Dominant mutations of the Notch ligand Jagged1 cause peripheral neuropathy

Sullivan, Jeremy M.; Motley, William W.; Johnson, Janel O.; Aisenberg, William H.; Marshall, Katherine L.; Barwick, Katy; Kong, Lingling; Huh, Jennifer S.; Saavedra-Rivera, Pamela C.; McEntagart, Meriel; Marion, Marie Helene; Hicklin, Lucy A.; Modarres, Hamid; Baple, Emma L.; Farah, Mohamed H.; Zuberi, Aamir; Lutz, Cathleen; Gaudet, Rachelle; Traynor, Bryan J.; Crosby, Andrew H.; Sumner, Charlotte J.

doi:10.1172/jci128152

Cited by 13 publications

(13 citation statements)

References 24 publications

(26 reference statements)

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“…9 Dominant, heterozygous truncating, or missense mutations in Notch ligands can cause severe congenital disorders, including the JAG1-associated Alagille syndrome 1 (AGS [MIM: 118450]); tetralogy of Fallot (TOF [MIM: 187500]); deafness, congenital heart defects, and posterior embryotoxon (DCHE [MIM: 617992]); peripheral neuropathy; DLL1-associated neurodevelopmental disorder with nonspecific brain abnormalities and with or without seizures (NEDBAS [MIM: 618709]); and DLL4associated Adams-Oliver syndrome 6 (AOS6 [MIM: 616589]). [10][11][12][13][14][15] The DLL3-associated autosomal recessive spondylocostal dysostosis (SCDO1 [MIM: 277300]) is caused by bi-allelic DLL3 pathogenic variants. 16 JAG2 is located at chromosomal region 14q32.33, comprises 26 exons, and is constrained for predicted loss-of-function (pLoF) variants in the gnomAD.…”

Section: Introductionmentioning

confidence: 99%

A form of muscular dystrophy associated with pathogenic variants in JAG2

Coppens

Barnard

Puusepp

et al. 2021

The American Journal of Human Genetics

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Section: Introductionmentioning

confidence: 99%

A form of muscular dystrophy associated with pathogenic variants in JAG2

Coppens

Barnard

Puusepp

et al. 2021

The American Journal of Human Genetics

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“…There is increasing evidence of the importance of Notch signaling through its ligand Jag1 in the context of the peripheral nerve disorders. Mutations in Jag1 have been associated with peripheral neuropathy in humans [ 83 ]. Transgenic mice bearing the same mutations in Jag1 as affected patients display abnormal focally folded myelin [ 83 ].…”

Section: Bace1 Substrates With Immunomodulatory Potentialmentioning

confidence: 99%

“…Mutations in Jag1 have been associated with peripheral neuropathy in humans [ 83 ]. Transgenic mice bearing the same mutations in Jag1 as affected patients display abnormal focally folded myelin [ 83 ]. More broadly, Notch signaling has been shown to play a role in the regulation of Schwann cells and post-natal myelination [ 84 ].…”

Section: Bace1 Substrates With Immunomodulatory Potentialmentioning

confidence: 99%

“…Given the abundance of Notch receptors and Notch ligands, it is unlikely that BACE1 would have absolute regulatory control over any of these effects, but rather it could be a crucial mediator that helps tip the balance of signaling towards a pro-regenerative phenotype in the peripheral nerve. The link between mutations in Jag1 and peripheral neuropathies [ 83 ] also highlights an interesting avenue of clinically significant research to pursue in the future.…”

Section: Bace1 Substrates With Immunomodulatory Potentialmentioning

confidence: 99%

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The influence of BACE1 on macrophage recruitment and activity in the injured peripheral nerve

Fissel

Farah

2021

J Neuroinflammation

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Following peripheral nerve injury, multiple cell types, including axons, Schwann cells, and macrophages, coordinate to promote nerve regeneration. However, this capacity for repair is limited, particularly in older populations, and current treatments are insufficient. A critical component of the regeneration response is the network of cell-to-cell signaling in the injured nerve microenvironment. Sheddases are expressed in the peripheral nerve and play a role in the regulation if this cell-to-cell signaling through cleavage of transmembrane proteins, enabling the regulation of multiple pathways through cis- and trans-cellular regulatory mechanisms. Enhanced axonal regeneration has been observed in mice with deletion of the sheddase beta-secretase (BACE1), a transmembrane aspartyl protease that has been studied in the context of Alzheimer’s disease. BACE1 knockout (KO) mice display enhanced macrophage recruitment and activity following nerve injury, although it is unclear whether this plays a role in driving the enhanced axonal regeneration. Further, it is unknown by what mechanism(s) BACE1 increases macrophage recruitment and activity. BACE1 has many substrates, several of which are known to have immunomodulatory activity. This review will discuss current knowledge of the role of BACE1 and other sheddases in peripheral nerve regeneration and outline known immunomodulatory BACE1 substrates and what potential roles they could play in peripheral nerve regeneration. Currently, the literature suggests that BACE1 and substrates that are expressed by neurons and Schwann cells are likely to be more important for this process than those expressed by macrophages. More broadly, BACE1 may play a role as an effector of immunomodulation beyond the peripheral nerve.

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“…Les immunomarquages des protéines membranaires sont normaux hormis un CAS CLINIQUE nerveux central (SNC) (mutations dominantes de DLL1) [8][9][10][11], au syndrome CADASIL consécutif aux mutations du gène NOTCH3 (Cerebral autosomal dominant arteriopathy with subcortical infarcts and leukoencephalopathy) [14], ainsi qu'au syndrome de dysostose spondylocostale (mutations récessives du gène DLL3) [12]. Par ailleurs, des mutations du gène JAG1 ont été également associées à des neuropathies périphériques héréditaires avec atteinte des cordes vocales [13]. Concernant la dystrophie musculaire liée au gène JAG2, le début des symptômes est variable, s'étendant de la petite enfance à l'adolescence.…”

Section: Observationunclassified