Novel ADNP Syndrome Mice Reveal Dramatic Sex-Specific Peripheral Gene Expression With Brain Synaptic and Tau Pathologies

Gidon Karmon; Shlomo Sragovich; Gal Hacohen-Kleiman; Inbar Ben-Horin-Hazak; Petr Kasparek; Björn Schuster; Radislav Sedlacek; Metsada Pasmanik-Chor; Paschalis Theotokis; Olga Touloumi; Sofia Zoidou; Linxuan Huang; Pei You Wu; Roy Shi; Oxana Kapitansky; Alexandra Lobyntseva; Eliezer Giladi; Guy Shapira; Noam Shomron; Stefan Bereswill; Markus M Heimesaat; Nikolaos Grigoriadis; R Anne McKinney; Moran Rubinstein; Illana Gozes

doi:10.1016/j.biopsych.2021.09.018

Novel ADNP Syndrome Mice Reveal Dramatic Sex-Specific Peripheral Gene Expression With Brain Synaptic and Tau Pathologies

Biol Psychiatry. 2022 Jul 1;92(1):81-95. doi: 10.1016/j.biopsych.2021.09.018. Epub 2021 Sep 28.

Authors

Gidon Karmon¹, Shlomo Sragovich¹, Gal Hacohen-Kleiman¹, Inbar Ben-Horin-Hazak¹, Petr Kasparek², Björn Schuster², Radislav Sedlacek², Metsada Pasmanik-Chor³, Paschalis Theotokis⁴, Olga Touloumi⁴, Sofia Zoidou⁴, Linxuan Huang⁵, Pei You Wu⁵, Roy Shi⁵, Oxana Kapitansky¹, Alexandra Lobyntseva¹, Eliezer Giladi¹, Guy Shapira⁶, Noam Shomron⁶, Stefan Bereswill⁷, Markus M Heimesaat⁷, Nikolaos Grigoriadis⁴, R Anne McKinney⁵, Moran Rubinstein⁸, Illana Gozes⁹

Affiliations

¹ Elton Laboratory for Molecular Neuroendocrinology, Department of Human Molecular Genetics and Biochemistry, Sackler Faculty of Medicine, Sagol School of Neuroscience and Adams Super Center for Brain Studies, Tel Aviv University, Tel Aviv, Israel.
² Department of Transgenic Models of Diseases and Czech Centre for Phenogenomics, Institute of Molecular Genetics of the Czech Academy of Sciences, Vestec, Czech Republic.
³ Bioinformatics Unit, George S. Wise Faculty of Life Sciences, Tel Aviv University, Tel Aviv, Israel.
⁴ Department of Neurology, Laboratory of Experimental Neurology, AHEPA University Hospital, Aristotle University of Thessaloniki, Thessaloniki, Greece.
⁵ Department of Pharmacology and Therapeutics, McGill University, Montreal, Quebec, Canada.
⁶ Department of Cell and Developmental Biology and Edmond J. Safra Center for Bioinformatics, Sackler Faculty of Medicine, Tel Aviv University, Tel Aviv, Israel.
⁷ Gastrointestinal Microbiology Research Group, Institute for Microbiology, Infectious Diseases and Immunology, Charité-University Medicine Berlin, Berlin, Germany.
⁸ Elton Laboratory for Molecular Neuroendocrinology, Department of Human Molecular Genetics and Biochemistry, Sackler Faculty of Medicine, Sagol School of Neuroscience and Adams Super Center for Brain Studies, Tel Aviv University, Tel Aviv, Israel; Goldschleger Eye Research Institute, Sackler Faculty of Medicine, Tel Aviv University, Tel Aviv, Israel.
⁹ Elton Laboratory for Molecular Neuroendocrinology, Department of Human Molecular Genetics and Biochemistry, Sackler Faculty of Medicine, Sagol School of Neuroscience and Adams Super Center for Brain Studies, Tel Aviv University, Tel Aviv, Israel. Electronic address: igozes@tauex.tau.ac.il.

PMID: 34865853
DOI: 10.1016/j.biopsych.2021.09.018

Abstract

Background: ADNP is essential for embryonic development. As such, de novo ADNP mutations lead to an intractable autism/intellectual disability syndrome requiring investigation.

Methods: Mimicking humans, CRISPR (clustered regularly interspaced short palindromic repeats)-Cas9 editing produced mice carrying heterozygous Adnp p.Tyr718∗ (Tyr), a paralog of the most common ADNP syndrome mutation. Phenotypic rescue was validated by treatment with the microtubule/autophagy-protective ADNP fragment NAPVSIPQ (NAP).

Results: RNA sequencing of spleens, representing a peripheral biomarker source, revealed Tyr-specific sex differences (e.g., cell cycle), accentuated in females (with significant effects on antigen processing and cellular senescence) and corrected by NAP. Differentially expressed, NAP-correctable transcripts, including the autophagy and microbiome resilience-linked FOXO3, were also deregulated in human patient-derived ADNP-mutated lymphoblastoid cells. There were also Tyr sex-specific microbiota signatures. Phenotypically, Tyr mice, similar to patients with ADNP syndrome, exhibited delayed development coupled with sex-dependent gait defects. Speech acquisition delays paralleled sex-specific mouse syntax abnormalities. Anatomically, dendritic spine densities/morphologies were decreased with NAP amelioration. These findings were replicated in the Adnp^+/- mouse, including Foxo3 deregulation, required for dendritic spine formation. Grooming duration and nociception threshold (autistic traits) were significantly affected only in males. Early-onset tauopathy was accentuated in males (hippocampus and visual cortex), mimicking humans, and was paralleled by impaired visual evoked potentials and correction by acute NAP treatment.

Conclusions: Tyr mice model ADNP syndrome pathology. The newly discovered ADNP/NAP target FOXO3 controls the autophagy initiator LC3 (microtubule-associated protein 1 light chain 3), with known ADNP binding to LC3 augmented by NAP, protecting against tauopathy. NAP amelioration attests to specificity, with potential for drug development targeting accessible biomarkers.

Keywords: ADNP; Autism; Biomarkers; CRISPR; DEGs; Differentially expressed genes; Lymph; Lymphoblastoid cells; NAP; Tyr Adnpmouse; VEP; Visual evoked potential.

Publication types

Research Support, Non-U.S. Gov't
Research Support, U.S. Gov't, Non-P.H.S.

MeSH terms

Animals
Autistic Disorder* / pathology
Brain / metabolism
Evoked Potentials, Visual
Female
Gene Expression
Homeodomain Proteins / genetics
Humans
Intellectual Disability* / genetics
Intellectual Disability* / metabolism
Male
Mice
Nerve Tissue Proteins / genetics
Tauopathies* / metabolism
tau Proteins

Substances

ADNP protein, human
Adnp protein, mouse
Homeodomain Proteins
Nerve Tissue Proteins
tau Proteins