Igor S Tolokh, Nicholas Allen Kinney, Igor V Sharakhov, Alexey V Onufriev
{"title":"高度动态的薄层相关结构域与核膜之间的强烈相互作用稳定了果蝇间期染色质的三维结构。","authors":"Igor S Tolokh, Nicholas Allen Kinney, Igor V Sharakhov, Alexey V Onufriev","doi":"10.1186/s13072-023-00492-9","DOIUrl":null,"url":null,"abstract":"<p><strong>Background: </strong>Interactions among topologically associating domains (TADs), and between the nuclear envelope (NE) and lamina-associated domains (LADs) are expected to shape various aspects of three-dimensional (3D) chromatin structure and dynamics; however, relevant genome-wide experiments that may provide statistically significant conclusions remain difficult.</p><p><strong>Results: </strong>We have developed a coarse-grained dynamical model of D. melanogaster nuclei at TAD resolution that explicitly accounts for four distinct epigenetic classes of TADs and LAD-NE interactions. The model is parameterized to reproduce the experimental Hi-C map of the wild type (WT) nuclei; it describes time evolution of the chromatin over the G1 phase of the interphase. The simulations include an ensemble of nuclei, corresponding to the experimentally observed set of several possible mutual arrangements of chromosomal arms. The model is validated against multiple structural features of chromatin from several different experiments not used in model development. Predicted positioning of all LADs at the NE is highly dynamic-the same LAD can attach, detach and move far away from the NE multiple times during interphase. The probabilities of LADs to be in contact with the NE vary by an order of magnitude, despite all having the same affinity to the NE in the model. These probabilities are mostly determined by a highly variable local linear density of LADs along the genome, which also has the same strong effect on the predicted positioning of individual TADs -- higher probability of a TAD to be near NE is largely determined by a higher linear density of LADs surrounding this TAD. The distribution of LADs along the chromosome chains plays a notable role in maintaining a non-random average global structure of chromatin. Relatively high affinity of LADs to the NE in the WT nuclei substantially reduces sensitivity of the global radial chromatin distribution to variations in the strength of TAD-TAD interactions compared to the lamin depleted nuclei, where a small (0.5 kT) increase of cross-type TAD-TAD interactions doubles the chromatin density in the central nucleus region.</p><p><strong>Conclusions: </strong>A dynamical model of the entire fruit fly genome makes multiple genome-wide predictions of biological interest. The distribution of LADs along the chromatin chains affects their probabilities to be in contact with the NE and radial positioning of highly mobile TADs, playing a notable role in creating a non-random average global structure of the chromatin. We conjecture that an important role of attractive LAD-NE interactions is to stabilize global chromatin structure against inevitable cell-to-cell variations in TAD-TAD interactions.</p>","PeriodicalId":49253,"journal":{"name":"Epigenetics & Chromatin","volume":null,"pages":null},"PeriodicalIF":4.2000,"publicationDate":"2023-05-30","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10228000/pdf/","citationCount":"0","resultStr":"{\"title\":\"Strong interactions between highly dynamic lamina-associated domains and the nuclear envelope stabilize the 3D architecture of Drosophila interphase chromatin.\",\"authors\":\"Igor S Tolokh, Nicholas Allen Kinney, Igor V Sharakhov, Alexey V Onufriev\",\"doi\":\"10.1186/s13072-023-00492-9\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<p><strong>Background: </strong>Interactions among topologically associating domains (TADs), and between the nuclear envelope (NE) and lamina-associated domains (LADs) are expected to shape various aspects of three-dimensional (3D) chromatin structure and dynamics; however, relevant genome-wide experiments that may provide statistically significant conclusions remain difficult.</p><p><strong>Results: </strong>We have developed a coarse-grained dynamical model of D. melanogaster nuclei at TAD resolution that explicitly accounts for four distinct epigenetic classes of TADs and LAD-NE interactions. The model is parameterized to reproduce the experimental Hi-C map of the wild type (WT) nuclei; it describes time evolution of the chromatin over the G1 phase of the interphase. The simulations include an ensemble of nuclei, corresponding to the experimentally observed set of several possible mutual arrangements of chromosomal arms. The model is validated against multiple structural features of chromatin from several different experiments not used in model development. Predicted positioning of all LADs at the NE is highly dynamic-the same LAD can attach, detach and move far away from the NE multiple times during interphase. The probabilities of LADs to be in contact with the NE vary by an order of magnitude, despite all having the same affinity to the NE in the model. These probabilities are mostly determined by a highly variable local linear density of LADs along the genome, which also has the same strong effect on the predicted positioning of individual TADs -- higher probability of a TAD to be near NE is largely determined by a higher linear density of LADs surrounding this TAD. The distribution of LADs along the chromosome chains plays a notable role in maintaining a non-random average global structure of chromatin. Relatively high affinity of LADs to the NE in the WT nuclei substantially reduces sensitivity of the global radial chromatin distribution to variations in the strength of TAD-TAD interactions compared to the lamin depleted nuclei, where a small (0.5 kT) increase of cross-type TAD-TAD interactions doubles the chromatin density in the central nucleus region.