Article
Neurosciences
Rachel M. Rahn, Allen Yen, Siyu Chen, Seana H. Gaines, Annie R. Bice, Lindsey M. Brier, Raylynn G. Swift, LeiLani Lee, Susan E. Maloney, Joseph P. Culver, Joseph D. Dougherty
Summary: In this study, widefield optical fluorescence imaging was used to evaluate calcium functional connectivity (FC) in the brain of the Mecp2 mutant mouse model. Results showed disrupted FC between cortical regions in Mecp2 mutant males during both juvenile development and early adulthood. Female Mecp2 mice exhibited increased contralateral FC in the motor cortex at P35, while more posterior parietal regions were implicated in adulthood. The amplitude of connection strength was increased in the male cortex, with more positive correlations and negative anticorrelations. Restoring MeCP2 protein in GABAergic neurons did not rescue these functional deficits or increase male lifespan.
Article
Clinical Neurology
Johanna Maeder, Valentina Mancini, Corrado Sandini, Fiona Journal, Maude Schneider, Matthias Kliegel, Stephan Eliez
Summary: This study extends the current knowledge on the effects of MPH in patients with 22q11DS. Treatment was found to be effective for core ADHD symptoms and cognitive measures of attention and inhibition. However, no significant improvement was found for other executive functions, learning, or memory. The side effects were frequent but mild in intensity.
INTERNATIONAL JOURNAL OF NEUROPSYCHOPHARMACOLOGY
(2022)
Article
Psychiatry
Caren Latreche, Johanna Maeder, Valentina Mancini, Maude Schneider, Stephan Eliez
Summary: This study is the first double-blind study aimed at investigating the potential neuroprotective effect of antipsychotics in individuals with 22q11DS at risk for psychosis. The results indicate short-term improvements in SIPS items and reliable enhancements in working memory and attention measures for treated participants.
FRONTIERS IN PSYCHIATRY
(2022)
Article
Genetics & Heredity
Erica Soster, Brittany Dyr, Jill Rafalko, Eyad Almasri, Phillip Cacheris
Summary: Non-invasive prenatal screening (NIPS) using cell-free DNA (cfDNA) from maternal plasma can detect fetal chromosome disorders, including 22q11.2 deletion syndrome (22q11.2DS). However, prenatal screening for 22q11.2DS faces challenges such as varying deletion sizes/locations, maternal 22q11.2 deletions, and confirmatory test choice.
FRONTIERS IN GENETICS
(2023)
Article
Genetics & Heredity
Ewelina Wolanska, Agnieszka Pollak, Malgorzata Rydzanicz, Karolina Pesz, Magdalena Klaniewska, Anna Rozensztrauch, Pawel Skiba, Piotr Stawinski, Rafal Ploski, Robert Smigiel
Summary: The main symptoms of dysmorphic syndrome associated with intergenic deletion in the Xq24 chromosome region include psychomotor delay, hypotonia, and intellectual disability, as well as heart defects, urogenital malformations, and characteristic cranio-facial dysmorphism. Limited information is available in the literature regarding the symptoms and clinical course of the Xq24 deletion, and a case of a nine-year-old boy with this deletion involving the UBE2A and CXorf56 genes was presented in this report. The deletion of 35kb in the Xq24 region, including the UBE2A and CXorf56 genes, was revealed through array comparative genomic hybridization (array-CGH) and whole exome sequencing (WES) tests.
Article
Medicine, General & Internal
Guoming Chu, Pingping Li, Juan Wen, Gaoyan Zheng, Yanyan Zhao, Rong He
Summary: This study aimed to investigate the genotype-phenotype correlation of 5p deletion syndrome and redefine the relevant regions. Through studying three families and two children, different sizes of 5p deletions were detected and their pathogenicity was determined. Additionally, the potential of whole genome sequencing in identifying chromosomal breakpoints in prenatal diagnosis was demonstrated.
