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PITX2的表达以及HS3ST3A1中尼安德特人基因渗入导致了现代人类牙齿尺寸的差异。

PITX2 expression and Neanderthal introgression in HS3ST3A1 contribute to variation in tooth dimensions in modern humans.

作者信息

Li Qing, Faux Pierre, Wentworth Winchester Emma, Yang Guangrui, Chen Yingjie, Ramírez Luis Miguel, Fuentes-Guajardo Macarena, Poloni Lauriane, Steimetz Emilie, Gonzalez-José Rolando, Acuña Victor, Bortolini Maria-Cátira, Poletti Giovanni, Gallo Carla, Rothhammer Francisco, Rojas Winston, Zheng Youyi, Cox James C, Patel Vaishali, Hoffman Matthew P, Ding Li, Peng Chenchen, Cotney Justin, Navarro Nicolas, Cox Timothy C, Delgado Miguel, Adhikari Kaustubh, Ruiz-Linares Andrés

机构信息

Ministry of Education Key Laboratory of Contemporary Anthropology and Collaborative Innovation Center of Genetics and Development, School of Life Sciences and Human Phenome Institute, Fudan University, 825 Zhangheng Road, Pudong District, Shanghai 200433, China; State Key Laboratory of Complex Severe and Rare Diseases, Department of Orthopedic Surgery, Peking Union Medical College Hospital, Peking Union Medical College, and Chinese Academy of Medical Sciences, No.1 Shuaifuyuan Wangfujing, Dongcheng District, Beijing 100730, China.

Aix-Marseille Université, CNRS, EFS, ADES, 27 Boulevard Jean Moulin, Marseille 13005, France; GenPhySE Université de Toulouse, INRAE, ENVT, 24 Chemin de Borde Rouge, 31326 Castanet Tolosan, France.

出版信息

Curr Biol. 2025 Jan 6;35(1):131-144.e6. doi: 10.1016/j.cub.2024.11.027. Epub 2024 Dec 12.

Abstract

Dental morphology varies greatly throughout evolution, including in the human lineage, but little is known about the biology of this variation. Here, we use multiomics analyses to examine the genetics of variation in tooth crown dimensions. In a human cohort with mixed continental ancestry, we detected genome-wide significant associations at 18 genome regions. One region includes EDAR, a gene known to impact dental features in East Asians. Furthermore, we find that EDAR variants increase the mesiodistal diameter of all teeth, following an anterior-posterior gradient of decreasing strength. Among the 17 novel-associated regions, we replicate 7/13 in an independent human cohort and find that 4/12 orthologous regions affect molar size in mice. Two association signals point to compelling candidate genes. One is ∼61 kb from PITX2, a major determinant of tooth development. Another overlaps HS3ST3A1, a paralogous neighbor of HS3ST3B1, a tooth enamel knot factor. We document the expression of Pitx2 and Hs3st3a1 in enamel knot and dental epithelial cells of developing mouse incisors. Furthermore, associated SNPs in PITX2 and HS3ST3A1 overlap enhancers active in these cells, suggesting a role for these SNPs in gene regulation during dental development. In addition, we document that Pitx2 and Hs3st3a1/Hs3st3b1 knockout mice show alterations in dental morphology. Finally, we find that associated SNPs in HS3ST3A1 are in a DNA tract introgressed from Neanderthals, consistent with an involvement of HS3ST3A1 in tooth size variation during human evolution.

摘要

在整个进化过程中,包括人类谱系,牙齿形态差异很大,但对于这种变异的生物学机制知之甚少。在这里,我们使用多组学分析来研究牙冠尺寸变异的遗传学。在一个具有混合大陆血统的人类队列中,我们在18个基因组区域检测到全基因组显著关联。其中一个区域包括EDAR,这是一个已知会影响东亚人牙齿特征的基因。此外,我们发现EDAR变异会增加所有牙齿的近远中直径,并遵循强度递减的前后梯度。在17个新的关联区域中,我们在一个独立的人类队列中重复验证了7/13,并且发现12个直系同源区域中的4个会影响小鼠的磨牙大小。两个关联信号指向引人注目的候选基因。一个距离牙齿发育的主要决定因素PITX2约61 kb。另一个与HS3ST3A1重叠,HS3ST3A1是牙釉质结因子HS3ST3B1的旁系同源邻居。我们记录了Pitx2和Hs3st3a1在发育中小鼠切牙的釉结和牙上皮细胞中的表达。此外,PITX2和HS3ST3A1中的相关单核苷酸多态性(SNP)与这些细胞中活跃的增强子重叠,表明这些SNP在牙齿发育过程中的基因调控中发挥作用。此外,我们记录到Pitx2和Hs3st3a1/Hs3st3b1基因敲除小鼠的牙齿形态发生了改变。最后,我们发现HS3ST3A1中的相关SNP位于从尼安德特人渗入的DNA片段中,这与HS3ST3A1参与人类进化过程中的牙齿大小变异一致。

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