. 2022 Aug;27(8):3316-3327.

doi: 10.1038/s41380-022-01603-w. Epub 2022 May 10.

SH3- and actin-binding domains connect ADNP and SHANK3, revealing a fundamental shared mechanism underlying autism

Yanina Ivashko-Pachima^{1

2}, Maram Ganaiem^{1

2}, Inbar Ben-Horin-Hazak^{1

2}, Alexandra Lobyntseva^{1

2}, Naomi Bellaiche^{1

2}, Inbar Fischer², Gilad Levy², Shlomo Sragovich^{1

2}, Gidon Karmon^{1

2}, Eliezer Giladi^{1

2}, Shula Shazman³, Boaz Barak^{2

4}, Illana Gozes^{5

6}

Affiliations

¹ The Elton Laboratory for Neuroendocrinology, Department of Human Molecular Genetics and Biochemistry, Sackler Faculty of Medicine, Adams Super Center for Brain Studies, Tel Aviv University, Tel Aviv, Israel.
² Sagol School of Neuroscience, Tel Aviv University, Tel Aviv, Israel.
³ Department of Mathematics and Computer Science, The Open University of Israel, Raanana, Israel.
⁴ School of Psychological Sciences, Faculty of Social Sciences, Tel Aviv University, Tel Aviv, Israel.
⁵ The Elton Laboratory for Neuroendocrinology, Department of Human Molecular Genetics and Biochemistry, Sackler Faculty of Medicine, Adams Super Center for Brain Studies, Tel Aviv University, Tel Aviv, Israel. igozes@tauex.tau.ac.il.
⁶ Sagol School of Neuroscience, Tel Aviv University, Tel Aviv, Israel. igozes@tauex.tau.ac.il.

PMID: 35538192
DOI: 10.1038/s41380-022-01603-w

SH3- and actin-binding domains connect ADNP and SHANK3, revealing a fundamental shared mechanism underlying autism

Yanina Ivashko-Pachima et al. Mol Psychiatry. 2022 Aug.

. 2022 Aug;27(8):3316-3327.

doi: 10.1038/s41380-022-01603-w. Epub 2022 May 10.

Authors

Affiliations

¹ The Elton Laboratory for Neuroendocrinology, Department of Human Molecular Genetics and Biochemistry, Sackler Faculty of Medicine, Adams Super Center for Brain Studies, Tel Aviv University, Tel Aviv, Israel.
² Sagol School of Neuroscience, Tel Aviv University, Tel Aviv, Israel.
³ Department of Mathematics and Computer Science, The Open University of Israel, Raanana, Israel.
⁴ School of Psychological Sciences, Faculty of Social Sciences, Tel Aviv University, Tel Aviv, Israel.
⁵ The Elton Laboratory for Neuroendocrinology, Department of Human Molecular Genetics and Biochemistry, Sackler Faculty of Medicine, Adams Super Center for Brain Studies, Tel Aviv University, Tel Aviv, Israel. igozes@tauex.tau.ac.il.
⁶ Sagol School of Neuroscience, Tel Aviv University, Tel Aviv, Israel. igozes@tauex.tau.ac.il.

PMID: 35538192
DOI: 10.1038/s41380-022-01603-w

Abstract

De novo heterozygous mutations in activity-dependent neuroprotective protein (ADNP) cause autistic ADNP syndrome. ADNP mutations impair microtubule (MT) function, essential for synaptic activity. The ADNP MT-associating fragment NAPVSIPQ (called NAP) contains an MT end-binding protein interacting domain, SxIP (mimicking the active-peptide, SKIP). We hypothesized that not all ADNP mutations are similarly deleterious and that the NAPV portion of NAPVSIPQ is biologically active. Using the eukaryotic linear motif (ELM) resource, we identified a Src homology 3 (SH3) domain-ligand association site in NAP responsible for controlling signaling pathways regulating the cytoskeleton, namely NAPVSIP. Altogether, we mapped multiple SH3-binding sites in ADNP. Comparisons of the effects of ADNP mutations p.Glu830synfs*83, p.Lys408Valfs*31, p.Ser404* on MT dynamics and Tau interactions (live-cell fluorescence-microscopy) suggested spared toxic function in p.Lys408Valfs*31, with a regained SH3-binding motif due to the frameshift insertion. Site-directed-mutagenesis, abolishing the p.Lys408Valfs*31 SH3-binding motif, produced MT toxicity. NAP normalized MT activities in the face of all ADNP mutations, although, SKIP, missing the SH3-binding motif, showed reduced efficacy in terms of MT-Tau interactions, as compared with NAP. Lastly, SH3 and multiple ankyrin repeat domains protein 3 (SHANK3), a major autism gene product, interact with the cytoskeleton through an actin-binding motif to modify behavior. Similarly, ELM analysis identified an actin-binding site on ADNP, suggesting direct SH3 and indirect SHANK3/ADNP associations. Actin co-immunoprecipitations from mouse brain extracts showed NAP-mediated normalization of Shank3-Adnp-actin interactions. Furthermore, NAP treatment ameliorated aberrant behavior in mice homozygous for the Shank3 ASD-linked InsG3680 mutation, revealing a fundamental shared mechanism between ADNP and SHANK3.

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SH3- and actin-binding domains connect ADNP and SHANK3, revealing a fundamental shared mechanism underlying autism

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SH3- and actin-binding domains connect ADNP and SHANK3, revealing a fundamental shared mechanism underlying autism

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