Nodal

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  • 文章类型: Journal Article
    迄今为止,NODAL在正常和异常L-R不对称中的作用已得到证实。在最近的一篇论文中,已经报道了该基因的突变发生在异位以及具有D-或L-心室环的转座中。NODAL和其他侧向性基因的作用可以在所有三个心脏段中分别识别:对于心房的拓扑结构和分隔,对于心室循环,以及大动脉的螺旋和对齐。
    To date, the role of NODAL in normal and abnormal L-R asymmetry has been well established. In a recent paper, mutations of this gene have been reported in heterotaxy but also in transposition with D- or L-ventricular loop. The effects of NODAL and other laterality genes can be recognized separately in all three cardiac segments: for topology and septation of the atria, for ventricular looping, and for spiralization and alignment of the great arteries.
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  • 文章类型: Journal Article
    淋巴瘤是一类主要在淋巴结中出现的肿瘤疾病。它们主要分为霍奇金淋巴瘤和非霍奇金淋巴瘤(NHL)。NHL可以是B,T和空细胞类别具有基于其组织学特征的其他亚型。淋巴瘤可以是淋巴结和淋巴结外。头颈部区域是结外淋巴瘤的第二常见部位,扁桃体是最常见的受累部位;其他部位包括鼻咽和舌根。B-细胞类型是最常见的类型。主要发生在老年人身上。演示文稿取决于所涉及的网站。各种方式,如手术治疗,化疗(或)放疗是可用的。取决于患者因素,每个阶段具有不同的存活率和预后以及对治疗的反应。在本文中,我们报告了2例扁桃体非霍奇金淋巴瘤患者,术前临床诊断和放射学诊断尚无定论,最终诊断是根据组织病理学检查确定的。
    Lymphomas are a diverse group of neoplastic disorders arising primarily in lymph nodes. They have been majorly classified into Hodgkin and Non-Hodgkin lymphomas(NHL). NHL can be of B, T and Null cell categories having further subtypes based on their histological characteristics. Lymphomas can be nodal and extra nodal. The head and neck area are the second most common site of extra nodal lymphoma, with tonsils being the most common site of involvement; other sites include the nasopharynx and tongue base. B- Cell type being the most common type. Predominantly occurs in elderly. Presentations depends on the site involved. Various modalities like surgical treatment, chemotherapy (or) radiotherapy is available. Each stage has varied survival rates and prognosis and responses to the treat depending on the patient factors. In this paper,  we report two cases of patients with non-Hodgkin lymphoma of tonsil, where the preoperative clinical diagnosis and radiological diagnosis was inconclusive and final diagnosis was established based on histopathological examination.
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  • 文章类型: Journal Article
    目的本研究旨在调查西印度人群的乳腺癌淋巴结受累情况,同时将其与各种组织学参数相关联,并评估前哨淋巴结活检的作用。方法回顾性研究2018年至2021年所有乳腺癌相关活检的组织学报告,共813个样本,已获得。将这些报告中的组织学参数提取到电子表格中,并使用统计产品和服务解决方案(SPSS,版本28.0;IBMSPSSStatisticsforWindows,Armonk,NY)用于TNM分期以及腋窝和前哨淋巴结清扫的软件,在组织学报告中发现的其他领域。结果在44.8%的病例中,患者出现在T2期有相关淋巴结扩散。对于大小为T2和更高的肿瘤,每个T分期涉及的淋巴结比未涉及的淋巴结多。相反,对于T2下分期的肿瘤,未受累的淋巴结通常多于受累的淋巴结。发现较大的肿瘤具有晚期N分期,尤其是在T3类别中,与其他T分期相比,发现N2和N3分期的病例比例明显更高。这种趋势在M分期中也可以看到,较大的肿瘤比较小的肿瘤转移更多(T4a为40%,0%为T1)。尽管观察到明显的淋巴结受累,前哨淋巴结活检通常为阴性。结论该人群中有淋巴结受累的患者多于没有淋巴结受累的患者。较大的乳腺癌肿瘤与较大的淋巴结受累有关,特别是在T2和更高的阶段。前哨淋巴结活检可以省略在较小的乳腺癌肿瘤达2厘米,尽管前哨淋巴结活检的假阴性率约为10%,但局部复发率较低。