FRONTIERS IN MEDICINE
(2022)
Article
Virology
Hussein M. Abkallo, Johanneke D. Hemmink, Bernard Oduor, Emmanuel M. Khazalwa, Nicholas Svitek, Nacyra Assad-Garcia, Jeremiah Khayumbi, Walter Fuchs, Sanjay Vashee, Lucilla Steinaa
Summary: This study reports the effects of gene deletions on pig herds caused by African swine fever virus. Single deletion of the A238L gene did not result in complete attenuation, but the double deletions of A238L and EP402R genes improved safety and provided partial protection against challenge with the wildtype ASFV virus.
Article
Orthopedics
Juyi Li, Xiaofang Liang, Xiufang Wang, Pei Yang, Xiaofei Jian, Lei Fu, Aiping Deng, Chao Liu, Jianxin Liu
Summary: A Chinese family with brachydactyly type A1 (BDA1) and multiple-synostoses syndrome 2 (SYNS2) was found to have a genetic variant (S475N) in the GDF5 gene, which disrupts the formation of salt bridges and impairs protein function, leading to abnormalities in cartilage and bone development.
Article
Genetics & Heredity
Tracy Heung, Brigid Conroy, Sarah Malecki, Joanne Ha, Erik Boot, Maria Corral, Anne S. Bassett
Summary: 22q11.2 deletion syndrome affects final adult height distribution, with around 22.7% of patients having short stature, a significantly higher rate than expected in the general population. Factors such as moderate-to-severe intellectual disability, major congenital heart disease, and the common LCR22A-LCR22D (A-D) deletion are independent risk factors for short stature.
Article
Multidisciplinary Sciences
Pui Wang, Siu-Ying Lau, Shaofeng Deng, Pin Chen, Bobo Wing-Yee Mok, Anna Jinxia Zhang, Andrew Chak-Yiu Lee, Kwok-Hung Chan, Rachel Chun-Yee Tam, Haoran Xu, Runhong Zhou, Wenjun Song, Li Liu, Kelvin Kai-Wang To, Jasper Fuk-Woo Chan, Zhiwei Chen, Kwok-Yung Yuen, Honglin Chen
Summary: The study demonstrates that the cell-adapted SARS-CoV-2 variant Ca-DelMut replicates more efficiently than the wild-type virus and induces a strong neutralizing antibody and T cell response in hamsters, while causing no apparent pathological changes. Animals immunized with Ca-DelMut are fully protected with sterilizing immunity against subsequent wild-type SARS-CoV-2 challenge.
NATURE COMMUNICATIONS
(2021)
Article
Multidisciplinary Sciences
Julia Kolle, Theodor Zimmermann, Alexander Kiefer, Ralf J. Rieker, Paraskevi Xepapadaki, Sebastian Zundler, Nikolaos G. Papadopoulos, Susetta Finotto
Summary: The study found that increased IL-3 secretion in PBMCs of asthmatic children was directly related to improved lung function. IL-3(-/-) asthmatic mice exhibited increased asthmatic traits. Additionally, IL-3-deficient mice had a defect in T regulatory cells in the lung.
Article
Endocrinology & Metabolism
Han-Yi Lin, Wen-Yu Tsai, Yi-Ching Tung, Shih-Yao Liu, Ni-Chung Lee, Yin-Hsiu Chien, Wuh-Liang Hwu, Cheng-Ting Lee
Summary: This study aimed to investigate the clinical manifestations of endocrine disorders in Taiwanese patients with 22q11.2 deletion syndrome (22q11.2DS). The results showed that hypoparathyroidism is a common endocrine disorder in these patients, and it is important to assess parathyroid function to prevent symptomatic hypocalcemia. Although thyroid disorders are less common, screening for thyroid dysfunction is justified in these patients. Additionally, patients with 22q11.2DS exhibit a delayed growth pattern, and regular monitoring of growth is recommended.
