Article
Pathology
Akari Iwakoshi, Eiichi Sasaki, Mariko Sato, Keiji Sugiyama, Yoshihito Kogure, Chiyoe Kitagawa, Rieko Nishimura
Summary: This study reports three cases of thoracic undifferentiated tumors with loss of SMARCA2 expression but retained expression of SMARCA4 and SMARCB1. These tumors have similar histological features as SMARCA4-UTs, except for the expression of SMARCA4. This variant may expand the spectrum of SWItch/Sucrose NonFermentable-deficient undifferentiated tumors in the thoracic region.
AMERICAN JOURNAL OF SURGICAL PATHOLOGY
(2022)
Article
Cell Biology
Mahsa S. Ahadi, Talia L. Fuchs, Adele Clarkson, Amy Sheen, Loretta Sioson, Angela Chou, Anthony J. Gill
Summary: Loss of expression of mammalian SWI/SNF complex subunits is rare but enriched in MMRd cases of CRC. This deficiency is associated with higher grade, right-sided location, mismatch repair deficiency, and BRAF V600E mutation, and shows statistically worse overall survival and prognosis.
Review
Pharmacology & Pharmacy
Andrew Hartley, Hing Y. Leung, Imran Ahmad
Summary: This review consolidates current knowledge of the BAF complex in prostate cancer and explores potential therapeutic approaches. Personalized medicine could be used to target mutated BAF complex and exploit synthetic lethal strategies in patient stratification for improved treatment outcomes.
EXPERT OPINION ON DRUG DISCOVERY
(2021)
Article
Genetics & Heredity
Xilian Zhang, Hanjiang Chen, Ying Song, Zhaoyuan Chen, Xuan Liu, Ping Rong, Rong Ma
Summary: Nicolaides-Baraitser syndrome (NCBRS) is a clinical subtype of SWI/SNF-related intellectual disability syndromes with a unique genotype-phenotype correlation. Due to the scarcity of reported cases and limitations in diagnosis methods, the understanding of NCBRS is lagging. This article presents a follow-up of a new patient with NCBRS and summarizes the clinical features and genotype-phenotype correlation of the 80 reported cases. It is believed that the actual number of cases is likely higher than reported due to insufficient studies and lack of attention to the syndrome.
MOLECULAR GENETICS & GENOMIC MEDICINE
(2022)
Article
Oncology
Malin Linden, Christoffer Vannas, Tobias Osterlund, Lisa Andersson, Ayman Osman, Mandy Escobar, Henrik Fagman, Anders Stahlberg, Pierre Aman
Summary: FET fusion oncoproteins bind with SWI/SNF complexes and indirectly interact with BRD4, co-localizing on chromatin and interacting with transcription factors and RNA Polymerase II.
MOLECULAR ONCOLOGY
(2022)
Article
Public, Environmental & Occupational Health
Shanshan Sun, Qiujing Li, Zhenkun Zhang, Sili Xiong, Yujie Zhang, Qian Liu, Zhe Li, Fujun Yang, Shukun Zhang
Summary: SMARCA2-negative expression is an independent predictor of a poor outcome of NSCLC and a potential target for NSCLC treatment.
ENVIRONMENTAL HEALTH AND PREVENTIVE MEDICINE
(2022)
Article
Chemistry, Medicinal
Sandra C. Ordonez-Rubiano, Chad A. Maschinot, Sijie Wang, Surbhi Sood, Luisa F. Baracaldo-Lancheros, Brayden P. Strohmier, Alexander J. McQuade, Brian C. Smith, Emily C. Dykhuizen
Summary: The researchers discovered the important role of BRD7 in cancer but lacked selective chemical probes to study its function in disease. Through crystal structure analysis, they identified a specific binding pocket exclusive to BRD7. They designed a series of ligands and identified two inhibitors, 1-78 and 2-77, with increased selectivity towards BRD7, which showed submicromolar affinity to the BRD7 bromodomain. Finally, they validated the utility and selectivity of these compounds in cell-based models of prostate cancer.
