Your search keyword '"Monika Gos"' showing total 94 results

1. Newborn screening and gene therapy in SMA: Challenges related to vaccinations

Author

Katarzyna Kotulska, Sergiusz Jozwiak, Maria Jedrzejowska, Monika Gos, Magdalena Ogrodnik, Jacek Wysocki, Hanna Czajka, and Ernest Kuchar

Subjects

spinal muscular atrophy, newborn screening, vaccinations, gene therapy, onasemnogene abeparvovec, Neurology. Diseases of the nervous system, RC346-429

Abstract

Spinal muscular atrophy (SMA) affects one in 7,500–10,000 newborns. Before the era of disease-modifying therapies, it used to be the major genetic cause of mortality in infants. Currently, there are three therapies approved for SMA, including two molecules modifying the splicing of the SMN2 gene and one gene therapy providing a healthy copy of the SMN gene with a viral vector. The best effects of any of these therapies are achieved when the treatment is administered in the presymptomatic stage of the disease, therefore newborn screening programs are being introduced in many countries. Patients identified in newborn screening might be eligible for gene therapy. However, gene therapy and the associated administration of steroids in newborns might interfere with the vaccination schedule, which includes live immunization against tuberculosis in some countries. The timing of gene therapy in patients who received live vaccinations has not yet been addressed neither in the clinical trials nor in the existing international guidelines. The Polish Vaccinology Association has developed the first recommendations for gene therapy administration in newborns who received live vaccination against tuberculosis. Their statement was implemented in the current guidelines for Polish SMA patients identified in the newborn screening program and might be helpful for medical professionals in other countries where live vaccine against tuberculosis is still in routine use in newborns.

Published

2022

2. Case Report: Further Delineation of Neurological Symptoms in Young Children Caused by Compound Heterozygous Mutation in the PIEZO2 Gene

Author

Magdalena Klaniewska, Maria Jedrzejowska, Malgorzata Rydzanicz, Justyna Paprocka, Mateusz Biela, Ewelina Wolanska, Agnieszka Pollak, Emilia Debek, Maria Sasiadek, Rafal Ploski, Monika Gos, and Robert Smigiel

Subjects

PIEZO2, arthrogryposis, impaired proprioception and touch, DAIPT, heterozygous mutation, Genetics, QH426-470

Abstract

PIEZO2 protein is a unique ion channel that converts mechanical impulses into cellular signals in somatosensory neurons and is involved in various mechanotransduction pathways. The recessive PIEZO2 loss-of-function pathogenic variants are associated with distal arthrogryposis with impaired proprioception and touch (DAIPT). Here we present three new DAIPT patients. The genetic diagnosis was established by exome sequencing and let us to identify 6 novel loss-of-function PIEZO2 variants: four splicing (c.1080+1G>A, c.4092+1G>T, c.6355+1G>T, and c.7613+1G>A), one nonsense (c.6088C>T) and one frameshift variant (c.6175_6191del) for which mosaic variant was identified in proband's mother. All patients presented typical symptoms at birth, with congenital contractures, bilateral hip dislocation/dysplasia, generalized hypotonia, transient feeding and difficulties. Two were afflicted by transient respiratory insufficiency. In all children motor development was severely delayed. In one patient, severe cognitive delay was also observed. Moreover, among the cases described by us there is the youngest diagnosed child to date.

Published

2021

3. Expanding the genetics and phenotypic spectrum of Lysine-specific demethylase 5C (KDM5C): a report of 13 novel variants

Author

Emanuela Leonardi, Maria Cristina Aspromonte, Denise Drongitis, Elisa Bettella, Lucia Verrillo, Roberta Polli, Meriel McEntagart, Laura Licchetta, Robertino Dilena, Stefano D’Arrigo, Claudia Ciaccio, Silvia Esposito, Vincenzo Leuzzi, Annalaura Torella, Demetrio Baldo, Fortunato Lonardo, Giulia Bonato, Serena Pellegrin, Franco Stanzial, Renata Posmyk, Ewa Kaczorowska, Miryam Carecchio, Monika Gos, Sylwia Rzońca-Niewczas, Maria Giuseppina Miano, Alessandra Murgia, Leonardi, Emanuela, Aspromonte, Maria Cristina, Drongitis, Denise, Bettella, Elisa, Verrillo, Lucia, Polli, Roberta, Mcentagart, Meriel, Licchetta, Laura, Dilena, Robertino, D'Arrigo, Stefano, Ciaccio, Claudia, Esposito, Silvia, Leuzzi, Vincenzo, Torella, Annalaura, Baldo, Demetrio, Lonardo, Fortunato, Bonato, Giulia, Pellegrin, Serena, Stanzial, Franco, Posmyk, Renata, Kaczorowska, Ewa, Carecchio, Miryam, Gos, Monika, Rzońca-Niewczas, Sylwia, Miano, Maria Giuseppina, and Murgia, Alessandra

Subjects

Genetics, Genetics (clinical)

Abstract

Lysine-specific demethylase 5C (KDM5C) has been identified as an important chromatin remodeling gene, contributing to X-linked neurodevelopmental disorders (NDDs). The KDM5C gene, located in the Xp22 chromosomal region, encodes the H3K4me3-me2 eraser involved in neuronal plasticity and dendritic growth. Here we report 30 individuals carrying 13 novel and one previously identified KDM5C variants. Our cohort includes the first reported case of somatic mosaicism in a male carrying a KDM5C nucleotide substitution, and a dual molecular finding in a female carrying a homozygous truncating FUCA1 alteration together with a de novo KDM5C variant. With the use of next generation sequencing strategies, we detected 1 frameshift, 1 stop codon, 2 splice-site and 10 missense variants, which pathogenic role was carefully investigated by a thorough bioinformatic analysis. The pattern of X-chromosome inactivation was found to have an impact on KDM5C phenotypic expression in females of our cohort. The affected individuals of our case series manifested a neurodevelopmental condition characterized by psychomotor delay, intellectual disability with speech disorders, and behavioral features with particular disturbed sleep pattern; other observed clinical manifestations were short stature, obesity and hypertrichosis. Collectively, these findings expand the current knowledge about the pathogenic mechanisms leading to dysfunction of this important chromatin remodeling gene and contribute to a refinement of the KDM5C phenotypic spectrum.

Published

2022

4. Splicing mutations in human genetic disorders: examples, detection, and confirmation

Author

Anna, Abramowicz and Monika, Gos

Published

2018

5. Recommendations of the Polish Sarcoma Group on diagnostic-therapeutic procedures and control in patients with type 1 neurofibromatosis (NF1) and the associated malignant neoplasm of peripheral nerve sheaths

Author

Piotr Rutkowski, Anna Raciborska, Anna Szumera-Ciećkiewicz, Paweł Sobczuk, Mateusz Spałek, Hanna Koseła-Paterczyk, Iwona Ługowska, Katarzyna Bilska, Monika Gos, Janusz Ryś, Ewa Chmielik, Andrzej Tysarowski, Konrad Zaborowski, Małgorzata Oczko-Wojciechowska, Patrycja Castaneda-Wysocka, Donata Makuła, Marcin Zdzienicki, Marcin Ziętek, Piotr Fonrobert, Kamil Dolecki, Marek Dedecjus, and Anna M. Czarnecka

Subjects

Cancer Research, Oncology

Published

2022

6. Destabilization of mutated human PUS3 protein causes intellectual disability

Author

Ting‐Yu Lin, Robert Smigiel, Bozena Kuzniewska, Joanna J. Chmielewska, Joanna Kosińska, Mateusz Biela, Anna Biela, Anna Kościelniak, Dominika Dobosz, Izabela Laczmanska, Andrzej Chramiec‐Głąbik, Jakub Jeżowski, Jakub Nowak, Monika Gos, Sylwia Rzonca‐Niewczas, Magdalena Dziembowska, Rafał Ploski, and Sebastian Glatt

Subjects

Intellectual Disability, Genetics, Humans, RNA Processing, Post-Transcriptional, Genetics (clinical), Hydro-Lyases, Pseudouridine

Abstract

Pseudouridine (Ψ) is an RNA base modification ubiquitously found in many types of RNAs. In humans, the isomerization of uridine is catalyzed by different stand-alone pseudouridine synthases (PUS). Genomic mutations in the human pseudouridine synthase 3 gene (PUS3) have been identified in patients with neurodevelopmental disorders. However, the underlying molecular mechanisms that cause the disease phenotypes remain elusive. Here, we utilize exome sequencing to identify genomic variants that lead to a homozygous amino acid substitution (p.[(Tyr71Cys)];[(Tyr71Cys)]) in human PUS3 of two affected individuals and a compound heterozygous substitution (p.[(Tyr71Cys)];[(Ile299Thr)]) in a third patient. We obtain wild-type and mutated full-length human recombinant PUS3 proteins and characterize the enzymatic activity in vitro. Unexpectedly, we find that the p.Tyr71Cys substitution neither affect tRNA binding nor pseudouridylation activity in vitro, but strongly impair the thermostability profile of PUS3, while the p.Ile299Thr mutation causes protein aggregation. Concomitantly, we observe that the PUS3 protein levels as well as the level of PUS3-dependent Ψ levels are strongly reduced in fibroblasts derived from all three patients. In summary, our results directly illustrate the link between the identified PUS3 variants and reduced Ψ levels in the patient cells, providing a molecular explanation for the observed clinical phenotypes.