FRONTIERS IN ENDOCRINOLOGY
(2022)
Article
Biochemistry & Molecular Biology
Kathleen Rooney, Michael A. Levy, Sadegheh Haghshenas, Jennifer Kerkhof, Daniela Rogaia, Maria Giovanna Tedesco, Valentina Imperatore, Amedea Mencarelli, Gabriella Maria Squeo, Eleonora Di Venere, Giuseppe Di Cara, Alberto Verrotti, Giuseppe Merla, Matthew L. Tedder, Barbara R. DuPont, Bekim Sadikovic, Paolo Prontera
Summary: 22q11.2 deletion syndrome is the most common genomic disorder caused by a recurrent deletion, presenting with various syndromes. A unique episignature was identified in typical and proximal 22q11.2DS, serving as an effective tool for molecular diagnosis of this disorder.
INTERNATIONAL JOURNAL OF MOLECULAR SCIENCES
(2021)
Article
Dermatology
Janan Mohamad, Ofer Sarig, Paula Beattie, Kiril Malovitski, Sari Assaf, Edel O'Toole, Janice Schwartz, Holly Evans, Liat Samuelov, Eli Sprecher
Summary: This study reports on a novel clinical phenotype resulting from germline mosaicism for a large genomic deletion spanning six keratin genes. The genomic variant leads to a truncated form of keratin 17, which disrupts keratinocyte cell cytoskeleton formation in vitro.
BRITISH JOURNAL OF DERMATOLOGY
(2022)
Article
Oncology
Elizabeth K. Bancroft, Elizabeth C. Page, Mark N. Brook, Sarah Thomas, Natalie Taylor, Jennifer Pope, Jana McHugh, Ann-Britt Jones, Questa Karlsson, Susan Merson, Kai Ren Ong, Jonathan Hoffman, Camilla Huber, Lovise Maehle, Eli Marie Grindedal, Astrid Stormorken, D. Gareth Evans, Jeanette Rothwell, Fiona Lalloo, Angela F. Brady, Marion Bartlett, Katie Snape, Helen Hanson, Paul James, Joanne McKinley, Lyon Mascarenhas, Sapna Syngal, Chinedu Ukaegbu, Lucy Side, Tessy Thomas, Julian Barwell, Manuel R. Teixeira, Louise Izatt, Mohnish Suri, Finlay A. Macrae, Nicola Poplawski, Rakefet Chen-Shtoyerman, Munaza Ahmed, Hannah Musgrave, Nicola Nicolai, Lynn Greenhalgh, Carole Brewer, Nicholas Pachter, Allan D. Spigelman, Ashraf Azzabi, Brian T. Helfand, Dorothy Halliday, Saundra Buys, Teresa Ramon Y. Cajal, Alan Donaldson, Kathleen A. Cooney, Marion Harris, John McGrath, Rosemarie Davidson, Amy Taylor, Peter Cooke, Kathryn Myhill, Matthew Hogben, Neil K. Aaronson, Audrey Ardern-Jones, Chris H. Bangma, Elena Castro, David Dearnaley, Alexander Dias, Tim Dudderidge, Diana M. Eccles, Kate Green, Jorunn Eyfjord, Alison Falconer, Christopher S. Foster, Henrik Gronberg, Freddie C. Hamdy, Oskar Johannsson, Vincent Khoo, Hans Lilja, Geoffrey J. Lindeman, Jan Lubinski, Karol Axcrona, Christos Mikropoulos, Anita Mitra, Clare Moynihan, Holly Ni Raghallaigh, Gad Rennert, Rebecca Collier, Judith Offman, Zsofia Kote-Jarai, Rosalind A. Eeles
Summary: The IMPACT study found that men carrying pathogenic variants in the MLH1, MSH2, and MSH6 genes had a significantly higher incidence of prostate cancer after the first round of PSA screening, supporting the use of targeted PSA screening in these men to identify clinically significant prostate cancer.