JOURNAL OF MEDICINAL CHEMISTRY
(2023)
Article
Cell Biology
Saul Carcamo, Christie B. Nguyen, Elena Grossi, Dan Filipescu, Aktan Alpsoy, Alisha Dhiman, Dan Sun, Sonali Narang, Jochen Imig, Tiphaine C. Martin, Ramon Parsons, Iannis Aifantis, Aristotelis Tsirigos, Julio A. Aguirre-Ghiso, Emily C. Dykhuizen, Dan Hasson, Emily Bernstein
Summary: ARID2 is the most commonly mutated member of the SWI/SNF complex in melanoma. Its deficiency leads to defective assembly of the PBAF complex and redistribution of the BAF complex. ARID2 depletion results in reduced chromatin accessibility and gene expression in certain regions, while enhancers occupied by the BAF complex gain accessibility and gene expression related to invasion. The occupancy of melanoma-relevant transcription factors is affected by altered accessibility, and correlates significantly with the observed transcriptional changes. Furthermore, ARID2-deficient cells acquire the ability to colonize distal organs in multiple animal models.
Article
Multidisciplinary Sciences
Young-Kwon Park, Ji-Eun Lee, Zhijiang Yan, Kaitlin McKernan, Tommy O'Haren, Weidong Wang, Weiqun Peng, Kai Ge
Summary: The study reveals that BAF and MLL4 are interdependent in promoting enhancer activation by lineage-determining transcription factors during adipogenesis, providing a positive feedback mechanism for the activation of cell type-specific enhancers.
NATURE COMMUNICATIONS
(2021)
Article
Biochemistry & Molecular Biology
Lena Wischhof, Hang-Mao Lee, Janine Tutas, Clemens Overkott, Eileen Tedt, Miriam Stork, Michael Peitz, Oliver Bruestle, Thomas Ulas, Kristian Haendler, Joachim L. Schultze, Dan Ehninger, Pierluigi Nicotera, Paolo Salomoni, Daniele Bano
Summary: Mammalian SWI/SNF/BAF chromatin remodeling complexes, particularly the modulator BCL7A, play crucial roles in regulating Notch/Wnt pathway signaling and mitochondrial bioenergetics during neuronal progenitor cell differentiation, ultimately affecting neuronal morphogenesis, cognitive flexibility, and behavioral performance.
Article
Oncology
Theresa Bluemn, Jesse Schmitz, Yongwei Zheng, Robert Burns, Shikan Zheng, Joshua DeJong, Luke Christiansen, Olivia Arnold, Jesus Izaguirre-Carbonell, Demin Wang, Aniruddha J. Deshpande, Nan Zhu
Summary: The SWI/SNF nucleosome remodeling complexes have diverse roles in AML leukemogenesis, with Arid2 enhancing leukemia initiation but being required for leukemia maintenance, while the deletion of Arid1b promotes leukemogenesis at any stage.
Article
Oncology
Masayuki Hagiwara, Yota Yasumizu, Nami Yamashita, Hasan Rajabi, Atsushi Fushimi, Mark D. Long, Wei Li, Atrayee Bhattacharya, Rehan Ahmad, Mototsugu Oya, Song Liu, Donald Kufe
Summary: MUC1-C associates with E2F1 and activates a novel pathway related to prostate cancer stem cell function.
Review
Cell Biology
Ying Ye, Xi Chen, Wensheng Zhang
Summary: Embryonic stem cells have a unique ability to maintain and regulate the balance between self-renewal and multi-lineage cellular differentiation, largely dependent on gene expression regulations. Chromatin remodeling complexes play a crucial role in promoting chromatin structural changes that ultimately affect ESC fate choices.
FRONTIERS IN CELL AND DEVELOPMENTAL BIOLOGY
(2021)
Review
Genetics & Heredity
Lili Yang, Xiaoli Shu, Shujiong Mao, Yi Wang, Xiaonan Du, Chaochun Zou
Summary: Angelman syndrome is a rare neurodevelopmental disease caused by the loss of function of the maternal copy of UBE3A. It is characterized by developmental delay, intellectual disability, lack of speech, and ataxia. Different genetic types may show different phenotypes, and understanding genotype-phenotype correlations can lead to individualized treatment options.