Published

2022

7. Bullous diseases caused by KRT1 gene mutations: from epidermolytic hyperkeratosis to a novel variant of epidermolysis bullosa simplex

Author

Monika Gos, Katarzyna Wertheim-Tysarowska, Katarzyna Osipowicz, Cezary Kowalewski, Katarzyna Woźniak, Bartłomiej Kwiek, Ewa Jankowska, and Agnieszka Charzewska

Subjects

KRT1gene, medicine.medical_specialty, Bullous ichthyosis, integumentary system, business.industry, Dermatology, epidermolysis bullosa simplex, Gene mutation, medicine.disease, Epidermolytic hyperkeratosis, Original Papers, bullous ichthyosis, epidermolytic hyperkeratosis, Epidermolysis bullosa simplex, medicine, Immunology and Allergy, business

Abstract

Introduction Mutations in the KRT1 gene encoding keratin 1 cause epidermolytic hyperkeratosis characterized by blistering in the neonatal period followed by ichthyotic hyperkeratosis in childhood and adolescent life. We observed a spectrum of clinical manifestations of blistering disorders caused by different mutations in the same KRT1 gene. Aim To analyse the phenotypic spectrum of blistering disorders caused by the KRT1 mutations. Material and methods Four patients with an epidermal barrier defect manifesting as blistering with the KRT1 mutations were included to the study. The clinical course of the disease was analysed, histology, immunofluorescence and electron microscopic examinations were performed. Results An adult patient with severe ichthyosis with p.Asn188Lys mutation in exon 1 of KRT1 who occasionally develops blisters in adolescence represents epidermolytic hyperkeratosis, a newborn child who died 4 days after birth due to disruption of the epidermal barrier (extensive blister and erosions) with mutation p.Ser193Pro in the KTR1 gene and two adult sisters harbouring heterozygous mutation c.591+1A>G in the KRT1 gene who present superficial blisters induced by mild trauma from the birth up to adolescent life without ichthyosis suggesting the diagnosis of epidermolysis bullosa simplex. Histopathology in all adult patients showed cytoplasm disruption in keratinocytes of the stratum spinosum with keratohyalin granule-like structures and, on the ultrastructural level, the presence of keratin clumping confirming the pathology of keratin intermediate filaments. Conclusions This study extends the knowledge of the clinical spectrum for the KRT1 gene mutations. This is the first description of familial dominant epidermolysis bullosa simplex linked to the KRT1 mutation.

Published

2020

8. Wide Fontanels, Delayed Speech Development and Hoarse Voice as Useful Signs in the Diagnosis of KBG Syndrome: A Clinical Description of 23 Cases with Pathogenic Variants Involving the ANKRD11 Gene or Submicroscopic Chromosomal Rearrangements of 16q24.3

Author

Anna Kutkowska-Kaźmierczak, Maria Boczar, Ewa Kalka, Jennifer Castañeda, Jakub Klapecki, Aleksandra Pietrzyk, Artur Barczyk, Olga Malinowska, Aleksandra Landowska, Tomasz Gambin, Katarzyna Kowalczyk, Barbara Wiśniowiecka-Kowalnik, Marta Smyk, Mateusz Dawidziuk, Katarzyna Niepokój, Magdalena Paczkowska, Paweł Szyld, Beata Lipska-Ziętkiewicz, Krzysztof Szczałuba, Ewa Kostyk, Agata Runge, Karolina Rutkowska, Rafał Płoski, Beata Nowakowska, Jerzy Bal, Ewa Obersztyn, and Monika Gos

Subjects

wide, delayed closing fontanels, 16q24.3, dysmorphic syndrome, ANKRD11 gene, Genetics, hoarse voice, QH426-470, KBG syndrome

Abstract

KBG syndrome is a neurodevelopmental autosomal dominant disorder characterized by short stature, macrodontia, developmental delay, behavioral problems, speech delay and delayed closing of fontanels. Most patients with KBG syndrome are found to have a mutation in the ANKRD11 gene or a chromosomal rearrangement involving this gene. We hereby present clinical evaluations of 23 patients aged 4 months to 26 years manifesting clinical features of KBG syndrome. Mutation analysis in the patients was performed using panel or exome sequencing and array CGH. Besides possessing dysmorphic features typical of the KBG syndrome, nearly all patients had psychomotor hyperactivity (86%), 81% had delayed speech, 61% had poor weight gain, 56% had delayed closure of fontanel and 56% had a hoarse voice. Macrodontia and a height range of −1 SDs to −2 SDs were noted in about half of the patients; only two patients presented with short stature below −3 SDs. The fact that wide, delayed closing fontanels were observed in more than half of our patients with KBG syndrome confirms the role of the ANKRD11 gene in skull formation and suture fusion. This clinical feature could be key to the diagnosis of KBG syndrome, especially in young children. Hoarse voice is a previously undescribed phenotype of KBG syndrome and could further reinforce clinical diagnosis.

Published

2021

9. The

Author

Mateusz, Dawidziuk, Anna, Kutkowska-Kaźmierczak, Paweł, Gawliński, Wojciech, Wiszniewski, Monika, Gos, Piotr, Stawiński, Małgorzata, Rydzanicz, Joanna, Kosińska, Paweł, Własienko, Olga, Malinowska Kordowska, Magdalena, Bartnik-Głaska, Joanna, Bernaciak, Krzysztof, Szczałuba, Monika, Bekiesińska-Figatowska, Rafał, Płoski, Jerzy, Bal, and Sylwia, Olimpia Rzońca-Niewczas

Subjects

Male, Review Paper, Mediator Complex, Genetic Variation, Haploinsufficiency, MED13L, haploinsufficiency, Phenotype, Loss of Function Mutation, intellectual disability, Intellectual Disability, Mutation, Humans, Abnormalities, Multiple, Child, loss-of-function mutation

Abstract

The Mediator complex subunit 13-like is a part of the large Mediator complex. Recently, a large number of patients were diagnosed with mutations in this gene, which makes it one of the most frequent causes of syndromic intellectual disability. In this work, we report a patient with a novel de novo likely pathogenic variant c.5941C>T, p.(Gln1981*) in the MED13L gene with severe intellectual disability and facial dysmorphism. Uncommon findings like lack of speech, strabismus and self-destructive behaviour present in our patient allowed us to further define the phenotypic spectrum of mental retardation and distinctive facial features with or without cardiac defects syndrome.

Published

2021

10. Case Report: Further Delineation of Neurological Symptoms in Young Children Caused by Compound Heterozygous Mutation in the PIEZO2 Gene

Author

Justyna Paprocka, Maria M. Sasiadek, Małgorzata Rydzanicz, Robert Smigiel, Mateusz Biela, Agnieszka Pollak, Rafał Płoski, Magdalena Klaniewska, Monika Gos, Ewelina Wolańska, Maria Jędrzejowska, and Emilia Dębek

Subjects

0301 basic medicine, Proband, Pediatrics, medicine.medical_specialty, media_common.quotation_subject, Nonsense, Case Report, QH426-470, 030105 genetics & heredity, DAIPT, Compound heterozygosity, arthrogryposis, Frameshift mutation, 03 medical and health sciences, Genetics, medicine, Genetics (clinical), Exome sequencing, media_common, Arthrogryposis, impaired proprioception and touch, business.industry, heterozygous mutation, medicine.disease, 030104 developmental biology, Dysplasia, Molecular Medicine, PIEZO2, Congenital contracture, medicine.symptom, business

Abstract

PIEZO2 protein is a unique ion channel that converts mechanical impulses into cellular signals in somatosensory neurons and is involved in various mechanotransduction pathways. The recessive PIEZO2 loss-of-function pathogenic variants are associated with distal arthrogryposis with impaired proprioception and touch (DAIPT). Here we present three new DAIPT patients. The genetic diagnosis was established by exome sequencing and let us to identify 6 novel loss-of-function PIEZO2 variants: four splicing (c.1080+1G>A, c.4092+1G>T, c.6355+1G>T, and c.7613+1G>A), one nonsense (c.6088C>T) and one frameshift variant (c.6175_6191del) for which mosaic variant was identified in proband's mother. All patients presented typical symptoms at birth, with congenital contractures, bilateral hip dislocation/dysplasia, generalized hypotonia, transient feeding and difficulties. Two were afflicted by transient respiratory insufficiency. In all children motor development was severely delayed. In one patient, severe cognitive delay was also observed. Moreover, among the cases described by us there is the youngest diagnosed child to date.