    Objective This study aims to investigate breast cancer lymph node involvement in a West Indian population while correlating it with various histological parameters and evaluating the role of the sentinel lymph node biopsy. Method This is a retrospective study where histology reports for all breast cancer-related biopsies from 2018 to 2021, totaling 813 samples, were obtained. Histological parameters from these reports were extracted into a spreadsheet and analyzed using Statistical Product and Service Solutions (SPSS, version 28.0; IBM SPSS Statistics for Windows, Armonk, NY) software for TNM staging and axillary and sentinel lymph node dissections, among other fields found in histology reports. Results In 44.8% of cases, patients present at the T2 stage with associated lymph node spread. Each T stage had more lymph nodes involved than uninvolved for tumors sized T2 and higher. Inversely, for tumors staged under T2, there were generally more uninvolved lymph nodes than involved ones. Larger tumors were found to have advanced N staging, especially in the T3 category, where a significantly higher proportion of cases were found to have N2 and N3 staging compared to the other T stages. This trend is also seen in M staging, where larger tumors metastasize more than smaller tumors (40% for T4a, 0% for T1). Despite significant lymph node involvement being observed, sentinel lymph node biopsies were usually negative. Conclusion More patients in this population present with lymph node involvement than without. Larger breast cancer tumors are associated with greater lymph node involvement, particularly at T2 and higher stages. Sentinel lymph node biopsies can be omitted in smaller breast cancer tumors up to 2 cm in size, and the local recurrence rate is low despite a false-negative rate of around 10% in upfront sentinel lymph node biopsy.
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  • 文章类型: Journal Article
    我们报道了海胆中第一个基于RNAi的基因敲除。Dicer底物干扰RNA(DsiRNA)成功破坏了海胆Lytechinusvariagatus胚胎中多种转录本的表达,表型复制已知的吗啉代和抑制剂敲除。我们描述了我们设计最可能靶向感兴趣的mRNA的DsiRNAs的方法。针对pks1的DsiRNA的检查,一种色素生产所必需的酶,揭示pks1mRNA的破坏而不破坏现在的白化色素细胞。DsiRNA在该物种中Nodal-Lefty信号传导上的应用证实了众所周知的功能研究。基于DsiRNA的结节和左旋表型吗啉和药物抑制这些基因的表达。针对结节和左撇子的DsiRNA的稀释系列揭示了这些信号在指定背侧与腹侧中胚层方面的新扩散特性。
    DsiRNA提供了一种干扰海胆胚胎的RNAi方法。DsiRNA寡核苷酸的稀释系列揭示了Nodal梯度在建立背-腹轴中的性质。
    Dicer substrate interfering RNAs (DsiRNAs) destroy targeted transcripts using the RNA-Induced Silencing Complex (RISC) through a process called RNA interference (RNAi). This process is ubiquitous among eukaryotes. Here we report the utility of DsiRNA in embryos of the sea urchin Lytechinus variagatus (Lv). Specific knockdowns phenocopy known morpholino and inhibitor knockdowns, and DsiRNA offers a useful alternative to morpholinos. Methods for designing and obtaining specific DsiRNAs that lead to destruction of targeted mRNA are described. DsiRNAs directed against pks1, an enzyme necessary for pigment production, show how successful DsiRNA perturbations are monitored by RNA in situ analysis and by qPCR to determine relative destruction of targeted mRNA. DsiRNA-based knockdowns phenocopy morpholino- and drug-based inhibition of nodal and lefty. Other knockdowns demonstrate that the RISC operates early in development as well as on genes that are first transcribed hours after gastrulation is completed. Thus, DsiRNAs effectively mediate destruction of targeted mRNA in the sea urchin embryo. The approach offers significant advantages over other widely used methods in the urchin in terms of cost, and ease of procurement, and offers sizeable experimental advantages in terms of ease of handling, injection, and knockdown validation.
