Sprouty2/4 deficiency disrupts early signaling centers impacting chondrogenesis in the mouse forelimb.

IF 2.4 Q2 ENDOCRINOLOGY & METABOLISM JBMR Plus Pub Date : 2025-01-10 eCollection Date: 2025-03-01 DOI:10.1093/jbmrpl/ziaf002
Linda Dalecka, Eva Hruba, Marketa Andrasova, Klara Steklikova, Zuzana Pavlikova, Klara Kucerova, Tereza Szotkowska, Martin Bartos, Marcela Buchtova, Abigail Saffron Tucker, Maria Hovorakova
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Abstract

The FGF signaling pathway plays an important role in the regulation of limb development, controlling cell migration, proliferation, differentiation, and apoptosis. Sprouty proteins act as antagonists of the FGF pathway and control the extent of FGF signaling as part of a negative feedback loop. Sprouty2/4 deficient mice evince defects in endochondral bone formation and digit patterning in their forelimbs, with pathogenesis recently related to ciliopathies. To understand the mechanisms behind these pathologies, the limb defects in Sprouty2+/-;Sprouty4-/- male and female mice were characterized and correlated to the dynamic expression patterns of Sprouty2 and Sprouty4, and the impact on the main signaling centers of the limb bud was assessed. Sprouty2 and Sprouty4 exhibited dynamic expressions during limb development. Interestingly, despite similar expression patterns in all limbs, the hindlimbs did not evince any obvious alterations in development, while the forelimbs showed consistent phenotypes of variable severity. Prenatally as well as postnatally, the left forelimb was significantly more severely affected than the right one. A broad variety of pathologies was present in the autopodium of the forelimb, including changes in digit number, size, shape, and number of bones, hand clefts, and digit fusions. Ectopic ossification of bones and abnormal bone fusions detected in micro-CT scans were frequently observed in the digital as well as in the carpal and metacarpal areas. Sprouty2+/-;Sprouty4-/- limb buds showed patchy loss of Fgf8 expression in the apical ectodermal ridge, and a loss of tissue underlying these regions. The zone of polarizing activity was also impacted, with lineage analysis highlighting a change in the contribution of Sonic hedgehog expressing cells. These findings support the link between Sproutys and Hedgehog signaling during limb development and highlight the importance of Sprouty2 and Sprouty4 in controlling early signaling centers in the limb.

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Sprouty2/4缺乏破坏影响小鼠前肢软骨形成的早期信号中心。
FGF信号通路在肢体发育调控、细胞迁移、增殖、分化和凋亡等方面发挥着重要作用。发芽蛋白作为FGF通路的拮抗剂,并作为负反馈回路的一部分控制FGF信号的程度。Sprouty2/4缺陷小鼠在其前肢软骨内骨形成和手指图案方面存在缺陷,其发病机制最近与纤毛病有关。为了了解这些病理背后的机制,我们对Sprouty2+/-;Sprouty4-/-雄性和雌性小鼠的肢体缺陷进行了表征,并与Sprouty2和Sprouty4的动态表达模式进行了关联,并评估了其对肢体芽主要信号中心的影响。Sprouty2和Sprouty4在肢体发育过程中呈现动态表达。有趣的是,尽管所有肢体的表达模式相似,但后肢在发育过程中没有表现出任何明显的改变,而前肢则表现出一致的不同严重程度的表型。产前和产后,左前肢明显比右前肢更严重。前肢自心室出现多种病变,包括手指数目、大小、形状和骨骼数量的变化、手裂和手指融合。显微ct扫描中发现的骨异位骨化和异常骨融合在指骨以及腕和掌骨区经常被观察到。Sprouty2+/-;Sprouty4-/-肢体芽显示Fgf8在顶端外胚层脊的表达缺失,以及这些区域下组织的缺失。极化活性区也受到了影响,谱系分析显示Sonic hedgehog表达细胞的贡献发生了变化。这些发现支持了肢体发育过程中sproutyys和Hedgehog信号传导之间的联系,并强调了Sprouty2和Sprouty4在控制肢体早期信号中心中的重要性。
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来源期刊
JBMR Plus
JBMR Plus Medicine-Orthopedics and Sports Medicine
CiteScore
5.80
自引率
2.60%
发文量
103
审稿时长
8 weeks
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