Identification of limb-specific Lmx1b auto-regulatory modules with Nail-patella syndrome pathogenicity

Haro, Endika; Petit, Florence; Pira, Charmaine U.; Spady, Conor; Lucas-Toca, Sara; Yorozuya, Lauren I.; Gray, Austin L.; Escande, Fabienne; Jourdain, Anne‐Sophie; Nguyen, Andy; Fellmann, Florence; Good, Jean-Marc; Francannet, Christine; Manouvrier‐Hanu, Sylvie; Ros, María A.; Oberg, Kerby C.

doi:10.1038/s41467-021-25844-5

Cited by 20 publications

(31 citation statements)

References 36 publications

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“…As outlined above, master TFs whose HI leads to DDs are generally involved in positive feedback ( and ). Crucially, for many of these TFs, disruption of positive feedback has been identified as the cause of human disease, including LMX1B in nail–patella syndrome ( Haro et al, 2021 ), PAX6 in aniridia ( Bhatia et al, 2013 ), SOX10 in Waardenburg syndrome ( Lecerf et al, 2014 ), SOX9 in sex reversal ( Croft et al, 2018 ), FOXG1 in FOXG1 syndrome ( Ye et al, 2022 ), FOXP2 in speech–language disorder ( Becker et al, 2018 ), NFIA in a brain malformation syndrome ( Trevino et al, 2021 ), GATA2 in immunodeficiency ( Johnson et al, 2012 ), and HNF1A and HNF4A in MODY ( Hansen et al, 2002 ). If disruption of positive feedback is due to loss-of-function mutations in CREs (regulatory loss of function; Box 2 ), this frequently results in the isolated, rather than the syndromic, form of the disorder.…”

Section: A Unified Explanatory Frameworkmentioning

confidence: 99%

“…If disruption of positive feedback is due to loss-of-function mutations in CREs (regulatory loss of function; Box 2 ), this frequently results in the isolated, rather than the syndromic, form of the disorder. For example, LMX1B regulatory loss of function results in limb anomalies rather than full nail–patella syndrome ( Haro et al, 2021 ), SOX10 regulatory loss of function results in isolated Hirschsprung's disease rather than Waardenburg syndrome ( Lecerf et al, 2014 ), and FOXG1 regulatory loss of function results in isolated strabismus rather than FOXG1 syndrome ( Ye et al, 2022 ). The reason is that most CREs are tissue-specific and will, when mutated, only affect that tissue.…”

Section: A Unified Explanatory Frameworkmentioning

confidence: 99%

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Developmental disorders caused by haploinsufficiency of transcriptional regulators: a perspective based on cell fate determination

Zug

2022

Biology Open

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Many human birth defects and neurodevelopmental disorders are caused by loss-of-function mutations in a single copy of transcription factor (TF) and chromatin regulator genes. Although this dosage sensitivity has long been known, how and why haploinsufficiency (HI) of transcriptional regulators leads to developmental disorders (DDs) is unclear. Here I propose the hypothesis that such DDs result from defects in cell fate determination that are based on disrupted bistability in the underlying gene regulatory network (GRN). Bistability, a crucial systems biology concept to model binary choices such as cell fate decisions, requires both positive feedback and ultrasensitivity, the latter often achieved through TF cooperativity. The hypothesis explains why dosage sensitivity of transcriptional regulators is an inherent property of fate decisions, and why disruption of either positive feedback or cooperativity in the underlying GRN is sufficient to cause disease. I present empirical and theoretical evidence in support of this hypothesis and discuss several issues for which it increases our understanding of disease, such as incomplete penetrance. The proposed framework provides a mechanistic, systems-level explanation of HI of transcriptional regulators, thus unifying existing theories, and offers new insights into outstanding issues of human disease. This article has an associated Future Leader to Watch interview with the author of the paper.

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Section: A Unified Explanatory Frameworkmentioning

confidence: 99%

Section: A Unified Explanatory Frameworkmentioning

confidence: 99%

Developmental disorders caused by haploinsufficiency of transcriptional regulators: a perspective based on cell fate determination

Zug

2022

Biology Open

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Section: Resultsmentioning

confidence: 99%

“…We have recently characterized two limb-specific Lmx1b enhancers, termed LARM1 and LARM2 , that mediate Lmx1b limb dorsalization (Haro et al 2021). Mice homozygous for the removal of these two enhancers ( ΔLARM1/2 ) replicate the Lmx1b-null limb phenotype consisting of double-ventral distal limbs with sole pads in both surfaces and no nails (Haro et al 2021; Fig 1A-A’). In contrast to Lmx1b-null mutants that die perinatally, ΔLARM1/2 homozygous mutants survive, as they show no other Lmx1b-related systemic defects, allowing the analysis of fully differentiated double-ventral limbs.…”