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  • 文章类型: Journal Article
    几种分化方案已经使得能够从人多能干细胞(hPSC)产生中间中胚层(IM)来源的细胞。然而,用于生成IM细胞的现有协议之间的实质性可变性损害了它们的效率,再现性,和整体成功,可能阻碍泌尿生殖系统类器官的效用。这里,我们检查了高水平的Nodal信号和BMP活性的作用,以及来自UCSD167i-99-1人诱导多能干细胞(hiPSC)系的IM细胞的规范中的WNT信号传导。我们证明了WNT和BMP信号传导的精确调节显着增强了IM分化效率。在分化48小时后,用3μΜCHIR99021处理hPSC诱导TBXT+/MIXL1+中胚层祖细胞(MP)。用3μMCHIR99021和4ng/mLBMP4的组合进一步处理导致在随后的48小时内产生OSR1+/GATA3+/PAX2+IM细胞。通过免疫荧光染色和RT-qPCR确认分化细胞的分子表征。因此,这项研究为hiPSC分化为IM细胞建立了一个一致且可重复的方案,该方案忠实地概括了IM发育的分子特征.该协议有望改善旨在在体外产生泌尿生殖系统类器官的协议的成功。在再生医学中的潜在应用,药物发现,和疾病建模。
    Several differentiation protocols have enabled the generation of intermediate mesoderm (IM)-derived cells from human pluripotent stem cells (hPSC). However, the substantial variability between existing protocols for generating IM cells compromises their efficiency, reproducibility, and overall success, potentially hindering the utility of urogenital system organoids. Here, we examined the role of high levels of Nodal signaling and BMP activity, as well as WNT signaling in the specification of IM cells derived from a UCSD167i-99-1 human induced pluripotent stem cells (hiPSC) line. We demonstrate that precise modulation of WNT and BMP signaling significantly enhances IM differentiation efficiency. Treatment of hPSC with 3 μM CHIR99021 induced TBXT+/MIXL1+ mesoderm progenitor (MP) cells after 48 h of differentiation. Further treatment with a combination of 3 μM CHIR99021 and 4 ng/mL BMP4 resulted in the generation of OSR1+/GATA3+/PAX2+ IM cells within a subsequent 48 h period. Molecular characterization of differentiated cells was confirmed through immunofluorescence staining and RT-qPCR. Hence, this study establishes a consistent and reproducible protocol for differentiating hiPSC into IM cells that faithfully recapitulates the molecular signatures of IM development. This protocol holds promise for improving the success of protocols designed to generate urogenital system organoids in vitro, with potential applications in regenerative medicine, drug discovery, and disease modeling.
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  • 文章类型: Journal Article
    背景:结直肠癌干细胞(CCSC)是在结直肠癌(CRC)患者中可以自我更新并进行多向分化的异质细胞。CCSC通常被认为是CRC的重要来源,并负责进展,转移,和CRC的治疗抗性。因此,针对这一特定亚群已被认为是克服CRC的有希望的策略.
    目的:探讨VX-509对CCSCs的作用及其机制。
    方法:通过条件无血清培养基从CRC细胞系中富集CCSC。蛋白质印迹,Aldefluor,进行了transwell和肿瘤发生试验以验证CCSC的表型特征。通过进行细胞活力分析,在HCT116CCSCs和HT29CCSCs中评估了VX-509的抗癌功效。菌落形成,球体形成,流式细胞术,和蛋白质印迹评估体外和肿瘤生长,体内免疫组织化学和免疫荧光评估。
    结果:与亲本细胞相比,来自HCT116和HT29细胞的球形细胞呈现干细胞转录因子和干细胞标志物的表达增加,并且在促进迁移和肿瘤发生方面更有效,证明CRC球体细胞显示CSC特征。VX-509抑制结直肠癌干细胞样细胞的肿瘤恶性生物学行为,正如它们的扩散所表明的那样,体外迁移和克隆性,并在体内抑制CCSC来源的异种移植肿瘤。此外,VX-509在体外抑制CRC干细胞样细胞的CSC特征并抑制上皮-间质转化(EMT)信号传导的进展。通过对差异表达基因和CSC相关数据库信息的分析,确定Nodal为VX-509对CRC干细胞样细胞的调节因子。VX-509显著下调Nodal及其下游磷酸化Smad2/3的表达以抑制EMT进展。此外,VX-509逆转了CCSCs的去分化,并抑制了Nodal过表达诱导的EMT的进展。
    结论:VX-509通过抑制Nodal的转录和蛋白表达来阻止CCSCs中的EMT过程,抑制CCSCs的去分化自我更新。
    BACKGROUND: Colorectal cancer stem cells (CCSCs) are heterogeneous cells that can self-renew and undergo multidirectional differentiation in colorectal cancer (CRC) patients. CCSCs are generally accepted to be important sources of CRC and are responsible for the progression, metastasis, and therapeutic resistance of CRC. Therefore, targeting this specific subpopulation has been recognized as a promising strategy for overcoming CRC.