</p><p><strong>Conclusions: </strong>A dynamical model of the entire fruit fly genome makes multiple genome-wide predictions of biological interest. 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引用次数: 0
摘要
背景:拓扑关联结构域(TADs)之间以及核包膜(NE)和薄层关联结构域(LADs)之间的相互作用预计将塑造三维(3D)染色质结构和动力学的各个方面;然而,可能提供具有统计学意义的结论的相关全基因组实验仍然困难重重:结果:我们建立了一个粗粒度的黑腹蝇核(D. melanogaster nuclei)TAD分辨率动态模型,该模型明确考虑了四类不同的TAD表观遗传和LAD-NE相互作用。该模型的参数再现了野生型(WT)细胞核的实验Hi-C图谱;它描述了染色质在间期G1阶段的时间演变。模拟包括一组细胞核,与实验观察到的染色体臂的几种可能相互排列方式相对应。根据模型开发过程中未使用的几项不同实验中染色质的多种结构特征,对模型进行了验证。预测的所有 LAD 在染色质网的位置都是高度动态的--同一个 LAD 可以在细胞间期多次附着、分离并远离染色质网。尽管在模型中所有 LAD 与 NE 的亲和力相同,但 LAD 与 NE 接触的概率却相差一个数量级。这些概率主要是由沿基因组的 LADs 高度可变的局部线性密度决定的,而这种线性密度对单个 TADs 的预测定位也有同样强烈的影响--一个 TAD 靠近 NE 的概率越高,主要是由该 TAD 周围 LADs 的线性密度越高决定的。LADs 沿染色体链的分布在维持染色质非随机平均全局结构方面发挥了显著作用。在WT细胞核中,LADs与NE的亲和力相对较高,这大大降低了全局染色质径向分布对TAD-TAD相互作用强度变化的敏感性,而在去片基细胞核中,交叉型TAD-TAD相互作用的小幅(0.5 kT)增加会使细胞核中心区域的染色质密度增加一倍:果蝇整个基因组的动力学模型做出了多个具有生物学意义的全基因组预测。LADs沿染色质链的分布会影响它们与NE接触的概率以及高移动性TADs的径向定位,在形成染色质的非随机平均全局结构方面发挥着显著作用。我们推测,LAD与NE之间有吸引力的相互作用的一个重要作用是稳定全局染色质结构,防止TAD与TAD之间相互作用不可避免的细胞间变化。
Strong interactions between highly dynamic lamina-associated domains and the nuclear envelope stabilize the 3D architecture of Drosophila interphase chromatin.
Background: Interactions among topologically associating domains (TADs), and between the nuclear envelope (NE) and lamina-associated domains (LADs) are expected to shape various aspects of three-dimensional (3D) chromatin structure and dynamics; however, relevant genome-wide experiments that may provide statistically significant conclusions remain difficult.
Results: We have developed a coarse-grained dynamical model of D. melanogaster nuclei at TAD resolution that explicitly accounts for four distinct epigenetic classes of TADs and LAD-NE interactions. The model is parameterized to reproduce the experimental Hi-C map of the wild type (WT) nuclei; it describes time evolution of the chromatin over the G1 phase of the interphase. The simulations include an ensemble of nuclei, corresponding to the experimentally observed set of several possible mutual arrangements of chromosomal arms. The model is validated against multiple structural features of chromatin from several different experiments not used in model development. Predicted positioning of all LADs at the NE is highly dynamic-the same LAD can attach, detach and move far away from the NE multiple times during interphase. The probabilities of LADs to be in contact with the NE vary by an order of magnitude, despite all having the same affinity to the NE in the model. These probabilities are mostly determined by a highly variable local linear density of LADs along the genome, which also has the same strong effect on the predicted positioning of individual TADs -- higher probability of a TAD to be near NE is largely determined by a higher linear density of LADs surrounding this TAD. The distribution of LADs along the chromosome chains plays a notable role in maintaining a non-random average global structure of chromatin. Relatively high affinity of LADs to the NE in the WT nuclei substantially reduces sensitivity of the global radial chromatin distribution to variations in the strength of TAD-TAD interactions compared to the lamin depleted nuclei, where a small (0.5 kT) increase of cross-type TAD-TAD interactions doubles the chromatin density in the central nucleus region.
Conclusions: A dynamical model of the entire fruit fly genome makes multiple genome-wide predictions of biological interest. The distribution of LADs along the chromatin chains affects their probabilities to be in contact with the NE and radial positioning of highly mobile TADs, playing a notable role in creating a non-random average global structure of the chromatin. We conjecture that an important role of attractive LAD-NE interactions is to stabilize global chromatin structure against inevitable cell-to-cell variations in TAD-TAD interactions.
期刊介绍:
Epigenetics & Chromatin is a peer-reviewed, open access, online journal that publishes research, and reviews, providing novel insights into epigenetic inheritance and chromatin-based interactions. The journal aims to understand how gene and chromosomal elements are regulated and their activities maintained during processes such as cell division, differentiation and environmental alteration.