Section: Resultsmentioning

confidence: 99%

“…Lmx1b plays essential roles in a wide range of developmental processes including the development of the kidney, the anterior segment of the eye, and central nervous system (specifically dopaminergic and serotonergic neurons) (Sweeney et al 2003). Recently, we characterized two limb-specific Lmx1b enhancers, termed LARM1 and LARM2 ( L mx1b a ssociated r egulatory m odule 1 and 2) that are key regulators of Lmx1b expression in the limb (Haro et al 2017; 2021). Accordingly, deletion of both LARM enhancers results in mice ( ΔLARM1/2 ) that replicate the Lmx1b-null phenotype exclusively in the limb and are, therefore, viable.…”

Section: Introductionmentioning

confidence: 99%

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Failure of digit tip regeneration in the absence of Lmx1b suggests Lmx1b functions disparate from dorsoventral polarity

Castilla-Ibeas

Zdral

Galán

et al. 2022

Preprint

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Mammalian digit tip regeneration is linked to the presence of nail tissue, but a nail–explicit model is missing. Here, we report that nail–less double–ventral digits of ΔLARM1/2 mutants that lack limb–specific Lmx1b enhancers fail to regenerate. To separate the nail′s effect from the lack of DV polarity, we also interrogate double–dorsal double–nail digits and show that they regenerate. Thus, DV polarity is not a prerequisite for regeneration and the nail requirement is supported. Transcriptomic comparison between wild–type and non-regenerative ΔLARM1/2 mutant blastemas reveals differential upregulation of vascularization and connective tissue functional signatures in wild–type versus upregulation of inflammation in the mutant. These results, together with the finding of uniform Lmx1b expression in the wild–type blastema and in the dorsal dermis underneath the nail, indicate that, in addition of the nail′s effect, a direct role for Lmx1b in driving the progression of digit tip regeneration is likely.

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Lmx1b activation in axolotl limb regeneration

Yamamoto

Kashimoto

Furukawa

et al. 2022

Developmental Dynamics

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Background: Axolotls can regenerate their limbs. In their limb regeneration process, developmental genes are re-expressed and reorganize the developmental axes, in which the position-specific genes are properly re-expressed. However, how such position specificity is reorganized in the regeneration processes has not been clarified. To address this issue, we focused on the reactivation process of Lmx1b, which determines the limb dorsal identity in many animals.Results: Here, we show that Lmx1b expression is maintained in the dorsal skin before amputation and is activated after amputation. Furthermore, we demonstrate that only cells located in the dorsal side prior to limb amputation could reactivate Lmx1b after limb amputation. We also found that Lmx1b activation was achieved by nerve presence. The nerve factors, BMP2+FGF2+ FGF8 (B2FF), consistently reactivate Lmx1b when applied to the dorsal skin.Conclusions: These results imply that the retained Lmx1b expression in the intact skin plays a role in positional memory, which instruct cells about the spatial positioning before amputation. This memory is reactivated by nerves or nerve factors that can trigger the entire limb regeneration process. Our findings highlight the role of nerves in amphibian limb regeneration, including both the initiation of limb regeneration and the reactivation of positionspecific gene expression.accessory limb model (ALM), axolotl, dorsoventral, limb regeneration, Lmx1b, nerve Key Findings• The mechanism of cell spatial recognition in limb regeneration is unknown.• We investigated the activation process of Lmx1b, which is important to establish dorsal identity. • Lmx1b is activated only in cells that were located in the dorsal region before amputation. • Lmx1b is activated by nerves or by the nerve factors, BMP2+FGF2+FGF8.• We suggest that the positional memory of the cells is maintained as faint expressions of position-specific genes and that the nerve factors are required for its activation.

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Identification of limb-specific Lmx1b auto-regulatory modules with Nail-patella syndrome pathogenicity

Cited by 20 publications

References 36 publications

Developmental disorders caused by haploinsufficiency of transcriptional regulators: a perspective based on cell fate determination

Developmental disorders caused by haploinsufficiency of transcriptional regulators: a perspective based on cell fate determination

Failure of digit tip regeneration in the absence of Lmx1b suggests Lmx1b functions disparate from dorsoventral polarity

Lmx1b activation in axolotl limb regeneration

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