Article
Biochemistry & Molecular Biology
Marie Cade, Javier Munoz-Garcia, Antoine Babuty, Louis Pare, Denis Cochonneau, Karim Fekir, Mathias Chatelais, Marie-Francoise Heymann, Anna Lokajczyk, Catherine Boisson-Vidal, Dominique Heymann
Summary: This study discovered that recombinant human FVIII has direct biological activities on endothelial cells, including decreased cell adhesion, regulation of transcriptomic and protein profiles, increased vascular permeability, and enhanced monocyte adhesion. The findings highlight new functions of FVIII in regulating vascular permeability and leukocyte adhesion and migration.
CELLULAR AND MOLECULAR LIFE SCIENCES
(2022)
Article
Oncology
Borja Ruiz-Fernandez de Cordoba, Haritz Moreno, Karmele Valencia, Naiara Perurena, Pablo Ruedas, Thomas Walle, Alberto Pezonaga-Torres, Juan Hinojosa, Elisabet Guruceaga, Antonio Pineda-Lucena, Marta Abengozar-Muela, Denis Cochonneau, Carolina Zandueta, Susana Martinez-Canarias, Alvaro Teijeira, Daniel Ajona, Sergio Ortiz-Espinosa, Xabier Morales, Carlos Ortiz de Solorzano, Marta Santisteban, Luis Ramos-Garcia, Laura Guembe, Vratislav Strnad, Dominique Heymann, Sandra Hervas-Stubbs, Ruben Pio, Maria E. Rodriguez-Ruiz, Carlos E. de Andrea, Silvestre Vicent, Ignacio Melero, Fernando Lecanda, Rafael Martinez-Monge
Summary: Locoregional failure in breast cancer patients after surgery and irradiation is linked to a poor prognosis. The ENPP1/HP axis is exploited by tumor cells to promote local recurrence by suppressing immune cells. Blocking this axis offers new opportunities for therapeutic intervention.
Review
Genetics & Heredity
Clemence Jacquin, Emilie Landais, Celine Poirsier, Alexandra Afenjar, Ahmad Akhavi, Nathalie Bednarek, Caroline Benech, Adeline Bonnard, Damien Bosquet, Lydie Burglen, Patrick Callier, Sandra Chantot-Bastaraud, Christine Coubes, Charles Coutton, Bruno Delobel, Margaux Descharmes, Jean-Michel Dupont, Vincent Gatinois, Nicolas Gruchy, Sarah Guterman, Abdelkader Heddar, Lucas Herissant, Delphine Heron, Bertrand Isidor, Pauline Jaeger, Guillaume Jouret, Boris Keren, Paul Kuentz, Cedric Le Caignec, Jonathan Levy, Nathalie Lopez, Zoe Manssens, Dominique Martin-Coignard, Isabelle Marey, Cyril Mignot, Chantal Missirian, Celine Pebrel-Richard, Lucile Pinson, Jacques Puechberty, Sylvia Redon, Damien Sanlaville, Marta Spodenkiewicz, Anne-Claude Tabet, Alain Verloes, Gaelle Vieville, Catherine Yardin, Francois Vialard, Martine Doco-Fenzy
Summary: Chromosome 1p36 deletion syndrome is a common terminal deletion syndrome characterized by craniofacial features, developmental delay, hypotonia, epilepsy, and cardiac abnormalities. This study aims to evaluate the incidence of 1p36DS in the French population and compare it with other genetic syndromes, as well as refine the phenotype and improve patient management through genotype-phenotype correlation.
AMERICAN JOURNAL OF MEDICAL GENETICS PART A
(2023)
Article
Biochemistry & Molecular Biology
Philippine Garret, Martin Chevarin, Antonio Vitobello, Simon Verdez, Cyril Fournier, Alain Verloes, Emilie Tisserant, Pierre Vabres, Orlane Prevel, Christophe Philippe, Anne-Sophie Denomme-Pichon, Ange-Line Bruel, Frederic Tran Mau-Them, Hana Safraou, Aicha Boughalem, Jean-Marc Costa, Detlef Trost, Christel Thauvin-Robinet, Laurence Faivre, Yannis Duffourd
Summary: This study identified two de novo mobile element insertions (MEIs) in patients with developmental and neurological abnormalities, highlighting the importance of incorporating ME detection in exome sequencing for improved diagnostic rate.