Article
Biochemistry & Molecular Biology
Liselot van der Laan, Kathleen Rooney, Marielle Alders, Raissa Relator, Haley McConkey, Jennifer Kerkhof, Michael A. Levy, Peter Lauffer, Mio Aerden, Miel Theunis, Eric Legius, Matthew L. Tedder, Lisenka E. L. M. Vissers, Saskia Koene, Claudia Ruivenkamp, Mariette J. Hoffer, Dagmar Wieczorek, Nuria C. Bramswig, Theresia Herget, Vanesa Lopez Gonzalez, Fernando Santos-Simarro, Pernille M. Torring, Anne-Sophie Denomme-Pichon, Bertrand Isidor, Boris Keren, Sophie Julia, Elise Schaefer, Christine Francannet, Pierre-Yves Maillard, Mala Misra-Isrie, Hilde Van Esch, Marcel M. A. M. Mannens, Bekim Sadikovic, Mieke M. van Haelst, Peter Henneman
Summary: Clark-Baraitser syndrome is a rare intellectual disability syndrome caused by pathogenic variants in the TRIP12 gene. DNA methylation episignature analysis can help diagnose and identify pathogenic TRIP12 variants.
INTERNATIONAL JOURNAL OF MOLECULAR SCIENCES
(2022)
Article
Genetics & Heredity
Marion Aubert-Mucca, Celine Huber, Genevieve Baujat, Caroline Michot, Mohammed Zarhrate, Marc Bras, Lucile Boutaud, Valerie Malan, Tania Attie-Bitach, Valerie Cormier-Daire
Summary: We analyzed 50 clinically identified EVC cases from 45 families to further understand the EVC phenotype and its molecular basis. Our study confirmed the major role of EVC and EVC2 genes in EVC syndrome and identified previously unreported copy number variations. We also found a high proportion of heterozygous deletions in EVC/EVC2, mostly inherited from the mother, possibly resulting from recombinations involving Alu sequences.
JOURNAL OF MEDICAL GENETICS
(2023)
Article
Pediatrics
Lucia Micale, Federica Russo, Martina Mascaro, Silvia Morlino, Grazia Nardella, Carmela Fusco, Luigi Bisceglia, Germana Meroni, Marco Castori
Summary: This study investigated the functional effects of intronic variants in the MID1 gene on splicing using a minigene assay. The results demonstrated the potential pathogenicity of these variants and suggested the introduction of similar second-tier investigations in the molecular diagnostics workflow of Opitz syndrome. This study highlights the importance of minigene assays in supporting the clinical interpretation of intronic variants.
PEDIATRIC RESEARCH
(2023)
Article
Genetics & Heredity
Lottie D. Morison, Elisabeth Meffert, Miriam Stampfer, Irene Steiner-Wilke, Brigitte Vollmer, Katrin Schulze, Tracy Briggs, Ruth Braden, Adam Vogel, Daisy Thompson-Lake, Chirag Patel, Edward Blair, Himanshu Goel, Samantha Turner, Ute Moog, Angelika Riess, Frederique Liegeois, David A. Koolen, David J. Amor, Tjitske Kleefstra, Simon E. Fisher, Christiane Zweier, Angela T. Morgan
Summary: Disruptions of FOXP2 can cause severe speech disorder known as childhood apraxia of speech (CAS). This study examined individuals with pathogenic FOXP2-only variants and found that speech disorders, including CAS, were prevalent in these cases. Other comorbidities such as feeding difficulties, motor impairment, anxiety, depression, and sleep disturbance were also observed. The study emphasizes the importance of FOXP2 in understanding the neurobiological basis of speech disorder.