    OBJECTIVE: To investigate the effect of VX-509 on CCSCs and elucidate the underlying mechanism.
    METHODS: CCSCs were enriched from CRC cell lines by in conditioned serum-free medium. Western blot, Aldefluor, transwell and tumorigenesis assays were performed to verify the phenotypic characteristics of the CCSCs. The anticancer efficacy of VX-509 was assessed in HCT116 CCSCs and HT29 CCSCs by performing cell viability analysis, colony formation, sphere formation, flow cytometry, and western blotting assessments in vitro and tumor growth, immunohistochemistry and immunofluorescence assessments in vivo.
    RESULTS: Compared with parental cells, sphere cells derived from HCT116 and HT29 cells presented increased expression of stem cell transcription factors and stem cell markers and were more potent at promoting migration and tumorigenesis, demonstrating that the CRC sphere cells displayed CSC features. VX-509 inhibited the tumor malignant biological behavior of CRC-stem-like cells, as indicated by their proliferation, migration and clonality in vitro, and suppressed the tumor of CCSC-derived xenograft tumors in vivo. Besides, VX-509 suppressed the CSC characteristics of CRC-stem-like cells and inhibited the progression of epithelial-mesenchymal transition (EMT) signaling in vitro. Nodal was identified as the regulatory factor of VX-509 on CRC stem-like cells through analyses of differentially expressed genes and CSC-related database information. VX-509 markedly downregulated the expression of Nodal and its downstream phosphorylated Smad2/3 to inhibit EMT progression. Moreover, VX-509 reversed the dedifferentiation of CCSCs and inhibited the progression of EMT induced by Nodal overexpression.
    CONCLUSIONS: VX-509 prevents the EMT process in CCSCs by inhibiting the transcription and protein expression of Nodal, and inhibits the dedifferentiated self-renewal of CCSCs.
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  • 文章类型: Preprint
    脊椎动物身体计划的前后(AP)伸长是由中胚层和神经外胚层的会聚和延伸(C&E)胃内形成运动驱动的,但是C&E的分子调节在组织之间如何或是否有所不同仍然是一个悬而未决的问题。使用斑马鱼外植体模型的AP轴延伸,我们表明神经外胚层和中胚层的C&E可以离体分离,个体组织的形态发生是由不同的形态发生信号动力学引起的。使用BMP和节点信号的精确时间操作,我们确定了一个关键的发育窗口,在此期间,高或低BMP/Nodal比率诱导神经外胚层或中胚层驱动的C&E,分别。增加的BMP活性类似地增强C&E,特别是在完整的斑马鱼胃的外胚层,强调我们的研究结果在体内的相关性。一起,这些结果表明,BMP和Nodal形态发生素信号的时间动力学激活了不同的形态发生程序,从而控制了单个组织内的C&E原肠胚形成运动。
    结论:使用斑马鱼胚胎和外植体模型,我们证明,在脊椎动物身体计划形成过程中,形态发生素信号比率的时间动力学可区分组织特异性形态发生程序。
    Anteroposterior (AP) elongation of the vertebrate body plan is driven by convergence and extension (C&E) gastrulation movements in both the mesoderm and neuroectoderm, but how or whether molecular regulation of C&E differs between tissues remains an open question. Using a zebrafish explant model of AP axis extension, we show that C&E of the neuroectoderm and mesoderm can be uncoupled ex vivo, and that morphogenesis of individual tissues results from distinct morphogen signaling dynamics. Using precise temporal manipulation of BMP and Nodal signaling, we identify a critical developmental window during which high or low BMP/Nodal ratios induce neuroectoderm- or mesoderm-driven C&E, respectively. Increased BMP activity similarly enhances C&E specifically in the ectoderm of intact zebrafish gastrulae, highlighting the in vivo relevance of our findings. Together, these results demonstrate that temporal dynamics of BMP and Nodal morphogen signaling activate distinct morphogenetic programs governing C&E gastrulation movements within individual tissues.
