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1.
徐炳祥 (2024-03-31 16:26):
#paper doi: 10.1016/j.celrep.2020.108206 Cell Reports, 2020, tagHi-C Reveals 3D Chromatin Architecture Dynamics during Mouse Hematopoiesis。高通量染色质构象捕获技术(Hi-C)一直受限于对样品量的高要求而在一些只有有限样品的场景中应用受限。本文作者介绍了一种借助tagmentation原理的改进版tagHi-C,借助Tn5的低样品损失可以将Hi-C对样品的需求降低到百细胞量级。基于此,作者解析了小鼠造血系统发育过程中的染色质构象改变。发现染色质区室结构随造血系统的发育是高度动态的,终端分化细胞染色质呈现凝聚状态,高表达基因可自身形成结构域且结构域强度与表达水平正相关等结论。本文是in situ Hi-C以来对该技术的一项重大改进。提供了一套完整的Hi-C测试数据。
IF:7.500Q1 Cell reports, 2020-09-29. DOI: 10.1016/j.celrep.2020.108206 PMID: 32997998
Abstract:
Spatiotemporal chromatin reorganization during hematopoietic differentiation has not been comprehensively characterized, mainly because of the large numbers of starting cells required for current chromatin conformation capture approaches. Here, we introduce … >>>
Spatiotemporal chromatin reorganization during hematopoietic differentiation has not been comprehensively characterized, mainly because of the large numbers of starting cells required for current chromatin conformation capture approaches. Here, we introduce a low-input tagmentation-based Hi-C (tagHi-C) method to capture the chromatin structures of hundreds of cells. Using tagHi-C, we are able to map the spatiotemporal dynamics of chromatin structure in ten primary hematopoietic stem, progenitor, and differentiated cell populations from mouse bone marrow. Our results reveal that changes in compartment dynamics and the Rabl configuration occur during hematopoietic cell differentiation. We identify gene-body-associating domains (GADs) as general structures for highly expressed genes. Moreover, we extend the body of knowledge regarding genes influenced by genome-wide association study (GWAS) loci through spatial chromatin looping. Our study provides the tagHi-C method for studying the three-dimensional (3D) genome of a small number of cells and maps the comprehensive 3D chromatin landscape of bone marrow hematopoietic cells. <<<
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2.
muton (2023-11-30 23:05):
#paper: Schonhaut, D. R., Aghajan, Z. M., Kahana, M. J., & Fried, I. (2023). A neural code for time and space in the human brain. Cell Reports, 42(11). https://doi.org/10.1016/j.celrep.2023.113238 时间和空间对人类的记忆来说是非常重要的两个维度,不仅可以帮助构建我们的经验,也可以帮助我们预测未来。以往有部分研究发现了时间和空间的神经关联,比如时间细胞和位置细胞的发现等。但是这两个维度是如何在个体记忆中被整合的仍未可知。作者基于这一问题记录了在定时性空间导航虚拟游戏中10个病人的单细胞放电情况,任务分为延迟等待阶段,寻金时间(编码阶段),下一个延迟等待阶段和挖金阶段(提取阶段)。结果发现,内侧颞叶和前额叶皮层神经元在无任务延迟期间编码时间信息,在空间探索过程中,时间和位置是独立表征的,时间细胞会在相似的事件下重新编码(remap)但是位置细胞仍会以稳定的模式放电,群体神经活动代表序列中多个事件的时间信息。本文的亮点在于首次在人类中同时研究了时间和空间信息在记忆形成中的放电特征。
IF:7.500Q1 Cell reports, 2023-11-28. DOI: 10.1016/j.celrep.2023.113238 PMID: 37906595
Abstract:
Time and space are primary dimensions of human experience. Separate lines of investigation have identified neural correlates of time and space, yet little is known about how these representations converge … >>>
Time and space are primary dimensions of human experience. Separate lines of investigation have identified neural correlates of time and space, yet little is known about how these representations converge during self-guided experience. Here, 10 subjects with intracranially implanted microelectrodes play a timed, virtual navigation game featuring object search and retrieval tasks separated by fixed delays. Time cells and place cells activate in parallel during timed navigation intervals, whereas a separate time cell sequence spans inter-task delays. The prevalence, firing rates, and behavioral coding strengths of time cells and place cells are indistinguishable-yet time cells selectively remap between search and retrieval tasks, while place cell responses remain stable. Thus, the brain can represent time and space as overlapping but dissociable dimensions. Time cells and place cells may constitute a biological basis for the cognitive map of spatiotemporal context onto which memories are written. <<<
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3.
