A Novel Phosphodiesterase 1 Inhibitor DSR-141562 Exhibits Efficacies in Animal Models for Positive, Negative, and Cognitive Symptoms Associated with Schizophrenia

Enomoto, Takeshi; Tatara, Ayaka; Goda, Masao; Nishizato, Yohei; Nishigori, Kantaro; Kitamura, Akihiro; Kamada, Mami; Taga, Shiori; Hashimoto, Takashi; Ikeda, Kazuhito; Fujii, Y.

doi:10.1124/jpet.119.260869

Cited by 19 publications

(17 citation statements)

References 65 publications

(101 reference statements)

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“…A well-known inhibitor of PDE1B is DSR-141562, which inhibits locomotor hyperactivity and reverses social interaction and novel object recognition in normal mice and rats. This molecule was also shown to improve cognition in the marmoset, a non-human primate [ 59 ] by acting through CREB and DARPP32 [ 32 , 59 ] (Fig. 1 ).…”

Section: Introductionmentioning

confidence: 99%

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Role of phosphodiesterases in the pathophysiology of neurodevelopmental disorders

Delhaye

Bardoni

2021

Mol Psychiatry

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Phosphodiesterases (PDEs) are enzymes involved in the homeostasis of both cAMP and cGMP. They are members of a family of proteins that includes 11 subfamilies with different substrate specificities. Their main function is to catalyze the hydrolysis of cAMP, cGMP, or both. cAMP and cGMP are two key second messengers that modulate a wide array of intracellular processes and neurobehavioral functions, including memory and cognition. Even if these enzymes are present in all tissues, we focused on those PDEs that are expressed in the brain. We took into consideration genetic variants in patients affected by neurodevelopmental disorders, phenotypes of animal models, and pharmacological effects of PDE inhibitors, a class of drugs in rapid evolution and increasing application to brain disorders. Collectively, these data indicate the potential of PDE modulators to treat neurodevelopmental diseases characterized by learning and memory impairment, alteration of behaviors associated with depression, and deficits in social interaction. Indeed, clinical trials are in progress to treat patients with Alzheimer’s disease, schizophrenia, depression, and autism spectrum disorders. Among the most recent results, the application of some PDE inhibitors (PDE2A, PDE3, PDE4/4D, and PDE10A) to treat neurodevelopmental diseases, including autism spectrum disorders and intellectual disability, is a significant advance, since no specific therapies are available for these disorders that have a large prevalence. In addition, to highlight the role of several PDEs in normal and pathological neurodevelopment, we focused here on the deregulation of cAMP and/or cGMP in Down Syndrome, Fragile X Syndrome, Rett Syndrome, and intellectual disability associated with the CC2D1A gene.

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Section: Introductionmentioning

confidence: 99%

“…1 ). DSR-141562 has been proposed as a therapeutic candidate for positive, negative, and cognitive symptoms in schizophrenia [ 59 ].…”

Section: Introductionmentioning

confidence: 99%

Role of phosphodiesterases in the pathophysiology of neurodevelopmental disorders

Delhaye

Bardoni

2021

Mol Psychiatry

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“…Various phosphodiesterase (PDE) families are known to influence social behaviors ( Sano et al, 2008 ; Grauer et al, 2009a ; Alexander et al, 2016 ; Gurney et al, 2017 ; Maurin et al, 2018 ; Enomoto et al, 2019 ) or neuroinflammation ( Sebastiani et al, 2006 ; Peixoto et al, 2015 ; Schwenkgrub et al, 2017 ; Tibbo and Baillie, 2020 ; Ponsaerts et al, 2021 ); but evidence suggests the PDE11A family may be a key regulator of both. Although there are four isoforms of PDE11A, PDE11A4 is the longest and only isoform found in the brain ( Yuasa et al, 2001a ; Yuasa et al, 2001b ).…”