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  • 文章类型: Preprint
    不对称脊椎动物心脏发育是由一系列复杂的形态发生细胞运动驱动的,其协调需要心脏原基对信号线索的精确解释。在这里,我们表明Nodal在心脏管形成和不对称放置期间与FGF协同作用。这两种途径都作为心脏祖细胞(CPCs)的迁移刺激,但是FGF对于指导心脏导管不对称是可有可无的,由节点管理。我们进一步发现,Nodal通过在CPC中基于肌动蛋白的突起的形成中诱导左右不对称性来控制CPC迁移。此外,我们定义了一个发育窗口,在该窗口中,FGF信号是正确的心脏循环所必需的,并且在此过程中显示了FGF和Nodal之间的协同作用。我们提供证据,FGF可能通过增加次级心脏区域来促进心脏循环。最后,我们证明FGF信号的丢失会影响房室管(AVC)的正常发育,这可能有助于FGF缺乏心脏中异常的腔室形态。一起,我们的数据揭示了信号线索的时空动力学如何调节器官形态发生的细胞行为。
    这项研究探讨了Nodal和FGF信号在产生心脏不对称中的合作和独立作用。
    Asymmetric vertebrate heart development is driven by an intricate sequence of morphogenetic cell movements, the coordination of which requires precise interpretation of signaling cues by heart primordia. Here we show that Nodal functions cooperatively with FGF during heart tube formation and asymmetric placement. Both pathways act as migratory stimuli for cardiac progenitor cells (CPCs), but FGF is dispensable for directing heart tube asymmetry, which is governed by Nodal. We further find that Nodal controls CPC migration by inducing left-right asymmetries in the formation of actin-based protrusions in CPCs. Additionally, we define a developmental window in which FGF signals are required for proper heart looping and show cooperativity between FGF and Nodal in this process. We present evidence FGF may promote heart looping through addition of the secondary heart field. Finally, we demonstrate that loss of FGF signaling affects proper development of the atrioventricular canal (AVC), which likely contributes to abnormal chamber morphologies in FGF-deficient hearts. Together, our data shed insight into how the spatiotemporal dynamics of signaling cues regulate the cellular behaviors underlying organ morphogenesis.
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  • 文章类型: Journal Article
    妊娠成功取决于着床前期间母体耐受性的建立。调节性T细胞的免疫抑制功能对于限制由半同种异体胚泡的植入引起的炎症至关重要。母体对妊娠的免疫适应不足经常与女性不孕症和复发性植入失败有关。节点的作用,一种分泌的TGFβ超家族的形态发生原,最近在小鼠怀孕期间被牵连,因为其在女性生殖道中的条件性缺失(NodalΔ/Δ)导致严重的不育。这里,已经确定,尽管植入前过程正常,健康,有活力的胚胎,与NodalloxP/loxP对照相比,NodalΔ/Δ女性的植入失败率为50%。植入前,炎性细胞因子MCP-1、G-CSF、IFN-γ和IL-10在NodalΔ/Δ子宫中失调。对NodalΔ/Δ子宫中植入前白细胞种群的进一步分析显示浸润过多,促炎性CD11bhighLy6C+巨噬细胞与缺乏CD4+FOXP3+调节性T细胞偶联。因此,有人提出,子宫Nodal在植入前的表达在建立母体免疫耐受中具有新的作用,并且其失调应被认为是女性不孕症和复发性植入失败的潜在原因。
    Pregnancy success is dependent on the establishment of maternal tolerance during the preimplantation period. The immunosuppressive function of regulatory T cells is critical to limit inflammation arising from implantation of the semi-allogeneic blastocyst. Insufficient maternal immune adaptations to pregnancy have been frequently associated with cases of female infertility and recurrent implantation failure. The role of Nodal, a secreted morphogen of the TGFβ superfamily, was recently implicated during murine pregnancy as its conditional deletion (NodalΔ/Δ) in the female reproductive tract resulted in severe subfertility. Here, it was determined that despite normal preimplantation processes and healthy, viable embryos, NodalΔ/Δ females had a 50% implantation