JOURNAL OF MEDICAL GENETICS
(2023)
Article
Genetics & Heredity
Heba Morsy, Mehdi Benkirane, Elisa Cali, Clarissa Rocca, Kristina Zhelcheska, Valentina Cipriani, Evangelia Galanaki, Reza Maroofian, Stephanie Efthymiou, David Murphy, Mary O'Driscoll, Mohnish Suri, Siddharth Banka, Jill Clayton-Smith, Thomas Wright, Melody Redman, Jennifer A. Bassetti, Mathilde Nizon, Benjamin Cogne, Rami Abu Jamra, Tobias Bartolomaeus, Marion Heruth, Ilona Krey, Janina Gburek-Augustat, Dagmar Wieczorek, Felix Gattermann, Meriel Mcentagart, Alice Goldenberg, Lucie Guyant-Marechal, Hector Garcia-Moreno, Paola Giunti, Brigitte Chabrol, Severine Bacrot, Roger Buissonniere, Virginie Magry, Vykuntaraju K. Gowda, Varunvenkat M. Srinivasan, Bela Melegh, Andras Szabo, Katalin Sumegi, Mireille Cossee, Monica Ziff, Russell Butterfield, David Hunt, Georgina Bird-Lieberman, Michael Hanna, Michel Koenig, Michael Stankewich, Jana Vandrovcova, Henry Houlden
Summary: The purpose of this study was to understand the phenotypic spectrum of SPTAN1 variants. It was found that SPTAN1 variants were significantly enriched in families with hereditary ataxia or hereditary spastic paraplegia. A total of 31 individuals with SPTAN1 variants were identified, with 10 patients presenting with pure or complex HSP/HA and the remaining 21 patients having developmental delay and seizures. Fibroblasts derived from two patients showed irregular alpha II-spectrin aggregation.
GENETICS IN MEDICINE
(2023)
Article
Obstetrics & Gynecology
Olga Tsuiko, Yasmine El Ayeb, Tatjana Jatsenko, Joke Allemeersch, Cindy Melotte, Jia Ding, Sophie Debrock, Karen Peeraer, Arne Vanhie, Anne De Leener, Celine Pirard, Candice Kluyskens, Ellen Denayer, Eric Legius, Joris Robert Vermeesch, Hilde Brems, Eftychia Dimitriadou
Summary: Long-read amplicon sequencing is a simple and cost-effective strategy for preclinical preimplantation genetic testing in couples with a de novo pathogenic variant. This approach allows for the identification of the parental origin of the mutant allele and provides access to universal genome-wide haplotyping-based PGT programs. The success rate of this method is 75%.
HUMAN REPRODUCTION
(2023)
Article
Biochemistry & Molecular Biology
Naci Senkal, Istemi Serin, Sacide Pehlivan, Mustafa Pehlivan, Alpay Medetalibeyoglu, Timurhan Cebeci, Hilal Konyaoglu, Yasemin Oyaci, Gozde Yesil Sayin, Ummuhan Isoglu-Alkac, Tufan Tukek, Murat Kose
Summary: Oxidative stress and DNA damage caused by Coronavirus disease 2019 (COVID-19) were evaluated in a Turkish population. DNA repair gene variants (XRCC4 rs28360071, rs6869366, and XRCC1 rs25487) were found to be associated with COVID-19 susceptibility and clinical course. XRCC4 rs6869366 G/G genotype and G allele frequency were increased in patients compared to controls, while XRCC4 rs6869366 G/T and T/T genotypes were more common in controls. The A/A and A/G genotypes of XRCC1 rs25487 were significantly associated with COVID-19 disease. The study highlights the importance of DNA repair gene variants in COVID-19 susceptibility.
NUCLEOSIDES NUCLEOTIDES & NUCLEIC ACIDS
(2023)
Article
Cell Biology
Antje Kampmeier, Elsa Leitao, Ilaria Parenti, Jasmin Beygo, Christel Depienne, Nuria C. Bramswig, Tzung-Chien Hsieh, Alexandra Afenjar, Stefanie Beck-Woedl, Ute Grasshoff, Tobias B. Haack, Emilia K. Bijlsma, Claudia Ruivenkamp, Eva Lausberg, Miriam Elbracht, Maria K. Haanpaa, Hannele Koillinen, Uwe Heinrich, Imma Rost, Rami Abou Jamra, Denny Popp, Margarete Koch-Hogrebe, Kevin Rostasy, Vanesa Lopez-Gonzalez, Maria Jose Sanchez-Soler, Catarina Macedo, Ariane Schmetz, Carmen Steinborn, Sabine Weidensee, Hellen Lesmann, Felix Marbach, Pilar Caro, Christian P. Schaaf, Peter Krawitz, Dagmar Wieczorek, Frank J. Kaiser, Alma Kuechler
Summary: In 2016 and 2018, a new syndrome called Chung-Jansen syndrome caused by haploinsufficiency of PHIP was described. This syndrome is characterized by developmental delay, learning difficulties/intellectual disability, behavioral abnormalities, facial dysmorphism and obesity. The identification of distinct types of PHIP alterations using omics technologies has expanded the mutational and clinical spectrum of CHUJANS.