Section: Introductionmentioning

confidence: 99%

The Role of PDE11A4 in Social Isolation-Induced Changes in Intracellular Signaling and Neuroinflammation

et al. 2021

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Phosphodiesterase 11A (PDE11A), an enzyme that degrades cyclic nucleotides (cAMP and cGMP), is the only PDE whose mRNA expression in brain is restricted to the hippocampal formation. Previously, we showed that chronic social isolation changes subsequent social behaviors in adult mice by reducing expression of PDE11A4 in the membrane fraction of the ventral hippocampus (VHIPP). Here we seek extend these findings by determining 1) if isolation-induced decreases in PDE11A4 require chronic social isolation or if they occur acutely and are sustained long-term, 2) if isolation-induced decreases occur uniquely in adults (i.e., not adolescents), and 3) how the loss of PDE11 signaling may increase neuroinflammation. Both acute and chronic social isolation decrease PDE11A4 expression in adult but not adolescent mice. This decrease in PDE11A4 is specific to the membrane compartment of the VHIPP, as it occurs neither in the soluble nor nuclear fractions of the VHIPP nor in any compartment of the dorsal HIPP. The effect of social isolation on membrane PDE11A4 is also selective in that PDE2A and PDE10A expression remain unchanged. Isolation-induced decreases in PDE11A4 expression appear to be functional as social isolation elicited changes in PDE11A-relevant signal transduction cascades (i.e., decreased pCamKIIα and pS6-235/236) and behavior (i.e., increased remote long-term memory for social odor recognition). Interestingly, we found that isolation-induced decreases in membrane PDE11A4 correlated with increased expression of interleukin-6 (IL-6) in the soluble fraction, suggesting pro-inflammatory signaling for this cytokine. This effect on IL-6 is consistent with the fact that PDE11A deletion increased microglia activation, although it left astrocytes unchanged. Together, these data suggest that isolation-induced decreases in PDE11A4 may alter subsequent social behavior via increased neuroinflammatory processes in adult mice.

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“…Here, we use mouse models to test the hypothesis that genetic similarities within the cAMP-hydrolyzing enzyme phosphodiesterase 11A (PDE11A) may be a key neurobiological mechanism underlying mutual social preference. Several PDE families are known to influence social interactions in rodents 28 – 30 , but PDE11A is particularly interesting in the context of mutual social preference. First, PDE11A expression in the brain is enriched in neurons of the ventral hippocampal formation, a brain region critical to social behaviors 31 , and deletion of Pde11a alters gene expression in the oxytocin signaling cascade (i.e., a key regulator of social bonding 32 ).…”

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confidence: 99%

A genetic basis for friendship? Homophily for membrane-associated PDE11A-cAMP-CREB signaling in CA1 of hippocampus dictates mutual social preference in male and female mice

et al. 2021

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Although the physical and mental benefits of friendships are clear, the neurobiological mechanisms driving mutual social preferences are not well understood. Studies in humans suggest friends are more genetically similar, particularly for targets within the 3’,5’-cyclic adenosine monophosphate (cAMP) cascade. Unfortunately, human studies can not provide conclusive evidence for such a biological driver of friendship given that other genetically-related factors tend to co-segregate with friendship (e.g., geographical proximity). As such, here we use mice under controlled conditions to test the hypothesis that homophily in the cAMP-degrading enzyme phosphodiesterase 11A4 (PDE11A4) can dictate mutual social preference. Using C57BL/6J and BALB/cJ mice in 2 different behavioral assays, we showed that mice with 2 intact alleles of Pde11a prefer to interact with Pde11 wild-type (WT) mice of the same genetic background over knockout (KO) mice or novel objects; whereas, Pde11 KO mice prefer to interact with Pde11 KO mice over WT mice or novel objects. This mutual social preference was seen in both adult and adolescent mice, and social preference could be eliminated or artificially elicited by strengthening or weakening PDE11A homodimerization, respectively. Stereotactic delivery of an isolated PDE11A GAF-B domain to the mouse hippocampus revealed the membrane-associated pool of PDE11A-cAMP-CREB signaling specifically within the CA1 subfield of hippocampus is most critical for regulating social preference. Our study here not only identifies PDE11A homophily as a key driver of mutual social preference across the lifespan, it offers a paradigm in which other mechanisms can be identified in a controlled fashion.

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A Novel Phosphodiesterase 1 Inhibitor DSR-141562 Exhibits Efficacies in Animal Models for Positive, Negative, and Cognitive Symptoms Associated with Schizophrenia

Cited by 19 publications

References 65 publications

Role of phosphodiesterases in the pathophysiology of neurodevelopmental disorders

Role of phosphodiesterases in the pathophysiology of neurodevelopmental disorders

The Role of PDE11A4 in Social Isolation-Induced Changes in Intracellular Signaling and Neuroinflammation

A genetic basis for friendship? Homophily for membrane-associated PDE11A-cAMP-CREB signaling in CA1 of hippocampus dictates mutual social preference in male and female mice

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