failure rate compared to NodalloxP/loxP controls. Prior to implantation, the expression of inflammatory cytokines MCP-1, G-CSF, IFN-γ and IL-10 was dysregulated in the NodalΔ/Δ uterus. Further analysis of the preimplantation leukocyte populations in NodalΔ/Δ uteri showed an overabundance of infiltrating, pro-inflammatory CD11bhigh Ly6C+ macrophages coupled with the absence of CD4+ FOXP3+ regulatory T cells. Therefore, it is proposed that uterine Nodal expression during the preimplantation period has a novel role in the establishment of maternal immunotolerance, and its dysregulation should be considered as a potential contributor to cases of female infertility and recurrent implantation failure.
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  • 文章类型: Journal Article
    目的:在前哨淋巴结阳性(SN+ve)黑色素瘤患者中,主动监测与定期超声检查的节点领域已成为标准,而不是完成淋巴结清扫术(CLND)。现在,这些患者中有一部分接受了辅助全身治疗,并进行了常规的横断面成像(计算机断层扫描[CT]或正电子发射断层扫描[PET]/CT)。并行超声(US)监测在这些患者中的作用尚不清楚。我们研究的目的是描述SNve节点场中节点复发的检测方式。
    方法:纳入2016年1月1日至2020年12月31日未在单一机构接受CLND治疗的SN+ve黑色素瘤患者。
    结果:共纳入225名SN+ve患者,中位随访时间为23个月。其中,119人(53%)接受了辅助全身治疗。80(36%)在任何部位复发;24(11%)在SNve字段中首先复发,其中12例(5%)仅在2个月随访时被确认为结野复发.7例(3%)首次通过超声检测到淋巴结复发,7例CT(3%),7例(3%)患者的PET/CT。在US上明显的所有淋巴结复发在PET/CT上也很明显,反之亦然。
    结论:在同时进行横断面成像的方式下,结节外的高复发率和所有US检测到的结节复发的识别表明,对于进行常规横断面成像的SN+ve黑色素瘤患者,可能不需要常规的同时进行淋巴结阳性区域的超声监测。
    OBJECTIVE: In sentinel node-positive (SN+ve) melanoma patients, active surveillance with regular ultrasound examination of the node field has become standard, rather than completion lymph node dissection (CLND). A proportion of these patients now receive adjuvant systemic therapy and have routine cross-sectional imaging (computed tomography [CT] or positron emission tomography [PET]/CT). The role of concurrent ultrasound (US) surveillance in these patients is unclear. The purpose of our study was to describe the modality of detection of nodal recurrence in SN+ve node fields.
    METHODS: SN+ve melanoma patients who did not undergo CLND treated at a single institution from January 1, 2016 to December 31, 2020 were included.
    RESULTS: A total of 225 SN+ve patients with a median follow-up of 23 months were included. Of these, 119 (53%) received adjuvant systemic therapy. Eighty (36%) developed a recurrence at any site; 24 (11%) recurred first in the SN+ve field, of which 12 (5%) were confirmed node field recurrence only at 2 months follow-up. The nodal recurrences were first detected by ultrasound in seven (3%), CT in seven (3%), and PET/CT in seven (3%) patients. All nodal recurrences evident on US were also evident on PET/CT and vice versa.
    CONCLUSIONS: The high rate of recurrences outside the node field and the identification of all US-detected nodal recurrences on concurrent cross-sectional imaging modalities suggest that routine concurrent ultrasound surveillance of the node-positive field may be unnecessary for SN+ve melanoma patients having routine cross-sectional imaging.
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