FRONTIERS IN CELL AND DEVELOPMENTAL BIOLOGY
(2023)
Article
Neurosciences
Emrah Yucesan, Beyza Goncu, Cemil Ozgul, Arda Kebapci, Ayca Dilruba Aslanger, Enes Akyuz, Gozde Yesil
Summary: This study investigates the effects of KCNMA1 gene mutation on the function of calcium-activated potassium channels. Experimental results from two independent approaches show that the mutation leads to loss of function in the channel. The findings suggest that genes associated with channelopathies may have dual effects of both loss and gain of function.
INTERNATIONAL JOURNAL OF NEUROSCIENCE
(2023)
Article
Biochemistry & Molecular Biology
Jhih-Rong Lin, Yingjie Zhao, M. Reza Jabalameli, Nha Nguyen, Joydeep Mitra, Ann Swillen, Jacob A. S. Vorstman, Eva W. C. Chow, Marianne van den Bree, Beverly S. Emanuel, Joris R. Vermeesch, Michael J. Owen, Nigel M. Williams, Anne S. Bassett, Donna M. McDonald-McGinn, Raquel E. Gur, Carrie E. Bearden, Bernice E. Morrow, Herbert M. Lachman, Zhengdong D. Zhang
Summary: 22q11.2 deletion is a strong genetic risk factor for schizophrenia. Whole-genome sequencing of schizophrenia cases and controls with this deletion revealed the effects of rare coding variants in modifier genes, contributing to the pathogenesis of schizophrenia. The modifier genes affected synaptic function and developmental disorders and were coexpressed with 22q11.2 genes in specific brain regions.
MOLECULAR PSYCHIATRY
(2023)
Editorial Material
Genetics & Heredity
Lisa Hui, Katie Ellis, Dora Mayen, Mark D. D. Pertile, Rebecca Reimers, Luming Sun, Joris Vermeesch, Neeta L. L. Vora, Lyn S. S. Chitty, SPD Board of Directors
PRENATAL DIAGNOSIS
(2023)
Article
Genetics & Heredity
Ariane Schmetz, Joerg Schaper, Simon Thelen, Majeed Rana, Thomas Klenzner, Katharina Schaumann, Jasmin Beygo, Harald Surowy, Hermann-Josef Luedecke, Dagmar Wieczorek
Summary: Multiple synostoses syndrome (MSS) is a group of genetically heterogeneous autosomal dominant diseases characterized by abnormal bone unions. Pathogenic variants in FGF9 have been associated with MSS type 3 (SYNS3), with only five different missense variants reported so far. In this report, a large multigenerational family with a novel missense variant in FGF9 is described, expanding the phenotypic spectrum of SYNS3 to include cleft palate and conductive hearing loss, with emphasis on the high degree of intrafamilial phenotypic variability.
Article
Genetics & Heredity
Cosima M. Schmid, Anne Gregor, Gregory Costain, Chantal F. Morel, Lauren Massingham, Jennifer Schwab, Chloe Quelin, Marie Faoucher, Julie Kaplan, Rebecca Procopio, Carol J. Saunders, Ana S. A. Cohen, Gabrielle Lemire, Stephanie Sacharow, Anne O'Donnell-Luria, Ranit Jaron Segal, Jessica Kianmahd Shamshoni, Daniela Schweitzer, Darius Ebrahimi-Fakhari, Kristin Monaghan, Timothy Blake Palculict, Melanie P. Napier, Alice Tao, Bertrand Isidor, Kamran Moradkhani, Andre Reis, Heinrich Sticht, Wendy K. Chung, Christiane Zweier
Summary: Through international collaboration, we identified individuals carrying small chromosomal deletions, gene-disrupting or missense variants in LHX2, and they presented with neurodevelopmental phenotypes. Our findings implicate LHX2 haploinsufficiency as causative for neurodevelopmental disorders.