芝麻 (2023-09-21 13:34):
#paper https://www.ncbi.nlm.nih.gov/geo/query/acc.cgi?acc=GSE216877 Multi-modal characterization and simulation of human epileptic circuitry 颞叶癫痫是第四常见的神经系统疾病,大约有40%的患者对药物治疗无效。文章根据海马硬化严重程度将四个样本颞叶癫痫进行分级,然后进行单细胞核测序对比,发现了海马颗粒细胞在疾病进展中发生的改变,并将这些变化归因于三种电导通道:BK、Cav2.2和Kir2.1,最后作者在一个网络模型中通过调试以上三种电导通路的活性,达到了将疾病进展有关的变化逆转成一个较不易兴奋的“早期疾病样”状态
IF:7.500Q1 Cell reports, 2022-12-27. DOI: 10.1016/j.celrep.2022.111873 PMID: 36577383
Abstract:
Temporal lobe epilepsy is the fourth most common neurological disorder, with about 40% of patients not responding to pharmacological treatment. Increased cellular loss is linked to disease severity and pathological … >>>
Temporal lobe epilepsy is the fourth most common neurological disorder, with about 40% of patients not responding to pharmacological treatment. Increased cellular loss is linked to disease severity and pathological phenotypes such as heightened seizure propensity. While the hippocampus is the target of therapeutic interventions, the impact of the disease at the cellular level remains unclear. Here, we show that hippocampal granule cells change with disease progression as measured in living, resected hippocampal tissue excised from patients with epilepsy. We show that granule cells increase excitability and shorten response latency while also enlarging in cellular volume and spine density. Single-nucleus RNA sequencing combined with simulations ascribes the changes to three conductances: BK, Cav2.2, and Kir2.1. In a network model, we show that these changes related to disease progression bring the circuit into a more excitable state, while reversing them produces a less excitable, "early-disease-like" state. <<<
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4.
颜林林 (2023-03-12 15:29):
#paper doi:10.1016/j.celrep.2023.112230 Cell Reports, 2023, FAM193A is a positive regulator of p53 activity. 这是一篇典型的关于药物敏感机制探索的细胞学研究,通过分子细胞生物学方法和高通量筛选技术,找到一个新调控基因,并确认其功能。癌症研究中最著名的基因当属TP53(其蛋白则称为p53),这是个抑癌基因,在癌组织中常表现出发生突变或被异常调控。针对其抑制型调控蛋白(如MDM2和MDM4),设计的化合物抑制剂,可激活或促进p53功能,进而达到治疗癌症的目的。Nutlin正是这样的候选药物分子。然而Nutlin在不同细胞系或患者中的表现却差异巨大,其作用机制尚待深入研究。这篇论文通过对药物敏感数据库的分析,以及采用CRISPR screening技术,在多个不同细胞系中进行高通量筛选,识别出FAM193A蛋白,其与Nutlin药物敏感性密切相关,并通过一系列证据,证明FAM193A在p53通路中起到正向调节作用,为后续机制研究和药物开发提供了新的方向。
IF:7.500Q1 Cell reports, 2023-03-28. DOI: 10.1016/j.celrep.2023.112230 PMID: 36897777
Abstract:
Inactivation of the p53 tumor suppressor, either by mutations or through hyperactivation of repressors such as MDM2 and MDM4, is a hallmark of cancer. Although many inhibitors of the p53-MDM2/4 … >>>
Inactivation of the p53 tumor suppressor, either by mutations or through hyperactivation of repressors such as MDM2 and MDM4, is a hallmark of cancer. Although many inhibitors of the p53-MDM2/4 interaction have been developed, such as Nutlin, their therapeutic value is limited by highly heterogeneous cellular responses. We report here a multi-omics investigation of the cellular response to MDM2/4 inhibitors, leading to identification of FAM193A as a widespread regulator of p53 function. CRISPR screening identified FAM193A as necessary for the response to Nutlin. FAM193A expression correlates with Nutlin sensitivity across hundreds of cell lines. Furthermore, genetic codependency data highlight FAM193A as a component of the p53 pathway across diverse tumor types. Mechanistically, FAM193A interacts with MDM4, and FAM193A depletion stabilizes MDM4 and inhibits the p53 transcriptional program. Last, FAM193A expression is associated with better prognosis in multiple malignancies. Altogether, these results identify FAM193A as a positive regulator of p53. <<<
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5.
