<scp><i>PLXNA2</i></scp> and <scp><i>LRRC40</i></scp> as candidate genes in autism spectrum disorder

Pijuan, Jordi; Ortigoza‐Escobar, Juan Darío; Ortiz, Juan Pablo Amelio; Alcalá, A. Molina; Calvo, María José; Cubells, M.; Hernando‐Davalillo, Cristina; Palau, Francesc; Hoenicka, Janet

doi:10.1002/aur.2502

Cited by 6 publications

(1 citation statement)

References 55 publications

(59 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Among Plexin-B3, Plexin-A2, and Plexin-A3, the relationship between Plexin-A2, Plexin-A3, and ASD is known [42,43]. Whole exome sequencing analysis, in an ASD patient with complex neurobehavioral phenotypes, who also had epilepsy and another attention disorder, clarified that the Arg-205-to-Gln (R205Q) and Arg-1653-to-Gln (R1635Q) mutations of Plexin-A2, as well as the Leu-487-to-Pro (L487P) mutation of a functionally unidentified protein leucine-rich repeat containing 40 (LRRC40), were critically associated with these symptoms, including ASD.…”

Section: Discussionmentioning

confidence: 99%

RhoG-Binding Domain of Elmo1 Ameliorates Excessive Process Elongation Induced by Autism Spectrum Disorder-Associated Sema5A

Okabe,

Miyamoto,

Ikoma

et al. 2023

Pathophysiology

View full text Add to dashboard Cite

Autism spectrum disorder (ASD) is a neurodevelopmental disorder that includes autism, Asperger’s syndrome, and pervasive developmental disorder. ASD is characterized by poor interpersonal relationships and strong attachment. The correlations between activated or inactivated gene products, which occur as a result of genetic mutations affecting neurons in ASD patients, and ASD symptoms are now of critical concern. Here, for the first time, we describe the process in which that the respective ASD-associated mutations (Arg676-to-Cys [R676C] and Ser951-to-Cys [S951C]) of semaphorin-5A (Sema5A) localize Sema5A proteins themselves around the plasma membrane in the N1E-115 cell line, a model line that can achieve neuronal morphological differentiation. The expression of each mutated construct resulted in the promotion of excessive elongation of neurite-like processes with increased differentiation protein markers; R676C was more effective than S951C. The differentiated phenotypes were very partially neutralized by an antibody, against Plexin-B3 as the specific Sema5A receptor, suggesting that the effects of Sema5A act in an autocrine manner. R676C greatly increased the activation of c-Jun N-terminal kinase (JNK), one of the signaling molecules underlying process elongation. In contrast, the blocking of JNK signaling, by a chemical JNK inhibitor or an inhibitory construct of the interaction of RhoG with Elmo1 as JNK upstream signaling molecules, recovered the excessive process elongation. These results suggest that ASD-associated mutations of Sema5A, acting through the JNK signaling cascade, lead to excessive differentiated phenotypes, and the inhibition of JNK signaling recovers them, revealing possible therapeutic targets for recovering the potential molecular and cellular phenotypes underlying certain ASD symptoms.

show abstract

Section: Discussionmentioning

confidence: 99%