Published

2021

11. Pathogenic Mutations and Putative Phenotype-Affecting Variants in Polish Myofibrillar Myopathy Patients

Author

Jakub Piotr Fichna, Anna Potulska-Chromik, Cezary Zekanowski, Maria Jędrzejowska, Biruta Kierdaszuk, Andrzej Opuchlik, Edyta Rosiak, Aleksandra Maruszak, and Monika Gos

Subjects

lcsh:Medicine, Disease, Interactome, DNA sequencing, Article, 03 medical and health sciences, 0302 clinical medicine, Human Phenotype Ontology, Medicine, oligogenic inheritance, skeletal muscle, Gene, Exome sequencing, 030304 developmental biology, Genetics, 0303 health sciences, variant load, Genetic heterogeneity, business.industry, lcsh:R, General Medicine, Phenotype, NGS, genomic data, business, 030217 neurology & neurosurgery, WGS

Abstract

Myofibrillar myopathies (MFM) are heterogeneous hereditary muscle diseases with characteristic myopathological features of Z-disk dissolution and aggregates of its degradation products. The onset and progression of the disease are variable, with an elusive genetic background, and around half of the cases lacking molecular diagnosis. Here, we attempted to establish possible genetic foundations of MFM by performing whole exome sequencing (WES) in eleven unrelated families of 13 patients clinically diagnosed as MFM spectrum. A filtering strategy aimed at identification of variants related to the disease was used and included integrative analysis of WES data and human phenotype ontology (HPO) terms, analysis of muscle-expressed genes, and analysis of the disease-associated interactome. Genetic diagnosis was possible in eight out of eleven cases. Putative causative mutations were found in the DES (two cases), CRYAB, TPM3, and SELENON (four cases) genes, the latter typically presenting with a rigid spine syndrome. Moreover, a variety of additional, possibly phenotype-affecting variants were found. These findings indicate a markedly heterogeneous genetic background of MFM and show the usefulness of next generation sequencing in the identification of disease-associated mutations. Finally, we discuss the emerging concept of variant load as the basis of phenotypic heterogeneity.

Published

2021

12. Floppy infant syndrome as a first manifestation of LMNA-related congenital muscular dystrophy

Author

Bartłomiej Gielniewski, Robert Szymańczak, Agnieszka Madej-Pilarczyk, Anna Potulska-Chromik, Tomasz Gambin, Krystyna H. Chrzanowska, Maria Jędrzejowska, Agnieszka Sobczyńska, Edyta Rosiak, Anna Kostera-Pruszczyk, Agnieszka Stępień, Emilia Dębek, Bartosz Wojtaś, Elżbieta Ciara, and Monika Gos

Subjects

Proband, Male, Pediatrics, medicine.medical_specialty, Adolescent, Genotype, Laminopathy, Muscular Dystrophies, LMNA, 03 medical and health sciences, 0302 clinical medicine, 030225 pediatrics, medicine, Humans, Floppy Infant, Child, Exome, business.industry, Muscle weakness, General Medicine, medicine.disease, Lamin Type A, Magnetic Resonance Imaging, Hypotonia, Pedigree, Phenotype, Child, Preschool, Pediatrics, Perinatology and Child Health, Mutation, Congenital muscular dystrophy, Muscle Hypotonia, Female, Neurology (clinical), medicine.symptom, business, 030217 neurology & neurosurgery

Abstract

LMNA-related congenital muscular dystrophy (L-CMD) is the most severe phenotypic form of skeletal muscle laminopathies. This paper reports clinical presentation of the disease in 15 Polish patients from 13 families with genetically confirmed skeletal muscle laminopathy. In all these patients floppy infant syndrome was the first manifestation of the disease. The genetic diagnosis was established by next generation sequencing (targeted panel or exome; 11 patients) or classic Sanger sequencing (4 patients). In addition to known pathogenic LMNA variants: c.116A > G (p.Asn39Ser), c.745C > T (p.Arg249Trp), c.746G > A (p.Arg249Gln), c.1072G > A (p.Glu358Lys), c.1147G > A (p.Glu383Lys), c.1163G > C (p.Arg388Pro), c.1357C > T (p.Arg453Trp), c.1583C > G (p.Thr528Arg), we have identified three novel ones: c.121C > G (p.Arg41Gly), c.1127A > G (p.Tyr376Cys) and c.1160T > C (p.Leu387Pro). Eleven patients had de novo mutations, 4 – familial. In one family we observed intrafamilial variability of clinical course: severe L-CMD in the male proband, intermediate form in his sister and asymptomatic in their mother. One asymptomatic father had somatic mosaicism. L-CMD should be suspected in children with hypotonia in infancy and delayed motor development, who have poor head control, severe hyperlordosis and unstable and awkward gait. Serum creatine kinase may be high (~1000IU/l). Progression of muscle weakness is fast, leading to early immobilization. In some patients with L-CMD joint contractures can develop with time. MRI shows that the most frequently affected muscles are the serratus anterior, lumbar paraspinal, gluteus, vastus, adductor magnus, hamstrings, medial head of gastrocnemius and soleus. Ultra-rare laminopathies can be a relatively common cause of generalized hypotonia in children. Introduction of wide genome sequencing methods was a breakthrough in diagnostics of diseases with great clinical and genetic variability and allowed approach “from genotype do phenotype”. However target sequencing of LMNA gene could be considered in selected patients with clinical picture suggestive for laminopathy.

Published

2021

13. Successful Salvage Treosulfan-Based Megachemotherapy With Allogeneic Stem Cell Transplantation in Nonsyndromic, Therapy-Resistant Disseminated Juvenile Xanthogranuloma: A Case Report

Author

Małgorzata Janeczko-Czarnecka, Marek Ussowicz, Anna Raciborska, Blanka Rybka, Renata Ryczan-Krawczyk, Monika Gos, Kornelia Gajek, Krzysztof Kałwak, and Olga Malinowska Kordowska

Subjects

Male, medicine.medical_specialty, Juvenile xanthogranuloma, Disease, Treosulfan, medicine, Humans, Antineoplastic Agents, Alkylating, Busulfan, Histiocyte, Salvage Therapy, Transplantation, business.industry, Remission Induction, Hematopoietic Stem Cell Transplantation, Hematopoietic stem cell, medicine.disease, Dermatology, Combined Modality Therapy, Histiocytosis, medicine.anatomical_structure, Child, Preschool, Surgery, Stem cell, business, Xanthogranuloma, Juvenile, medicine.drug

Abstract

Juvenile xanthogranuloma (JXG) is a rare histiocytic disorder classified as non-Langerhans cell histiocytosis; although it is usually a benign and self-limiting disease, it can be fatal in some cases, especially with systemic dissemination. We present a case report of a boy with therapy-resistant disseminated JXG who was treated with systemic chemotherapy and received 3 allogeneic hematopoietic stem cell transplantations (allo-HSCTs) from an unrelated donor. The post-transplant period was complicated by acute graft vs host disease and lymphoproliferative disease caused by Epstein-Barr virus. Currently, almost 7.5 years after the first transplantation, the boy is in complete remission with full donor chimerism and without symptoms of JXG. The presented data confirm rare observations that allo-HSCT can lead to durable remission of systemic JXG, which warrants its use in life-threatening, therapy-resistant subtypes of disease.