EUROPEAN JOURNAL OF HUMAN GENETICS
(2023)
Article
Biochemistry & Molecular Biology
Ella Vintschger, Dennis Kraemer, Pascal Joset, Anselm H. C. Horn, Anita Rauch, Heinrich Sticht, Ruxandra Bachmann-Gagescu
Summary: Next generation sequencing (NGS) is used to detect carrier status for rare recessive disorders. The recent ACMG recommendations support NGS-based carrier screening (NGS-CS) for genes with a carrier frequency > 1/200. However, variant interpretation in healthy individuals presents challenges, and the true carrier frequencies are uncertain. Thus, genetic counseling for NGS-CS should disclose these limitations.
EUROPEAN JOURNAL OF HUMAN GENETICS
(2023)
Article
Genetics & Heredity
Tanja Frey, Ivan Ivanovski, Angela Bahr, Markus Zweier, Julia Laube, Isabelle Luchsinger, Katharina Steindl, Anita Rauch
Summary: Costello syndrome is a severe neurodevelopmental disorder caused by activating variants in HRAS. We report a unique and attenuated phenotype in six individuals with the HRAS variant c.176C>T p.(Ala59Gly), which has not been reported before as a germline variant. These individuals show ectodermal anomalies and mild features of a RASopathy, similar to patients with a Noonan syndrome-like disorder. Our findings suggest a distinct HRAS-related RASopathy for patients carrying HRAS variants affecting codons 58, 59, 60.
AMERICAN JOURNAL OF MEDICAL GENETICS PART A
(2023)
Letter
Dermatology
Magali Croquette, Alicia Faugeroux, Clemence Fonlupt, Julie Godet, Eric Frouin, Martine Garcia, Francois-Xavier Bernard, Sevda Cordier-Dirikoc, Nathalie Pedretti, Guillaume Larid, Laure Favot, Pascal Roblot, Damien Boutin, Ewa Hainaut-Wierzbicka, Dominique Heymann, Jean-Claude Lecron, Franck Morel, Jean-Francois Jegou
JOURNAL OF INVESTIGATIVE DERMATOLOGY
(2023)
Article
Clinical Neurology
Charlotte C. M. Zuurbier, Romain Bourcier, Pacome Constant Dit Beaufils, Richard Redon, Hubert Desal, Anne S. E. P. Bor, Gabriel J. E. M. Rinkel, Jacoba Greving, Ynte Ruigrok
Summary: In individuals with a positive family history of aSAH, the risk of developing a new intracranial aneurysm can be predicted after initial screening. A model incorporating three easily retrievable predictors (sex, previous history of intracranial aneurysm/aSAH, and older age) provides risk estimates for finding new intracranial aneurysms at 5, 10, and 15 years after initial screening.
Review
Endocrinology & Metabolism
Isidora Panez-Toro, Javier W. Munoz-Garcia, Jorge Vargas-Franco, Axelle Renodon-Corniere, Marie-Francoise Heymann, Frederic Lezot, Dominique Heymann
Summary: This article provides an overview of recent developments in the treatment of osteosarcoma, including targeting signaling pathways, immune checkpoint inhibitors, drug delivery strategies, and identification of new therapeutic targets.
