of hypoxia was sufficient to induce PASMC migration and proliferation, whereas inhibiting ezrin phosphorylation with NSC668394 suppressed NHE1/SMA co-localization and migration in hypoxic PASMCs. Finally, overexpressing a version of human NHE1 in which amino acids were mutated to prevent NHE1/ezrin/SMA interactions was unable to increase PASMC migration and proliferation despite exhibiting normal Na+/H+ exchange activity. From these results, we conclude that hypoxic exposure increases ezrin phosphorylation in PASMCs, leading to enhanced ezrin/NHE1/SMA interaction. We further speculate that these interactions promote anchoring of the actin cytoskeleton to the membrane to facilitate the changes in cell movement and shape required for migration and proliferation.
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  • 文章类型: Case Reports
    背景:眼眶血管平滑肌瘤通常被认为是一种罕见的肿瘤;已经报道了大约40例。然而,在他们3年内在他们的单一机构连续6例病例的经验之后,作者推测眼眶血管平滑肌瘤的发病率可能被低估了.
    方法:一名34岁女性表现为持续2年的进行性眼球突出。眼眶计算机断层扫描和磁共振成像显示,眼眶肿瘤具有部分和异质的钆增强。Tech-99m红细胞单光子发射计算机断层扫描在血池后期显示阳性灌注,这与海绵状血管瘤的发现完全一致。在海绵状血管瘤的印象下,作者通过内镜经鼻入路获取肿块,并完全切除肿块,无神经功能缺损.病理检查显示,最终诊断为血管平滑肌瘤,平滑肌肌动蛋白(SMA)免疫染色结果为阳性。
    结论:眼眶血管平滑肌瘤的发病率可能不是很低,因为这些病变由于组织学上的相似性而可能被误诊为眼眶海绵状血管瘤。由于眼眶血管平滑肌瘤的稀有性和放射学发现相似,因此术前推测和区分海绵状血管瘤非常具有挑战性。SMA免疫染色对于区分眼眶血管平滑肌瘤与海绵状血管瘤可能至关重要。
    BACKGROUND: Orbital angioleiomyoma is generally considered a rare tumor; approximately 40 cases have been reported. However, after their experience with 6 consecutive cases in their single institution during 3 years, the authors speculate that the incidence of orbital angioleiomyomas is possibly underestimated.
    METHODS: A 34-year-old female presented with progressive exophthalmos of 2 years\' duration. Orbital computed tomography and magnetic resonance imaging revealed a well-circumscribed orbital tumor with partial and heterogeneous gadolinium enhancement. Technetium-99m red blood cell single-photon emission computed tomography showed positive perfusion in the late blood-pool phase, which was exactly consistent with the finding of a cavernous hemangioma. Under the impression of a cavernous hemangioma, the authors accessed the mass with an endoscopic endonasal approach and completely removed it without neurological deficit. Pathological examination revealed that the final diagnosis was an angioleiomyoma with positive immunostaining results for smooth muscle actin (SMA).
    CONCLUSIONS: The incidence of orbital angioleiomyomas may not be very low, as these lesions have possibly been misdiagnosed as orbital cavernous hemangiomas because of their histological similarity. Preoperative presumption and differentiation from cavernous hemangiomas are very challenging because of the rarity of orbital angioleiomyoma and similar radiological findings. SMA immunostaining may be critical to differentiate orbital angioleiomyomas from cavernous hemangiomas.
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  • 文章类型: Journal Article
    未经证实:肾细胞癌强血管化,新血管的形成是一个复杂的多步骤过程。在这项研究中,我们分析了中间血管的亚型,如双重免疫组织化学所示。
    未经鉴定:通过基于CD34和平滑肌细胞肌动蛋白的双重免疫染色鉴定肿瘤相关血管。基于上述两种标志物的表达对血管进行定量和定性分类。对中间血管进行亚分类的主要标准是存在,分布,和血管周围细胞的排列。
    未经证实:我们描述了特别在肿瘤区域发现的中间血管的三种亚型:亚型1缺乏血管周围细胞,亚型2显示分散的周细胞附着在血管壁上,亚型3在一侧显示出连续的血管周围细胞层。
    未经授权:我们首次描述了肾细胞癌相关中间血管的三种亚型,这可能是重要的预后和抗血管治疗的潜在目标。
    UNASSIGNED: Renal cell carcinoma is strongly vascularized, and formation of new blood vessels is a complex and multi-step process. In this study, we analysed the subtypes of intermediate blood vessels, as shown by double immunohistochemistry.
    UNASSIGNED: Tumour-associated blood vessels were identified by double immunostaining based on CD34 and smooth muscle cell actin. Blood vessels were classified both quantitatively and qualitatively based on the expression of the aforementioned two markers. The main criteria to sub-classify intermediate blood vessels was the presence, distribution, and arrangement of perivascular cells.
    UNASSIGNED: We described three subtypes of intermediate blood vessels found particularly in the tumour area: Subtype 1 lacked perivascular cells, subtype 2 showed scattered pericytes attached to the vascular wall, and subtype 3 showed a continuous layer of perivascular cells on one side.
    UNASSIGNED: We describe for the first time three subtypes of renal cell carcinoma-associated intermediate blood vessels, which could be important in prognosis and as potential targets for anti-vascular therapy.
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