Published

2020

14. Mutation in the KRT1 gene causing epidermolysis bullosa simplex

Author

Agnieszka Charzewska, Ewa Jankowska, Katarzyna Wertheim-Tysarowska, Katarzyna Woźniak, Cezary Kowalewski, Katarzyna Osipowicz, and Monika Gos

Subjects

Genetics, Epidermolysis bullosa simplex, business.industry, Mutation (genetic algorithm), Immunology and Allergy, Medicine, Dermatology, business, medicine.disease, Gene

Published

2020

15. The remarkable phenotypic variability of the p.Arg269HiS variant in the TRPV4 gene

Author

Małgorzata Rydzanicz, Piotr Gasperowicz, Maria Jędrzejowska, Elżbieta Ciara, Aleksandra Jezela-Stanek, Paulina Halat, Bartłomiej Kowalczyk, Monika Gos, Emilia Dębek, and Anna Kostera-Pruszczyk

Subjects

0301 basic medicine, Sanger sequencing, Weakness, Physiology, business.industry, Congenital distal spinal muscular atrophy, Cranial nerves, Scoliosis, 030105 genetics & heredity, medicine.disease, Bioinformatics, Hypotonia, 03 medical and health sciences, Cellular and Molecular Neuroscience, symbols.namesake, 0302 clinical medicine, Physiology (medical), Anticipation (genetics), symbols, Medicine, Neurology (clinical), Congenital contracture, medicine.symptom, business, 030217 neurology & neurosurgery

Abstract

Introduction Mutations in the TRPV4 gene are associated with neuromuscular disorders and skeletal dysplasias, which present a phenotypic overlap. Methods Next-generation sequencing and Sanger sequencing were used to analyze the TRPV4 gene. Results We present 2 Polish families with TRPV4-related disorder harboring the same p.Arg269His mutation. The disease phenotypic expression was extremely variable (from mild scapular winging to severe hypotonia, global weakness, inability to walk unaided, congenital contractures, scoliosis, and respiratory insufficiency), but did not suggest anticipation. The 2 most severely affected patients showed congenital distal contractures of the upper limbs and involvement of cranial nerves (manifesting as facial asymmetry and strabismus). The disease course seemed to be stable, although in later stages it caused respiratory insufficiency and progression of physical disability. Discussion The phenotypic variability observed in p.Arg269His carriers suggests that an additional modifier or a more complex pathogenic mechanism exists. Muscle Nerve 59:129-133, 2019.

Published

2018

16. Wide Fontanels, Delayed Speech Development and Hoarse Voice as Useful Signs in the Diagnosis of KBG Syndrome: A Clinical Description of 23 Cases with Pathogenic Variants Involving the ANKRD11 Gene or Submicroscopic Chromosomal Rearrangements of 16q24.3

Author

Jerzy Bal, Olga Malinowska, Jennifer Castaneda, Mateusz Dawidziuk, Maria Boczar, Aleksandra Landowska, Ewa Obersztyn, Agata Runge, Marta Smyk, Beata Nowakowska, Katarzyna Niepokój, Karolina Rutkowska, Magdalena Paczkowska, Anna Kutkowska-Kaźmierczak, Katarzyna Kowalczyk, Ewa Kostyk, Barbara Wiśniowiecka-Kowalnik, Aleksandra Pietrzyk, Jakub Klapecki, Ewa Kalka, Artur Barczyk, Krzysztof Szczałuba, Monika Gos, Tomasz Gambin, Beata S. Lipska-Ziętkiewicz, Pawel Szyld, and Rafał Płoski

Subjects

Male, speech delay, Pediatrics, Psychomotor agitation, psychomotor hyperactivity, ANKRD11 gene, 16q24.3, dysmorphic syndrome, hoarse voice, Child, Genetics (clinical), Exome sequencing, wide, delayed closing fontanels, Comparative Genomic Hybridization, KBG syndrome, Phenotype, Child, Preschool, Speech delay, Female, medicine.symptom, Adult, medicine.medical_specialty, Adolescent, Dwarfism, Chromosomal rearrangement, Short stature, Article, Young Adult, Intellectual Disability, Exome Sequencing, Genetics, medicine, Humans, Abnormalities, Multiple, Genetic Predisposition to Disease, Gene, Chromosome Aberrations, Bone Diseases, Developmental, Tooth Abnormalities, business.industry, Facies, Infant, medicine.disease, short stature, Repressor Proteins, Hoarse voice, Macrodontia (tooth), Mutation, business, Chromosomes, Human, Pair 16

Abstract

KBG syndrome is a neurodevelopmental autosomal dominant disorder characterized by short stature, macrodontia, developmental delay, behavioral problems, speech delay and delayed closing of fontanels. Most patients with KBG syndrome are found to have a mutation in the ANKRD11 gene or a chromosomal rearrangement involving this gene. We hereby present clinical evaluations of 23 patients aged 4 months to 26 years manifesting clinical features of KBG syndrome. Mutation analysis in the patients was performed using panel or exome sequencing and array CGH. Besides possessing dysmorphic features typical of the KBG syndrome, nearly all patients had psychomotor hyperactivity (86%), 81% had delayed speech, 61% had poor weight gain, 56% had delayed closure of fontanel and 56% had a hoarse voice. Macrodontia and a height range of −1 SDs to −2 SDs were noted in about half of the patients, only two patients presented with short stature below −3 SDs. The fact that wide, delayed closing fontanels were observed in more than half of our patients with KBG syndrome confirms the role of the ANKRD11 gene in skull formation and suture fusion. This clinical feature could be key to the diagnosis of KBG syndrome, especially in young children. Hoarse voice is a previously undescribed phenotype of KBG syndrome and could further reinforce clinical diagnosis.

Published

2021

17. Correction to: Splicing mutations in human genetic disorders: examples, detection, and confirmation

Author

Monika Gos and Anna Abramowicz

Subjects

0106 biological sciences, 0301 basic medicine, RNA Splicing, DNA Mutational Analysis, MEDLINE, Computational biology, Biology, 01 natural sciences, 03 medical and health sciences, Genetics, Humans, Point Mutation, Computer Simulation, Published Erratum, Search engine indexing, Genetic Diseases, Inborn, Correction, Computational Biology, General Medicine, Exons, Human genetics, Introns, 030104 developmental biology, RNA splicing, Mutation, Pyrimidine Nucleotides, RNA Splice Sites, Algorithms, 010606 plant biology & botany

Abstract

Precise pre-mRNA splicing, essential for appropriate protein translation, depends on the presence of consensus "cis" sequences that define exon-intron boundaries and regulatory sequences recognized by splicing machinery. Point mutations at these consensus sequences can cause improper exon and intron recognition and may result in the formation of an aberrant transcript of the mutated gene. The splicing mutation may occur in both introns and exons and disrupt existing splice sites or splicing regulatory sequences (intronic and exonic splicing silencers and enhancers), create new ones, or activate the cryptic ones. Usually such mutations result in errors during the splicing process and may lead to improper intron removal and thus cause alterations of the open reading frame. Recent research has underlined the abundance and importance of splicing mutations in the etiology of inherited diseases. The application of modern techniques allowed to identify synonymous and nonsynonymous variants as well as deep intronic mutations that affected pre-mRNA splicing. The bioinformatic algorithms can be applied as a tool to assess the possible effect of the identified changes. However, it should be underlined that the results of such tests are only predictive, and the exact effect of the specific mutation should be verified in functional studies. This article summarizes the current knowledge about the "splicing mutations" and methods that help to identify such changes in clinical diagnosis.

Published

2019

18. NovelCol12A1variant expands the clinical picture of congenital myopathies with extracellular matrix defects

Author

Carsten G. Bönnemann, Maria JȨdrzejowska, Anna Kostera-Pruszczyk, Anna Kamińska, Akanchha Kesari, Ying Hu, Jaya Punetha, Eric P. Hoffman, Monika Gos, Yaqun Zou, and Irena Hausmanowa-Petrusewicz

Subjects

0301 basic medicine, medicine.medical_specialty, Pathology, Physiology, Ullrich congenital muscular dystrophy, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, Collagen VI, Physiology (medical), Internal medicine, medicine, Missense mutation, Myopathy, business.industry, Bethlem myopathy, Overlap syndrome, medicine.disease, Congenital myopathy, Hypotonia, 030104 developmental biology, Endocrinology, Neurology (clinical), medicine.symptom, business, 030217 neurology & neurosurgery

Abstract

Introduction Mutations in the COL12A1 (collagen, type XII, alpha 1) gene have been described in a milder Bethlem-like myopathy in 6 patients from 3 families (dominant missense), and in a severe congenital form with failure to attain ambulation in 2 patients in a single pedigree (recessive loss-of-function). Methods We describe an 8-year-old girl of Polish origin who presented with profound hypotonia and joint hyperlaxity at birth after a pregnancy complicated by oligohydramnios and intrauterine growth retardation. Results We identified a novel, potentially pathogenic heterozygous missense COL12A1 c.8329G>C (p.Gly2777Arg) variant using a targeted sequencing panel. Patient fibroblast studies confirmed intracellular retention of the COL12A1 protein, consistent with a dominant-negative mutation. Conclusions As our patient showed a more intermediate phenotype, this case expands the phenotypic spectrum for COL12A1 disorders. So far, COL12A1 disorders seem to cover much of the severity range of an Ehlers-Danlos/Bethlem-like myopathy overlap syndrome associated with both connective tissue abnormalities and muscle weakness. Muscle Nerve 55: 277-281, 2017.

