Mutation-specific pathophysiological mechanisms define different neurodevelopmental disorders associated with SATB1 dysfunction

Hoed, Joery den; Boer, Elke de; Voisin, Norine; Dingemans, Alexander J.M.; Guex, Nicolas; Wiel, Laurens; Nellåker, Christoffer; Amudhavalli, Shivarajan; Banka, Siddharth; Béna, Frédérique; Ben‐Zeev, Bruria; Bonagura, V.R.; Bruel, Ange‐Line; Brunet, Theresa; Brunner, Han G.; Chew, Hui Bein; Chrast, Jacqueline; Cimbalistienė, Loreta; Coon, Hilary; Délot, Emmanuèlle C.; Démurger, Florence; Denommé‐Pichon, Anne‐Sophie; Depienne, Christel; Donnai, Dian; Dyment, David A.; Elpeleg, Orly; Faivre, Laurence; Gilissen, Christian; Granger, Leslie; Haber, Benjamin; Hachiya, Yasuo; Abedi, Yasmin Hamzavi; Hanebeck, Jennifer; Hehir-Kwa, Jayne Y.; Horist, Brooke; Itai, Toshiyuki; Jackson, Adam; Jewell, Rosalyn; Jones, Kelly L.; Joss, Shelagh; Kashii, Hirofumi; Kato, Mitsuhiro; Kattentidt-Mouravieva, Anja A; Kok, Fernando; Kotzaeridou, Urania; Krishnamurthy, Vidya; Kučinskas, Vaidutis; Kuechler, Alma; Lavillaureix, Alinoë; Liu, Pengfei; Manwaring, Linda; Matsumoto, Naomichi; Mazel, Benoît; McWalter, Kirsty; Meiner, Vardiella; Mikati, Mohamad A.; Miyatake, Satoko; Mizuguchi, Takeshi; Moey, L.H.; Mohammed, Shehla; Mor‐Shaked, Hagar; Mountford, Hayley S.; Newbury‐Ecob, Ruth; Odent, Sylvie; Orec, Laura; Osmond, Matthew; Palculict, Timothy Blake; Parker, Michael; Petersen, Andrea; Pfundt, Rolph; Preikšaitienė, Eglė; Radtke, Kelly; Ranza, Emmanuelle; Rosenfeld, Jill A.; Santiago‐Sim, Teresa; Schwager, Caitlin; Sinnema, Margje; Blok, Lot Snijders; Spillmann, Rebecca C.; Stegmann, Alexander P.A.; Thiffault, Isabelle; Tran, Linh M.; Vaknin‐Dembinsky, Adi; Vedovato-dos-Santos, J.H.; Vergano, Samantha A. Schrier; Vilain, Éric; Vitobello, Antonio; Wagner, Matias; Waheeb, A.; Willing, Marcia; Zuccarelli, Britton; Kini, Usha; Newbury, Dianne F.; Kleefstra, Tjitske; Reymond, Alexandre; Fisher, Simon E.; Vissers, Lisenka E.L.M.

doi:10.1016/j.ajhg.2021.01.007

Cited by 32 publications

(29 citation statements)

References 41 publications

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“…Further complexifying matters: well-defined clinical entities can be caused by mutations in several genes (as it is the case for Noonan syndrome, linked to mutations in 14 different genes) ( 12 ), while mutations occurring in a same gene can result into a wide spectrum of symptoms, as exemplified by MECP2 mutations in Rett syndrome ( 13 ). Adjunctly, different kinds of mutations can result in different pathophysiological mechanisms, as recently exemplified by mutations in SATB1 , in which three different kinds of variants were associated to distinct pathological consequences ( 14 ).…”

Section: Introduction: Heterogeneity Beyond Idiopathic Neurodevelopmental Disordersmentioning

confidence: 99%

Heterogeneity in Fragile X Syndrome Highlights the Need for Precision Medicine-Based Treatments

Verdura¹,

Pérez-Cano²,

Sabido-Vera³

et al. 2021

Front. Psychiatry

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Fragile X syndrome (FXS) is the most frequent monogenic cause of autism or intellectual disability, and research on its pathogenetic mechanisms has provided important insights on this neurodevelopmental condition. Nevertheless, after 30 years of intense research, efforts to develop treatments have been mostly unsuccessful. The aim of this review is to compile evidence from existing research pointing to clinical, genetic, and therapeutic response heterogeneity in FXS and highlight the need of implementing precision medicine-based treatments. We comment on the high genetic and phenotypic heterogeneity present in FXS, as a contributing factor to the difficulties found during drug development. Given that several clinical trials have showed a non-negligeable fraction of positive responders to drugs targeting core FXS symptoms, we propose that success of clinical trials can be achieved by tackling the underlying heterogeneity in FXS by accurately stratifying patients into drug-responder subpopulations. These precision medicine-based approaches, which can be first applied to well-defined monogenic diseases such as FXS, can also serve to define drug responder profiles based on specific biomarkers or phenotypic features that can associate patients with different genetic backgrounds to a same candidate drug, thus repositioning a same drug for a larger number of patients with NDDs.