GENETICS IN MEDICINE
(2023)
Article
Biochemistry & Molecular Biology
Marie De Borre, Huiwen Che, Qian Yu, Lore Lannoo, Kobe De Ridder, Leen Vancoillie, Pauline Dreesen, Mika Van Den Ackerveken, Mio Aerden, Eva Galle, Jeroen Breckpot, Joachim Van Keirsbilck, Wilfried Gyselaers, Koen Devriendt, Joris Robert Vermeesch, Kristel Van Calsteren, Bernard Thienpont
Summary: By profiling the cell-free DNA methylation of plasma, it is possible to identify the risk of preeclampsia in early pregnancy, providing guidance for prevention and treatment.
Article
Genetics & Heredity
Lore Lannoo, Joke Van Camp, Nathalie Brison, Ilse Parijs, Leen Vancoillie, Kris van den Bogaert, Joris Robert Vermeesch, Koen Devriendt, Kristel Van Calsteren
Summary: This study assessed the maternal characteristics and comorbidities in patients with persistent uninterpretable non-invasive prenatal testing (NIPT) and evaluated the association with adverse pregnancy outcomes. The findings showed that patients with persistent uninterpretable NIPT were more likely to have obesity, multiple pregnancies, and obstetric complications, and had a higher incidence of adverse pregnancy outcomes compared to the general population.
PRENATAL DIAGNOSIS
(2023)
Article
Medicine, Research & Experimental
Charlotte Gehin, Museer A. Lone, Winston Lee, Laura Capolupo, Sylvia Ho, Adekemi M. Adeyemi, Erica H. Gerkes, Alexander P. A. Stegmann, Estrella Lopez-Martin, Eva Bermejo-Sanchez, Beatriz Martinez-Delgado, Christiane Zweier, Cornelia Kraus, Bernt Popp, Vincent Strehlow, Daniel Graefe, Ina Knerr, Eppie R. Jones, Stefano Zamuner, Luciano A. Abriata, Vidya Kunnathully, Brandon E. Moeller, Anthony Vocat, Samuel Rommelaere, Jean-Philippe Bocquete, Evelyne Ruchti, Greta Limoni, Marine Van Campenhoudt, Samuel Bourgeat, Petra Henklein, Christian Gilissen, Bregje W. van Bon, Rolph Pfundt, Marjolein H. Willemsen, Jolanda H. Schieving, Emanuela Leonardi, Fiorenza Soli, Alessandra Murgia, Hui Guo, Qiumeng Zhang, Kun Xia, Christina R. Fagerberg, Christoph P. Beier, Martin J. Larsen, Irene Valenzuela, Paula Fernandez-alvarez, Shiyi Xiong, Robert Smigiel, Vanesa Lopez-Gonzalez, Lluis Armengol, Manuela Morleo, Angelo Selicorni, Annalaura Torella, Moira Blyth, Nicola S. Cooper, Valerie Wilson, Renske Oegema, Yvan Herenger, Aurore Garde, Ange-Line Bruel, Frederic Tran Mau-Them, Alexis B. R. Maddocks, Jennifer M. Bain, Musadiq A. Bhat, Gregory Costain, Peter Kannu, Ashish Marwaha, Neena L. Champaigne, Michael J. Friez, Ellen B. Richardson, Vykuntaraju K. Gowda, Varunvenkat M. Srinivasan, Yask Gupta, Tze Y. Lim, Simone Sanna-Cherchi, Bruno Lemaitre, Toshiyuki Yamaji, Kentaro Hanada, John E. Burke, Ana Marjia Jaksic, Brian D. McCabe, Paolo De Los Rios, Thorsten Hornemann, Giovanni D'Angelo, Vincenzo A. Gennarino
Summary: By studying individuals with de novo missense variants in CERT1, it was found that CERT autoregulation plays a central role in the control of sphingolipid biosynthetic flux. Inhibiting CERT pharmacologically can correct the morphological and motor abnormalities in CerTra syndrome, suggesting a potential therapeutic approach for patients.
JOURNAL OF CLINICAL INVESTIGATION
(2023)