Published

2016

19. Zespół Noonan u noworodka z przeważającymi objawami niewydolności oddechowej oraz kardiomiopatii przerostowej i nadciśnienia płucnego

Author

Monika Gos, Karolina Jeleń, Robert Śmigiel, Ewa Terpińska, and Barbara Królak-Olejnik

Subjects

0301 basic medicine, medicine.medical_specialty, business.industry, Cardiomyopathy, Hypertrophic cardiomyopathy, medicine.disease, Short stature, Gastroenterology, PTPN11, 03 medical and health sciences, 030104 developmental biology, Endocrinology, Internal medicine, Pediatrics, Perinatology and Child Health, medicine, Noonan syndrome, Webbed neck, medicine.symptom, Hypertelorism, Trisomy, business

Abstract

Noonan syndrome (NS) is a clinically heterogeneous and autosomal dominant disorder which occurs with a frequency of 1:1000–2500 live births regardless of gender. The most characteristic clinical features are: short stature, congenital heart defects, numerous and various dysmorphic features (eg.: hypertelorism, palpebral fissures slant down, low-set ears, short and broad neck with excess skin, webbed neck, low hair line on the neck), as well as deformities of the chest, skeletal and urogenital system as well as coagulation disturbances. Psychomotor development is delayed. NS is the second, after trisomy of chromosome 21, the most common genetic cause of congenital heart defects. Mutation of one gene – between fifteen genes known – encoding proteins in RAS/MAPK cellular pathway is the genetic cause of illness. Approximately 50% of patients have a mutation in the PTPN11 gene; mutations in other genes are considerably rare (up to 10–15% for SOS1, RAF1 and RIT1, up to 1–2% for others). The literature describes the correlation between the RAF1 mutation and the incidence of hypertrophic cardiomyopathy, or primary pulmonary hypertension in these group of patients. The paper presents the case of infant with hypertrophic cardiomyopathy and pulmonary hypertension where RAF1 c.770C> T mutation was confirmed, as the reason of Noonan syndrome.

Published

2016

20. Neurofibromin – protein structure and cellular functions in the context of neurofibromatosis type I pathogenesis

Author

Anna Abramowicz and Monika Gos

Subjects

Microbiology (medical), congenital, hereditary, and neonatal diseases and abnormalities, Neurofibromatosis 1, Protein Conformation, szlak RAS/MAPK, nerwiakowłókniakowatość typu I, lcsh:Medicine, Biology, neurofibromina, medicine, Humans, szlak cAMP/PKA, Protein kinase A, PI3K/AKT/mTOR pathway, Regulation of gene expression, Neurofibromatosis type I, Neurofibromin 1, lcsh:R, neurofibromin, medicine.disease, Actin cytoskeleton, Cell biology, nervous system diseases, Alternative Splicing, Infectious Diseases, Mutation, Cancer research, biology.protein, Signal transduction, Protein Processing, Post-Translational, Cyclase activity, Signal Transduction

Abstract

Neurofibromatosis type I (NF1) is multisystemic disease characterized by pigmentary skin changes, increased susceptibility to tumor formation, neurological deficits and skeletal defects. The disease is a monogenic, autosomal dominant disorder, caused by the presence of mutations in the NF1 gene encoding neurofibromin - a multifunctional regulatory protein. The basic function of neurofibromin protein is modulation of the RAS protein activity necessary for regulation of cell proliferation and differentiation by the RAS/MAPK and RAS/PI3K/AKT signal transduction pathways. In addition, neurofibromin is a regulator of adenylate cyclase activity and therefore may interfere with signaling by the cAMP/protein kinase A pathway that regulates cell cycle progression or learning and memory formation processes. Neurofibromin also interacts with many other proteins that are engaged in intracellular transport (tubulin, kinesin), actin cytoskeleton rearrangements (LIMK2, Rho and Rac) or morphogenesis of neural cells (syndecans, CRMP proteins). The activity of neurofibromin is strictly regulated by the expression of different NF1 mRNA isoforms depending on tissue type or period in organism development, the protein localization, posttranslational modifications (phosphorylation, ubiquitination) or interactions with other proteins (e.g. 14-3-3). The fact that neurofibromin is engaged in many cellular processes has significant consequences when the proper protein functioning is impaired due to decreased protein level or activity. It affects the normal cell function and results in disturbances of organism development that lead to the occurrence of clinical signs specific for NF1. In the article, the basic neurofibromin functions are presented in the context of the molecular pathogenesis of NF1.

Published

2015

21. The power of the Mediator complex-Expanding the genetic architecture and phenotypic spectrum of MED12-related disorders

Author

Andreas Tzschach, W. Hachmann, C Jensen, Magdalena Nawara, Jarosław Poznański, K. Kahrizi, Jerzy Bal, Vera M. Kalscheuer, M Bienek, Andreas Dufke, H. Enders, Johannes R. Lemke, Monika Gos, T. Chilarska, Dorota Hoffman-Zacharska, Agnieszka Charzewska, Hossein Najmabadi, Barbara Oehl-Jaschkowitz, R. Maiwald, and Ewa Obersztyn

Subjects

0301 basic medicine, Male, Models, Molecular, Genotype, FG syndrome, X-linked intellectual disability, Protein Conformation, Mutation, Missense, Biology, MED12, 03 medical and health sciences, Structure-Activity Relationship, Lujan–Fryns syndrome, Genes, X-Linked, X Chromosome Inactivation, Exome Sequencing, Genetics, medicine, Missense mutation, Humans, Genetic Predisposition to Disease, Genetics (clinical), X chromosome, Alleles, Genetic Association Studies, Mediator Complex, Facies, Genetic Variation, medicine.disease, Genetic architecture, Pedigree, 030104 developmental biology, Phenotype, Amino Acid Substitution, Female, Single Palmar Crease

Abstract

MED12 is a member of the large Mediator complex that controls cell growth, development, and differentiation. Mutations in MED12 disrupt neuronal gene expression and lead to at least three distinct X-linked intellectual disability syndromes (FG, Lujan-Fryns, and Ohdo). Here, we describe six families with missense variants in MED12 (p.(Arg815Gln), p.(Val954Gly), p.(Glu1091Lys), p.(Arg1295Cys), p.(Pro1371Ser), and p.(Arg1148His), the latter being first reported in affected females) associated with a continuum of symptoms rather than distinct syndromes. The variants expanded the genetic architecture and phenotypic spectrum of MED12-related disorders. New clinical symptoms included brachycephaly, anteverted nares, bulbous nasal tip, prognathism, deep set eyes, and single palmar crease. We showed that MED12 variants, initially implicated in X-linked recessive disorders in males, may predict a potential risk for phenotypic expression in females, with no correlation of the X chromosome inactivation pattern in blood cells. Molecular modeling (Yasara Structure) performed to model the functional effects of the variants strongly supported the pathogenic character of the variants examined. We showed that molecular modeling is a useful method for in silico testing of the potential functional effects of MED12 variants and thus can be a valuable addition to the interpretation of the clinical and genetic findings.