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Section: Introduction: Heterogeneity Beyond Idiopathic Neurodevelopmental Disordersmentioning

confidence: 99%

Heterogeneity in Fragile X Syndrome Highlights the Need for Precision Medicine-Based Treatments

Verdura¹,

Pérez-Cano²,

Sabido-Vera³

et al. 2021

Front. Psychiatry

View full text Add to dashboard Cite

show abstract

“…In addition, other severe clinical features as spasticity, hypotonia, and epilepsy were significantly more common in patients with missense variants than in patients with PTVs. These observations were confirmed by the authors using a partitioning around medoids clustering algorithm [ 21 ] based on 100 features derived from standardized clinical data: the individuals were clustered into two separate clinical groups, one with PTVs and the other with missense variants [ 7 ]. Computational analysis of facial features also supported the existence of two separate clinical groups: patients with missense variants had a different facial gestalt from individuals carrying PTVs.…”

Section: Resultsmentioning

confidence: 81%

“…As expected, SATB1 and SATB2 patients display very strong overlapping phenotypes. However, subtle differences in the neurological phenotype have been reported: absence of speech and drooling seem to be more common in patients with SATB2 variants, whereas epilepsy seems to be more common in patients with SATB1 variants, especially in patients with missense variants, as previously discussed [ 7 ].…”

Section: Resultsmentioning

confidence: 93%

“…Recently SATB1 disrupting de novo pathogenetic variants has been identified in patients affected by NDD, suggesting a role for this gene also in neurodevelopment [ 1 , 20 ]. Den Hoed and colleagues [ 7 ] have just published a case series of 42 individuals with pathogenetic or likely pathogenetic SATB1 variants. Of these variants, twenty-eight were de novo, three were inherited from an affected parent, two were inherited from unaffected parent (reduced penetrance), five were probably due to parental mosaicism, and for the last four, inheritance could not be established.…”

Section: Resultsmentioning

confidence: 99%

See 1 more Smart Citation

Genotype–Phenotype Correlations in Relation to Newly Emerging Monogenic Forms of Autism Spectrum Disorder and Associated Neurodevelopmental Disorders: The Importance of Phenotype Reevaluation after Pangenomic Results

Lintas

Sacco

Azzarà

et al. 2021

JCM

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ASD genetic diagnosis has dramatically improved due to NGS technologies, and many new causative genes have been discovered. Consequently, new ASD phenotypes have emerged. An extensive exome sequencing study carried out by the Autism Sequencing Consortium (ASC) was published in February 2020. The study identified 102 genes which are de novo mutated in subjects affected by autism spectrum disorder (ASD) or similar neurodevelopmental disorders (NDDs). The majority of these genes was already known to be implicated in ASD or NDDs, whereas approximately 30 genes were considered “novel” as either they were not previously associated with ASD/NDDs or very little information about them was present in the literature. The aim of this work is to review the current literature since the publication of the ASC paper to see if new data mainly concerning genotype–phenotype correlations of the novel genes have been added to the existing one. We found new important clinical and molecular data for 6 of the 30 novel genes. Though the broad and overlapping neurodevelopmental phenotypes observed in most monogenic forms of NDDs make it difficult for the clinical geneticist to address gene-specific tests, knowledge of these new data can at least help to prioritize and interpret results of pangenomic tests to some extent. Indeed, for some of the new emerging genes analyzed in the present work, specific clinical features emerged that may help the clinical geneticist to make the final diagnosis by associating the genetic test results with the phenotype. The importance of this relatively new approach known as “reverse phenotyping” will be discussed.

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“…Repression of BCL11B in SATB2‐positive neurons is an essential mechanism in cortical lamination, resulting in upper‐layer neuron specification (Britanova et al , 2008 ). In humans, YY1 (MIM #617557), SATB1 (MIM # 619228 and #619229), and SATB2 (MIM #612313) are all implicated in neurodevelopmental disorders (Bengani et al , 2017 ; den Hoed et al , 2021 ; Gabriele et al , 2017 ). Notably, SATB2 mutations cause severe language impairments (Zarate & Fish, 2017 ).…”

Section: Foxp2 Transcriptional Regulationmentioning

confidence: 99%

Molecular networks of the FOXP2 transcription factor in the brain

2021

Self Cite

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The discovery of the FOXP2 transcription factor, and its implication in a rare severe human speech and language disorder, has led to two decades of empirical studies focused on uncovering its roles in the brain using a range of in vitro and in vivo methods. Here, we discuss what we have learned about the regulation of FOXP2, its downstream effectors, and its modes of action as a transcription factor in brain development and function, providing an integrated overview of what is currently known about the critical molecular networks.

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Mutation-specific pathophysiological mechanisms define different neurodevelopmental disorders associated with SATB1 dysfunction

Cited by 32 publications

References 41 publications

Heterogeneity in Fragile X Syndrome Highlights the Need for Precision Medicine-Based Treatments

Heterogeneity in Fragile X Syndrome Highlights the Need for Precision Medicine-Based Treatments

Genotype–Phenotype Correlations in Relation to Newly Emerging Monogenic Forms of Autism Spectrum Disorder and Associated Neurodevelopmental Disorders: The Importance of Phenotype Reevaluation after Pangenomic Results

Molecular networks of the FOXP2 transcription factor in the brain

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