小擎子 (2023-02-28 23:59):
#paper  The cancer chemotherapeutic 5-fluorouracil is a potent Fusobacterium nucleatum inhibitor and its activity is modified by intratumoral microbiota. Cell Rep. 2022 Nov 15;41(7):111625. doi: 10.1016/j.celrep.2022.111625. PMID: 36384132.文章发现结直肠癌里的肿瘤微生物群可以对一线CRC化疗药物5-氟尿嘧啶进行修饰,降低药物的功效。5-氟尿嘧啶既是对结直肠癌上皮细胞有毒性的,也是靶向结肠癌中的核梭杆菌Fn(与癌症进展和复发正相关)的。而肿瘤微生物群修饰5-氟尿嘧啶后,可以减轻对Fn和CRC上皮细胞的毒性。其中结直肠癌肿瘤微生物群里的大肠杆菌在修饰5-氟尿嘧啶的作用得到了证实。文章也用了随机森林对宏基因组数据进行了特征分类,大肠杆菌是5-FU暴露后“修饰者”组的分类,总体而言,具有最高的平均下降精度值,支持大肠杆菌作为模型中分类器的重要性。
IF:7.500Q1 Cell reports, 2022-11-15. DOI: 10.1016/j.celrep.2022.111625 PMID: 36384132
Abstract:
Fusobacterium nucleatum (Fn) is a dominant bacterial species in colorectal cancer (CRC) tissue that is associated with cancer progression and poorer patient prognosis. Following a small-molecule inhibitor screen of 1,846 … >>>
Fusobacterium nucleatum (Fn) is a dominant bacterial species in colorectal cancer (CRC) tissue that is associated with cancer progression and poorer patient prognosis. Following a small-molecule inhibitor screen of 1,846 bioactive compounds against a Fn CRC isolate, we find that 15% of inhibitors are antineoplastic agents including fluoropyrimidines. Validation of these findings reveals that 5-fluorouracil (5-FU), a first-line CRC chemotherapeutic, is a potent inhibitor of Fn CRC isolates. We also identify members of the intratumoral microbiota, including Escherichia coli, that are resistant to 5-FU. Further, CRC E. coli isolates can modify 5-FU and relieve 5-FU toxicity toward otherwise-sensitive Fn and human CRC epithelial cells. Lastly, we demonstrate that ex vivo patient CRC tumor microbiota undergo community disruption after 5-FU exposure and have the potential to deplete 5-FU levels, reducing local drug efficacy. Together, these observations argue for further investigation into the role of the CRC intratumoral microbiota in patient response to chemotherapy. <<<
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6.
笑对人生 (2022-06-30 23:48):
#paper BCL-XL inhibition induces an FGFR4-mediated rescue response in colorectal cancer.Cell Rep. 2022 Feb 15;38(7):110374. doi:10.1016/j.celrep.2022.110374 世界卫生组织国际癌症研究机构(IARC)公布的2020年全球最新癌症负担数据显示,我国结直肠癌的总体发病率已升至第二位。早期的结直肠癌患者,在采取有效治疗的情况下,5年生存率能达到90%。然而,如果对于晚期,尤其是发生转移的结直肠癌患者,尽管采取化疗和靶向治疗,生存率也仅为5%-15%。耐药性是治疗失败产生的重要原因之一。前期的研究表明,瘤内肿瘤干细胞(CSC)是导致结直肠癌患者发生耐药的潜在帮凶,未被杀死的CSC往往会利用本身干细胞特性,促进肿瘤的发生和发展。BCL-XL是Bcl-2家族成员之一,具有抗凋亡的功能。BCL-XL主要是通过两种机制来防止凋亡,一是通过与凋亡蛋白结合来抑制其凋亡作用,二是直接在线粒体外膜上形成寡聚体通道以在细胞应激时维持线粒体膜正常形态。BH3 mimetics是BCL-2、MCL1、BCL-XL 的特异性抑制剂。临床上,使用高剂量的BH3 mimetics虽然能够很好诱导肿瘤细胞的凋亡,但也对大大损伤正常细胞。本研究通过一种高效的药物靶点筛选系统,发现了FGFR4是在使用低剂量BCL-XL抑制剂下,负反馈调节通路中的一个重要协同物。同时,通过实验证实了FGFR4介导的信号通路下游分子ERK和MCL-1。ERK和MCL-1蛋白分别是促进细胞增殖和存活重要分子。体外细胞实验和患者来源体外类器官证实,FGFR4抑制剂能通过抑制MCL-1的表达,提高低剂量BCL-XL抑制剂对CSC的促凋亡作用,并且对正常结肠细胞和血小板的损伤较少。
IF:7.500Q1 Cell reports, 2022-02-15. DOI: 10.1016/j.celrep.2022.110374 PMID: 35172148
Abstract:
The heterogeneous therapy response observed in colorectal cancer is in part due to cancer stem cells (CSCs) that resist chemotherapeutic insults. The anti-apoptotic protein BCL-XL plays a critical role in … >>>
The heterogeneous therapy response observed in colorectal cancer is in part due to cancer stem cells (CSCs) that resist chemotherapeutic insults. The anti-apoptotic protein BCL-XL plays a critical role in protecting CSCs from cell death, where its inhibition with high doses of BH3 mimetics can induce apoptosis. Here, we screen a compound library for synergy with low-dose BCL-XL inhibitor A-1155463 to identify pathways that regulate sensitivity to BCL-XL inhibition and reveal that fibroblast growth factor receptor (FGFR)4 inhibition effectively sensitizes to A-1155463 both in vitro and in vivo. Mechanistically, we identify a rescue response that is activated upon BCL-XL inhibition and leads to rapid FGF2 secretion and subsequent FGFR4-mediated post-translational stabilization of MCL-1. FGFR4 inhibition prevents MCL-1 upregulation and thereby sensitizes CSCs to BCL-XL inhibition. Altogether, our findings suggest a cell transferable induction of a FGF2/FGFR4 rescue response in CRC that is induced upon BCL-XL inhibition and leads to MCL-1 upregulation. <<<
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