Published

2018

22. [Fragile X syndrome and FMR1-dependent diseases - clinical presentation, epidemiology and molecular background]

Author

Aleksandra, Landowska, Sylwia, Rzońca, Jerzy, Bal, and Monika, Gos

Subjects

Male, DNA Repeat Expansion, Original articles/Prace oryginalne, Primary Ovarian Insufficiency, Fragile X Mental Retardation Protein, Gene Expression Regulation, zespół łamliwego chromosomu X, Fragile X Syndrome, Mutation, Tremor, Humans, Ataxia, Female, FXTAS, FXS, FMR1, FXPOI

Abstract

Streszczenie Zespół łamliwego chromosomu X (ang. Fragile X Syndrome, FXS) jest, po zespole Downa, najczęstszą dziedziczną przyczyną niepełnosprawności intelektualnej (NI). Stopień niepełnosprawności intelektualnej pacjentów z FXS jest różny i zależy głównie od płci. Zaburzeniom intelektualnym towarzyszą dodatkowe objawy takie jak opóźnienie rozwoju psychoruchowego, zaburzenia zachowania czy emocji. W ponad 99% przypadków, choroba spowodowana jest występowaniem mutacji dynamicznej w genie FMR1 zlokalizowanym na chromosomie X. W wyniku ekspansji trójki nukleotydów CGG (>200 powtórzeń) dochodzi do zahamowania ekspresji genu, a tym samym znacznego obniżenia poziomu białka FMRP kodowanego przez gen FMR1. Ekspansja sekwencji CGG do zakresu premutacji (55-200 powtórzeń CGG) warunkuje wystąpienie nosicielstwa FXS i chorób FMR1-zależnych takich jak: przedwczesne wygasanie funkcji jajników związane z zespołem łamliwego chromosomu X (ang. Fragile X-associated Primary Ovarian Insufficiency, FXPOI) oraz zespołu drżenia i ataksji związanego z zespołem łamliwego chromosomu X (ang. Fragile X-associated Tremor/Ataxia Syndrome, FXTAS). W przypadku obu tych chorób objawy kliniczne występują dopiero u ludzi dorosłych. Celem pracy jest przybliżenie aktualnej wiedzy dotyczącej podłoża molekularnego i epidemiologii zespołu łamliwego chromosomu X oraz innych chorób FMR1-zależnych.

Published

2018

23. The remarkable phenotypic variability of the p.Arg269HiS variant in the TRPV4 gene

Author

Maria, Jędrzejowska, Emilia, Dębek, Bartłomiej, Kowalczyk, Paulina, Halat, Anna, Kostera-Pruszczyk, Elżbieta, Ciara, Aleksandra, Jezela-Stanek, Małgorzata, Rydzanicz, Piotr, Gasperowicz, and Monika, Gos

Subjects

Adult, Family Health, Male, Heterozygote, TRPV Cation Channels, Arginine, Muscular Atrophy, Spinal, Child, Preschool, Mutation, Humans, Female, Histidine, Creatine Kinase, Transaminases

Abstract

Mutations in the TRPV4 gene are associated with neuromuscular disorders and skeletal dysplasias, which present a phenotypic overlap.Next-generation sequencing and Sanger sequencing were used to analyze the TRPV4 gene.We present 2 Polish families with TRPV4-related disorder harboring the same p.Arg269His mutation. The disease phenotypic expression was extremely variable (from mild scapular winging to severe hypotonia, global weakness, inability to walk unaided, congenital contractures, scoliosis, and respiratory insufficiency), but did not suggest anticipation. The 2 most severely affected patients showed congenital distal contractures of the upper limbs and involvement of cranial nerves (manifesting as facial asymmetry and strabismus). The disease course seemed to be stable, although in later stages it caused respiratory insufficiency and progression of physical disability.The phenotypic variability observed in p.Arg269His carriers suggests that an additional modifier or a more complex pathogenic mechanism exists. Muscle Nerve 59:129-133, 2019.

Published

2017

24. Atypical fibrodysplasia ossificans progressiva diagnosed by whole-exome sequencing

Author

Hao Liu, Sarah L Sawyer, Monika Gos, David Grynspan, Kheirie Issa, Raveena Ramphal, Carmen Rotaru, FORGE Canada Consortium, Jacek Majewski, Kym M Boycott, Gail Graham, and Matthew Bromwich

Subjects

Pediatrics, medicine.medical_specialty, Thyroid Gland, Infantile myofibromatosis, Neonatal onset, ACVR1, Fatal Outcome, Genetics, Humans, Medicine, Exome, Hallux Valgus, Genetics (clinical), Exome sequencing, Respiratory Distress Syndrome, Newborn, Fetal Growth Retardation, Respiratory distress, business.industry, Uterus, Genetic disorder, High-Throughput Nucleotide Sequencing, medicine.disease, Myositis Ossificans, Child, Preschool, Fibrodysplasia ossificans progressiva, Mutation, Female, Heterotopic ossification, business, Activin Receptors, Type I

Abstract

Fibrodysplasia ossificans progressiva (FOP) is a rare genetic disorder characterized by congenital malformations of the great toes and progressive heterotopic ossification of connective tissue that begins during the first decade of life. Our patient presented with intrauterine growth retardation, respiratory distress, neonatal onset soft tissue masses, bilateral hallux valgus, and congenital anomalies of the thyroid and uterus. She was initially diagnosed with atypical infantile myofibromatosis based on clinical and pathological findings. She underwent whole-exome sequencing (WES) as part of the FORGE study to identify the gene for infantile myofibromatosis; however a de novo dominant mutation in ACVR1 (NM_001105.4:c.617G>A) revised the diagnosis to FOP. This patient highlights the utility of WES as an early diagnostic tool in the investigation of patients with unusual presentations of rare diseases, thereby providing clinicians with accurate molecular diagnoses and the opportunity to tailor clinical management to improve patient care.

Published

2015

25. MAP2K2 mutation as a cause of cardio-facio-cutaneous syndrome in an infant with a severe and fatal course of the disease

Author

Monika Gos, Teresa Kaczan, Aleksandra Landowska, Malgorzata Sasiadek, Robert Smigiel, Anna Abramowicz, and Jerzy Bal

Subjects

0301 basic medicine, Heart Defects, Congenital, Pediatrics, medicine.medical_specialty, Polyhydramnios, Hyperkeratosis, MAP Kinase Kinase 2, 030105 genetics & heredity, RASopathy, 03 medical and health sciences, 0302 clinical medicine, Fatal Outcome, Ectodermal Dysplasia, 030225 pediatrics, Genetics, medicine, Humans, Genetics (clinical), Pregnancy, business.industry, Infant, Newborn, Facies, medicine.disease, Hypotonia, Failure to Thrive, Phenotype, Premature birth, Failure to thrive, Mutation, Female, medicine.symptom, business, Congenital disorder

Abstract

Cardio-facio-cutaneous syndrome (CFCS), a rare congenital disorder of RASopathies, displays high phenotypic variability. Complications during pregnancy and in the perinatal period are commonly reported. Polyhydramnios is observed in over half of pregnancies and might occur with fetal macrocephaly, macrosomia, and/or heart defects. Premature birth is not uncommon and any complications like respiratory insufficiency, edema, and feeding difficulties are present and might delay accurate clinical diagnosis. Besides neonatal complications, CFCS newborns and later infants have distinctive dysmorphic features usually accompanied by neurological (hypotonia with motor delay, neurocognitive delay) findings. Also, heart defects usually present at birth. Herein, we present the case of a female baby born prematurely from a pregnancy complicated with polyhydramnios, presenting at birth with craniofacial features typical for RASopathies, heart defects, neurological abnormalities, and hyperkeratosis unusual for a neonatal period. Due to the presence of a heart defect and other complications related to premature birth, the course of the disease was severe with a fatal outcome at the age of 9 months. The RASopathy, particularly CFCS, clinical diagnosis was confirmed and de novo p.Phe57Ile mutation in MAP2K2 was identified.

