SIPA1L1/SPAR1 Interacts with the Neurabin Family of Proteins and is Involved in GPCR Signaling

Ken Matsuura; Shizuka Kobayashi; Kohtarou Konno; Miwako Yamasaki; Takahiro Horiuchi; Takao Senda; Tomoatsu Hayashi; Kiyotoshi Satoh; Fumiko Arima-Yoshida; Kei Iwasaki; Lumi Negishi; Naomi Yasui-Shimizu; Kazuyoshi Kohu; Shigenori Kawahara; Yutaka Kirino; Tsutomu Nakamura; Masahiko Watanabe; Tadashi Yamamoto; Toshiya Manabe; Tetsu Akiyama

doi:10.1523/JNEUROSCI.0569-21.2022

SIPA1L1/SPAR1 Interacts with the Neurabin Family of Proteins and is Involved in GPCR Signaling

J Neurosci. 2022 Mar 23;42(12):2448-2473. doi: 10.1523/JNEUROSCI.0569-21.2022. Epub 2022 Feb 4.

Authors

Ken Matsuura^{1

2}, Shizuka Kobayashi³, Kohtarou Konno⁴, Miwako Yamasaki⁴, Takahiro Horiuchi⁵, Takao Senda⁶, Tomoatsu Hayashi⁷, Kiyotoshi Satoh⁷, Fumiko Arima-Yoshida³, Kei Iwasaki⁷, Lumi Negishi⁷, Naomi Yasui-Shimizu⁷, Kazuyoshi Kohu⁷, Shigenori Kawahara^{5

8}, Yutaka Kirino^{5

9}, Tsutomu Nakamura⁷, Masahiko Watanabe⁴, Tadashi Yamamoto², Toshiya Manabe³, Tetsu Akiyama¹

Affiliations

¹ Laboratory of Molecular and Genetic Information, Institute for Quantitative Biosciences, The University of Tokyo, Bunkyo-ku, Tokyo 113-0032, Japan ken.matsuura@oist.jp akiyama@iqb.u-tokyo.ac.jp.
² Cell Signal Unit, Okinawa Institute of Science and Technology, Onna-son 904-0495, Japan.
³ Division of Neuronal Network, Department of Basic Medical Sciences, Institute of Medical Science, The University of Tokyo, Minato-ku, Tokyo 108-8639, Japan.
⁴ Department of Anatomy, Hokkaido University Graduate School of Medicine, Sapporo 060-8638, Japan.
⁵ Laboratory of Neurobiophysics, School of Pharmaceutical Sciences, The University of Tokyo, Tokyo 113-0033, Japan.
⁶ Department of Anatomy, Graduate School of Medicine, Gifu University, Gifu 501-1194, Japan.
⁷ Laboratory of Molecular and Genetic Information, Institute for Quantitative Biosciences, The University of Tokyo, Bunkyo-ku, Tokyo 113-0032, Japan.
⁸ Graduate School of Science and Engineering, University of Toyama, Toyama 930-8555, Japan.
⁹ Kagawa School of Pharmaceutical Sciences, Tokushima Bunri University, Sanuki, Kagawa 769-2101, Japan.

Abstract

Signal-induced proliferation-associated 1 (SIPA1)-like 1 (SIPA1L1; also known as SPAR1) has been proposed to regulate synaptic functions that are important in maintaining normal neuronal activities, such as regulating spine growth and synaptic scaling, as a component of the PSD-95/NMDA-R-complex. However, its physiological role remains poorly understood. Here, we performed expression analyses using super-resolution microscopy (SRM) in mouse brain and demonstrated that SIPA1L1 is mainly localized to general submembranous regions in neurons, but surprisingly, not to PSD. Our screening for physiological interactors of SIPA1L1 in mouse brain identified spinophilin and neurabin-1, regulators of G-protein-coupled receptor (GPCR) signaling, but rejected PSD-95/NMDA-R-complex components. Furthermore, Sipa1l1^-/- mice showed normal spine size distribution and NMDA-R-dependent synaptic plasticity. Nevertheless, Sipa1l1^-/- mice showed aberrant responses to α₂-adrenergic receptor (a spinophilin target) or adenosine A1 receptor (a neurabin-1 target) agonist stimulation, and striking behavioral anomalies, such as hyperactivity, enhanced anxiety, learning impairments, social interaction deficits, and enhanced epileptic seizure susceptibility. Male mice were used for all experiments. Our findings revealed unexpected properties of SIPA1L1, suggesting a possible association of SIPA1L1 deficiency with neuropsychiatric disorders related to dysregulated GPCR signaling, such as epilepsy, attention deficit hyperactivity disorder (ADHD), autism, or fragile X syndrome (FXS).SIGNIFICANCE STATEMENT Signal-induced proliferation-associated 1 (SIPA1)-like 1 (SIPA1L1) is thought to regulate essential synaptic functions as a component of the PSD-95/NMDA-R-complex. In our screening for physiological SIPA1L1-interactors, we identified G-protein-coupled receptor (GPCR)-signaling regulators. Moreover, SIPA1L1 knock-out (KO) mice showed striking behavioral anomalies, which may be relevant to GPCR signaling. Our findings revealed an unexpected role of SIPA1L1, which may open new avenues for research on neuropsychiatric disorders that involve dysregulated GPCR signaling. Another important aspect of this paper is that we showed effective methods for checking PSD association and identifying native protein interactors that are difficult to solubilize. These results may serve as a caution for future claims about interacting proteins and PSD proteins, which could eventually save time and resources for researchers and avoid confusion in the field.

Keywords: GPCR; PSD; SIPA1L1; SPAR; neurabin; spinophilin.

Publication types

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

MeSH terms

Animals
Disks Large Homolog 4 Protein
GTPase-Activating Proteins / metabolism*
Male
Mice
Mice, Knockout
Microfilament Proteins / metabolism
N-Methylaspartate*
Nerve Tissue Proteins* / genetics
Nerve Tissue Proteins* / metabolism
Receptor, Adenosine A1
Receptors, G-Protein-Coupled / metabolism

Substances

Disks Large Homolog 4 Protein
GTPase-Activating Proteins
Microfilament Proteins
Nerve Tissue Proteins
Receptor, Adenosine A1
Receptors, G-Protein-Coupled
Sipa1l1 protein, mouse
neurabin
N-Methylaspartate