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Hox11 的表达特征在于正在发育的轴附突关节滑膜关节,并与出生后关节软骨形态发生相耦合,在小鼠中形成功能区。

Hox11 expression characterizes developing zeugopod synovial joints and is coupled to postnatal articular cartilage morphogenesis into functional zones in mice.

机构信息

Translational Research Program in Pediatric Orthopaedics, Division of Orthopaedic Surgery, The Children's Hospital of Philadelphia, Philadelphia, PA, USA.

Translational Research Program in Pediatric Orthopaedics, Division of Orthopaedic Surgery, The Children's Hospital of Philadelphia, Philadelphia, PA, USA.

出版信息

Dev Biol. 2021 Sep;477:49-63. doi: 10.1016/j.ydbio.2021.05.007. Epub 2021 May 16.

Abstract

Previous studies on mouse embryo limbs have established that interzone mesenchymal progenitor cells emerging at each prescribed joint site give rise to joint tissues over fetal time. These incipient tissues undergo structural maturation and morphogenesis postnatally, but underlying mechanisms of regulation remain unknown. Hox11 genes dictate overall zeugopod musculoskeletal patterning and skeletal element identities during development. Here we asked where these master regulators are expressed in developing limb joints and whether they are maintained during postnatal zeugopod joint morphogenesis. We found that Hoxa11 was predominantly expressed and restricted to incipient wrist and ankle joints in E13.5 mouse embryos, and became apparent in medial and central regions of knees by E14.5, though remaining continuously dormant in elbow joints. Closer examination revealed that Hoxa11 initially characterized interzone and neighboring cells and was then restricted to nascent articular cartilage, intra joint ligaments and structures such as meniscal horns over prenatal time. Postnatally, articular cartilage progresses from a nondescript cell-rich, matrix-poor tissue to a highly structured, thick, zonal and mechanically competent tissue with chondrocyte columns over time, most evident at sites such as the tibial plateau. Indeed, Hox11 expression (primarily Hoxa11) was intimately coupled to such morphogenetic processes and, in particular, to the topographical rearrangement of chondrocytes into columns within the intermediate and deep zones of tibial plateau that normally endures maximal mechanical loads. Revealingly, these expression patterns were maintained even at 6 months of age. In sum, our data indicate that Hox11 genes remain engaged well beyond embryonic synovial joint patterning and are specifically tied to postnatal articular cartilage morphogenesis into a zonal and resilient tissue. The data demonstrate that Hox11 genes characterize adult, terminally differentiated, articular chondrocytes and maintain region-specificity established in the embryo.

摘要

先前关于鼠胚四肢的研究已经证实,在每个预定的关节部位出现的间质间充质祖细胞会在胎儿期产生关节组织。这些初生组织在出生后会经历结构成熟和形态发生,但调节的潜在机制尚不清楚。Hox11 基因在发育过程中决定了轴旁骨骼肌肉的整体模式和骨骼元素的身份。在这里,我们询问这些主调控因子在发育中的肢体关节中表达的位置,以及它们是否在出生后轴旁关节形态发生过程中被维持。我们发现,Hoxa11 在 E13.5 鼠胚中主要表达并局限于初始腕关节和踝关节,而在 E14.5 时在膝关节的内侧和中央区域变得明显,尽管在肘关节中持续处于休眠状态。进一步的研究表明,Hoxa11 最初特征性地标记间质和邻近细胞,然后局限于初生关节软骨、关节内韧带和半月板角等结构,在产前时间。出生后,关节软骨逐渐从富含细胞、基质贫乏的组织转变为具有结构的、厚的、分区的和具有机械能力的组织,随着时间的推移,在胫骨平台等部位,软骨细胞柱变得更加明显。事实上,Hox11 的表达(主要是 Hoxa11)与这些形态发生过程密切相关,特别是与软骨细胞在胫骨平台中间和深层区域的柱状排列的拓扑重排有关,而这种排列通常会承受最大的机械负荷。值得注意的是,这些表达模式甚至在 6 个月大时仍保持不变。总之,我们的数据表明,Hox11 基因在胚胎滑膜关节模式形成之后仍然活跃,并与出生后关节软骨的形态发生密切相关,形成一个分区和有弹性的组织。这些数据表明,Hox11 基因表征了成年、终末分化的关节软骨细胞,并维持了在胚胎中建立的区域特异性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/83d7/8277736/2bc19216774b/nihms-1708206-f0002.jpg

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