Published

2017

26. Contribution ofRIT1mutations to the pathogenesis of Noonan syndrome: Four new cases and further evidence of heterogeneity

Author

Jarosław Poznański, Jacek Majewski, Jakub Klapecki, Renata Posmyk, Jerzy Bal, Jolanta Wierzba, Małgorzata Piotrowicz, Monika Gos, Ewa Obersztyn, and Somayyeh Fahiminiya

Subjects

Molecular Sequence Data, Biology, RASopathy, medicine.disease_cause, Genetic Heterogeneity, symbols.namesake, Germline mutation, Genetics, medicine, Humans, Amino Acid Sequence, Genetics (clinical), Exome sequencing, Sanger sequencing, Mutation, Base Sequence, Noonan Syndrome, medicine.disease, Molecular biology, PTPN11, ras Proteins, SOS1, symbols, Noonan syndrome

Abstract

Noonan syndrome (NS) is a common developmental disorder presenting with dysmorphic craniofacial features, heart defects, and short stature. It belongs to the group of RASopathies caused by germline mutations in genes encoding proteins involved in the RAS/MAPK signaling pathway. Although mutations in nine genes are known to cause NS, approximately 30% of the cases still have unexplained etiology. To identify the new causative genes, 42 patients with a clinical diagnosis of NS, who had negative results on Sanger sequencing of PTPN11, SOS1, and RAF1 (the most common NS genes), were selected for whole exome sequencing. In two patients, mutations in recently described new NS gene—RIT1 were found (c.244T>G [p.Phe82Val] and c.270G>C [p.Met90Ile]). Further analysis of a larger cohort (n = 64) of NS patients with classic Sanger sequencing revealed the presence of RIT1 mutation c.284G>C (p.Gly95Ala) in two additional patients. All the detected mutations were localized in switch II domain responsible for GTPase activity. The modeling of RIT1 protein structure revealed that the mutated amino acids and their interacting residues are evolutionary conserved and any residue replacement might change the structural stability and/or protein internal dynamics influencing catalytic activity of the protein. It seems that the identified mutations might alter protein function and therefore, the activity of ERK and P38 MAPK pathways, thus underlying the specific phenotype observed in NS patients. Our study independently confirms the role of RIT1 in the pathogenesis of Noonan syndrome. © 2014 Wiley Periodicals, Inc.

Published

2014

27. TrkB expression level correlates with metastatic properties of L1 mouse sarcoma cells cultured in non‐adhesive conditions

Author

J. Miloszewska, Małgorzata Przybyszewska, Paweł Swoboda, H. Trembacz, and Monika Gos

Subjects

Lung Neoplasms, Cell Survival, Blotting, Western, Cell, Biology, Real-Time Polymerase Chain Reaction, Mice, Growth factor receptor, Cell Movement, Cell Line, Tumor, Gene expression, Cell Adhesion, medicine, Animals, Neoplasm Invasiveness, Anoikis, Neoplasm Metastasis, Cell adhesion, Tumor Stem Cell Assay, Oligonucleotide Array Sequence Analysis, Regulation of gene expression, Mice, Inbred BALB C, Membrane Glycoproteins, Sarcoma, Original Articles, Cell Biology, General Medicine, Protein-Tyrosine Kinases, Molecular biology, Neoplasm Proteins, Gene Expression Regulation, Neoplastic, medicine.anatomical_structure, Cell culture, Cancer cell

Abstract

OBJECTIVES: Ability of a cell to survive without adhesion, and to overcome anoikis, is indispensable for malignant cell invasion and metastasis formation. It has previously been shown that TrkB ‐neutrophin growth factor receptor might be involved in suppression of apoptosis, induced by the lack of adhesion. The aim of our study was to analyse changes in expression of genes and proteins as well as in biological properties of cancer cells cultured without adhesion. A mouse sarcoma, stable, adherent L1 cell line, derived from a spontaneously arisen Balb/c mouse lung tumour, was established in vitro. MATERIALS AND METHODS: L1 cells resistant to anoikis were established by culture of L1 cells without adhesion, followed by selection of clones with elevated expression levels of TrkB protein. Biological characteristics of the cells were studied by migration/invasion tests and colony forming assay. Gene expression analysis was performed by with the aid of cDNA Gene Expression Array and Real‐Time PCR. In vivo experiments were conducted in syngeneic Balb/c mice. RESULTS: Significant changes in gene expression, including higher expression level of TrkB, were found in cells that were able to survive without adhesion. Selected TrkB‐expressing clones were found to have higher clonogenicity and invasive potential, formed more colonies in mouse lungs, and induced larger tumours, when injected subcutaneously into Balb/c mice. CONCLUSION: Lack of adhesion induced significant changes in the cancer cells’ behaviour, which may result from alterations in gene and protein expression levels, including changes in anoikis‐connected protein – TrkB.

Published

2013

28. Towards a Better Molecular Diagnosis of FMR1-Related Disorders—A Multiyear Experience from a Reference Lab

Author

Michał Milewski, Jolanta Czekajska, Sylwia Rzonca, Aleksandra Landowska, Tadeusz Mazurczak, Anna Abramowicz, D Maciejko, Jerzy Bal, Monika Gos, Ewa Obersztyn, Daniel Szopa, Danuta Sielska-Rotblum, and Agnieszka Szpecht-Potocka

Subjects

pre-screening PCR, 0301 basic medicine, Pediatrics, medicine.medical_specialty, Fragile x, congenital, hereditary, and neonatal diseases and abnormalities, Ataxia, lcsh:QH426-470, Primary ovarian insufficiency, diagnostic, fragile X syndrome, FXTAS, FXPOI, FMR1, expansion, Southern blot, TP-PCR, Article, 03 medical and health sciences, Genetics, medicine, Genetics (clinical), business.industry, Triplet repeat, medicine.disease, Fmr1 gene, Fragile X syndrome, lcsh:Genetics, 030104 developmental biology, medicine.symptom, business

Abstract

The article summarizes over 20 years of experience of a reference lab in fragile X mental retardation 1 gene (FMR1) molecular analysis in the molecular diagnosis of fragile X spectrum disorders. This includes fragile X syndrome (FXS), fragile X-associated primary ovarian insufficiency (FXPOI) and fragile X-associated tremor/ataxia syndrome (FXTAS), which are three different clinical conditions with the same molecular background. They are all associated with an expansion of CGG repeats in the 5'UTR of FMR1 gene. Until 2016, the FMR1 gene was tested in 9185 individuals with the pre-screening PCR, supplemented with Southern blot analysis and/or Triplet Repeat Primed PCR based method. This approach allowed us to confirm the diagnosis of FXS, FXPOI FXTAS in 636/9131 (6.96%), 4/43 (9.3%) and 3/11 (27.3%) of the studied cases, respectively. Moreover, the FXS carrier status was established in 389 individuals. The technical aspect of the molecular analysis is very important in diagnosis of FXS-related disorders. The new methods were subsequently implemented in our laboratory. This allowed the significance of the Southern blot technique to be decreased until its complete withdrawal. Our experience points out the necessity of implementation of the GeneScan based methods to simplify the testing procedure as well as to obtain more information for the patient, especially if TP-PCR based methods are used.

Published

2016

29. Novel Col12A1 variant expands the clinical picture of congenital myopathies with extracellular matrix defects

Author

Jaya, Punetha, Akanchha, Kesari, Eric P, Hoffman, Monika, Gos, Anna, Kamińska, Anna, Kostera-Pruszczyk, Irena, Hausmanowa-Petrusewicz, Ying, Hu, Yaqun, Zou, Carsten G, Bönnemann, and Maria, JȨdrzejowska

Subjects

Collagen Type XII, Muscular Diseases, Humans, Female, Child, Polymorphism, Single Nucleotide, Article, Extracellular Matrix

Abstract

Mutations in the COL12A1 (collagen, type XII, alpha 1) gene have been described in a milder Bethlem-like myopathy in 6 patients from 3 families (dominant missense), and in a severe congenital form with failure to attain ambulation in 2 patients in a single pedigree (recessive loss-of-function).We describe an 8-year-old girl of Polish origin who presented with profound hypotonia and joint hyperlaxity at birth after a pregnancy complicated by oligohydramnios and intrauterine growth retardation.We identified a novel, potentially pathogenic heterozygous missense COL12A1 c.8329GC (p.Gly2777Arg) variant using a targeted sequencing panel. Patient fibroblast studies confirmed intracellular retention of the COL12A1 protein, consistent with a dominant-negative mutation.As our patient showed a more intermediate phenotype, this case expands the phenotypic spectrum for COL12A1 disorders. So far, COL12A1 disorders seem to cover much of the severity range of an Ehlers-Danlos/Bethlem-like myopathy overlap syndrome associated with both connective tissue abnormalities and muscle weakness. Muscle Nerve 55: 277-281, 2017.