CURRENT OSTEOPOROSIS REPORTS
(2023)
Article
Oncology
Lisa Oliver, Arturo alvarez-Arenas, Celine Salaud, Juan Jimenez-Sanchez, Gabriel F. Calvo, Juan Belmonte-Beitia, Stephanie Blandin, Luciano Vidal, Victor Perez, Dominique Heymann, Francois M. Vallette
Summary: Glioblastoma (GBM) is an incurable disease and personalized treatments are expected to be the key to therapeutic success due to the heterogeneity, complexity, and plasticity of GBM tumors. This study developed a 3D biosphere model using patient-derived cells (PDCs) from GBM and cancer-activated fibroblasts (CAFs) to mimic GBM progression and response to treatment. The co-culture of PDCs with CAFs showed similar growth and morphology to patients, and the response to standard therapy (Temozolomide and irradiation) was also consistent with GBM patients. This method provides a simple and reproducible way to obtain 3D cultures and has the potential for precision and personalized medicine.
Article
Biochemistry & Molecular Biology
Perrine Jacquot, Javier Munoz-Garcia, Maurine Fleury, Denis Cochonneau, Remi Gaussin, Elise Enouf, Caroline Roze, Emilie Ollivier, Mathieu Cinier, Dominique Heymann
Summary: Re-education of the tumor microenvironment with immune checkpoint inhibitors (ICI) has been a significant breakthrough in cancer treatment, but low response rates and immune-related adverse events (irAEs) remain challenges. A bispecific Nanofitin was engineered using anti-epidermal growth factor receptor (EGFR) and anti-programmed cell death ligand 1 (PDL1) modules to increase selectivity and safety. The study demonstrated that the bispecific Nanofitin elicited EGFR-directed PDL1 blockade, highlighting its potential in enhancing the safety and selectivity of PDL1 checkpoint inhibition.
Article
Pharmacology & Pharmacy
Nolwenn Dubois, Javier Munoz-Garcia, Dominique Heymann, Axelle Renodon-Corniere
Summary: Consuming high dietary glucose and having hyperglycemia can lead to chronic complications. This study investigated the effects of long-term exposure to high glucose on the intestinal barrier. The results showed that high glucose induced morphological changes and disrupted the structure of junction proteins. It also affected the functionalities of the intestinal barrier, and these alterations were more pronounced in co-culture models.
BIOCHEMICAL PHARMACOLOGY
(2023)
Article
Oncology
Yi Pu, Lu Li, Haoning Peng, Lunxu Liu, Dominique Heymann, Caroline Robert, Francois Vallette, Shensi Shen
Summary: Drug-tolerant persister (DTP) cell populations have been discovered in antibiotic-resistant bacterial biofilms and have also been identified in cancer cells. They are linked with treatment resistance and targeting these cells may offer new treatment opportunities.
NATURE REVIEWS CLINICAL ONCOLOGY
(2023)
Article
Biotechnology & Applied Microbiology
Camille Jubelin, Javier Munoz-Garcia, Denis Cochonneau, Emilie Ollivier, Francois Vallette, Marie-Francoise Heymann, Lisa Oliver, Dominique Heymann
Summary: This study reaffirms the relevance of simpler 3D culture methods, such as the Liquid Overlay Technique (LOT), for producing highly reproducible spheroids in the context of drug cytotoxicity measurements. The morphology of spheroids generated in round-bottom multiwell plates was found to be more repeatable than those generated in flat-bottom plates. The IC50 of doxorubicin on MNNG/HOS cells grown in 3D was significantly higher than in 2D cultures, indicating the potential of 3D models for drug response measurements.
FRONTIERS IN BIOENGINEERING AND BIOTECHNOLOGY
(2023)
Article
Endocrinology & Metabolism
Yentl Huybrechts, Raphael De Ridder, Ellen Steenackers, Jean-Pierre Devogelaer, Geert Mortier, Gretl Hendrickx, Wim Van Hul
Summary: Paget's disease of bone (PDB) is a bone disorder caused by pathogenic variants in genes such as Sequestosome 1 (SQSTM1), PFN1, and ZNF687. In this study, coding regions of PFN1 and ZNF687 were screened in a Belgian PDB cohort, and rare non-synonymous coding variants were identified in ZNF687. The study supports the involvement of genetic variation in ZNF687 in classical PDB, expanding its mutational spectrum.
CALCIFIED TISSUE INTERNATIONAL
(2023)