Published

2016

30. Genetic analysis in inherited metabolic disorders--from diagnosis to treatment. Own experience, current state of knowledge and perspectives

Author

Katarzyna, Wertheim-Tysarowska, Monika, Gos, Jolanta, Sykut-Cegielska, and Jerzy, Bal

Subjects

Neonatal Screening, Rare Diseases, Risk Factors, Incidence, Infant, Newborn, Humans, Genetic Testing, Metabolism, Inborn Errors

Abstract

Inherited metabolic disorders, also referred to as inborn errors of metabolism (IEM), are a group of congenital disorders caused by mutation in genomic or mitochondrial DNA. IEM are mostly rare disorders with incidence ranging from 1/50,000-1/150,000), however in total IEM may affect even 1/1000 people. A particular mutation affects specific protein or enzyme that improper function leads to alterations in specific metabolic pathway. Inborn errors of metabolism are monogenic disorders that can be inherited in autosomal recessive manner or, less frequently, in autosomal dominant or X-linked patterns. Some exceptions to Mendelian rules of inheritance have also been described. Vast majority of mutations responsible for IEM are small DNA changes affecting single or several nucleotides, although larger rearrangements were also identified. Therefore, the methods used for the identification of pathogenic mutations are mainly based on molecular techniques, preferably on Sanger sequencing. Moreover, the next generation sequencing technique seems to be another prospective method that can be successfully implemented for the diagnosis of inborn errors of metabolism. The identification of the genetic defect underlying the disease is not only indispensable for genetic counseling, but also might be necessary to apply appropriate treatment to the patient. Therapeutic strategies for IEM are continuously elaborated and tested (eg. enzyme replacement therapy, specific cells or organ transplantation or gene therapy, both in vivo and ex vivo) and have already been implemented for several disorders. In this article we present current knowledge about various aspects of IEM on the basis of our own experience and literature review.

Published

2016

31. Application of array comparative genomic hybridization in 102 patients with epilepsy and additional neurodevelopmental disorders

Author

Anetta Jeziorek, Mariola Rudzka-Dybała, Iwona Terczyńska, Marta Kędzior, Małgorzata Sobierajewicz, Elżbieta Szczepanik, Zofia Zalewska-Miszkurka, Kamila Ziemkiewicz, Tomasz Mazurczak, Alicja Goszczańska-Ciuchta, Dorota Antczak-Marach, Magdalena Bartnik, Maciej Sykulski, Anna Gambin, Katarzyna Derwińska, Hanna Mazurkiewicz, Tomasz Gambin, Tadeusz Mazurczak, Chad A. Shaw, Barbara Wiśniowiecka-Kowalnik, Hanna Mierzewska, Dorota Hoffman-Zacharska, Monika Gos, Ewa Bocian, Ewa Obersztyn, and Pawel Stankiewicz

Subjects

Male, congenital, hereditary, and neonatal diseases and abnormalities, Candidate gene, Adolescent, DNA Copy Number Variations, endocrine system diseases, Microarray, Developmental Disabilities, Gene Dosage, Biology, Cellular and Molecular Neuroscience, Epilepsy, KCNJ3, Intellectual Disability, mental disorders, medicine, Humans, Copy-number variation, Autistic Disorder, Child, Genetics (clinical), Genetics, Comparative Genomic Hybridization, Genome, Human, Infant, Exons, medicine.disease, Psychiatry and Mental health, Child, Preschool, biology.protein, Autism, Comparative genomic hybridization, CDH15

Abstract

Copy-number variants (CNVs) collectively represent an important cause of neurodevelopmental disorders such as developmental delay (DD)/intellectual disability (ID), autism, and epilepsy. In contrast to DD/ID, for which the application of microarray techniques enables detection of pathogenic CNVs in ∼10–20% of patients, there are only few studies of the role of CNVs in epilepsy and genetic etiology in the vast majority of cases remains unknown. We have applied whole-genome exon-targeted oligonucleotide array comparative genomic hybridization (array CGH) to a cohort of 102 patients with various types of epilepsy with or without additional neurodevelopmental abnormalities. Chromosomal microarray analysis revealed 24 non-polymorphic CNVs in 23 patients, among which 10 CNVs are known to be clinically relevant. Two rare deletions in 2q24.1q24.3, including KCNJ3 and 9q21.13 are novel pathogenic genetic loci and 12 CNVs are of unknown clinical significance. Our results further support the notion that rare CNVs can cause different types of epilepsy, emphasize the efficiency of detecting novel candidate genes by whole-genome array CGH, and suggest that the clinical application of array CGH should be extended to patients with unexplained epilepsies. © 2012 Wiley Periodicals, Inc.

Published

2012

32. Mouse sarcoma L1 cell line holoclones have a stemness signature

Author

H. Trembacz, P. Janik, Małgorzata Przybyszewska, M. Koronkiewicz, Monika Gos, and J. Miloszewska

Subjects

medicine.diagnostic_test, Cell Biology, General Medicine, Biology, medicine.disease, In vitro, Flow cytometry, Side population, Cancer stem cell, Cell culture, Immunology, medicine, Cancer research, MTT assay, Sarcoma, Clonogenic assay

Abstract

Accumulating data suggest that cancers contain a fraction of cells called cancer stem cells (CSCs), that may be responsible for upkeep and relapses of disease. In experimental settings, CSCs are regarded as most effective at tumour initiation in in vivo assays. Since the first isolation of cancer stem cells from acute myeloid leukaemia in 1994, cancer stem cells have been identified in human solid tumours and they have also been found in the established cell lines, based on ability of CSCs to form in vitro colonies of a specific morphology, called holoclones. Our study examined the ability of a mouse sarcoma cell line, derived from a lung metastasis of a BALB/c mouse and established as a stably growing line (L1), to produce holoclones in vitro. We aimed to verify a stemness signature of the holoclone cells. The L1 cell line was found to form holoclone colonies in vitro, which were shown to contain a percentage of CSC-like cells. A fraction of the L1 cells was able to repopulate the original cell line, and presented an increased clonogenic and metastatic potential (18th passage). In addition, MTT assay and flow cytometry of the side population fraction revealed that these cells were more resistant to chemotherapeutic drugs than the original cell line, and over-expressed the anti-apoptotic genes, GRP78 and GADD153. We conclude that mouse L1 sarcoma cell line contains CSC-like cells.

Published

2010

33. Identification of mutations in theNF2 gene in Polish patients with neurofibromatosis type 2

Author

Mikołaj Łaniewski-Wołłk, Andrzej Koziarski, Monika Gos, and Agnieszka Szpecht-Potocka

Subjects

Adult, Male, Neurofibromatosis 2, Adolescent, Loss of Heterozygosity, Biology, medicine.disease_cause, Polymerase Chain Reaction, Loss of heterozygosity, Germline mutation, otorhinolaryngologic diseases, Genetics, medicine, Humans, Neurofibromatosis type 2, Neurofibromatosis, Child, Gene, Germ-Line Mutation, Polymorphism, Single-Stranded Conformational, Mutation, Point mutation, Infant, Newborn, Infant, General Medicine, Middle Aged, medicine.disease, Human genetics, Child, Preschool, Cancer research, Female, Poland

Abstract

Point mutation and loss of heterozygosity (LOH) analyses were performed in 12 Polish patients with a classic symptom of NF2 — bilateral vestibular schwannomas (BVS). In 5 patients (41.7%), germline mutations were found in theNF2 gene: 2 previously reported substitutions (c.592C>T and c.52C>T) and 3 novel mutations (c.1001_1002insG, c.1029_1030insCC, c.774_778dupGAATG). In addition, LOH analysis of 30 tumour samples from 10 patients revealed a molecular basis of NF2 in 3 patients (25%) that did not have any germline mutation. The molecular defects in sporadic cases of NF2 are still being discussed.

Published

2008

34. Rare variants in SOS2 and LZTR1 are associated with Noonan syndrome

Author

Ingrid Cristian, Alexsandra C. Malaquias, Jacek Majewski, Michelle Buscarilli, Meire Aguena, Alexandre C. Pereira, Michel S Naslavsky, Olaf Bodamer, Débora Romeo Bertola, Anna Abramowicz, Guilherme L. Yamamoto, Mayana Zatz, Maria Rita Passos-Bueno, Alexander A. L. Jorge, Monika Gos, Chong Ae Kim, Christina Hung, Somayyeh Fahiminiya, and Jacek Pilch

Subjects

Proband, MAPK/ERK pathway, Male, Biology, Cohort Studies, Genetic variation, Genetics, medicine, Missense mutation, Humans, Gene, Genetics (clinical), Genetic Association Studies, Noonan Syndrome, Facies, Genetic Variation, medicine.disease, Phenotype, Pedigree, Son of Sevenless Proteins, SOS1, ras Proteins, Noonan syndrome, Female, Mitogen-Activated Protein Kinases, Signal Transduction, Transcription Factors

Abstract

Background Noonan syndrome is an autosomal dominant, multisystemic disorder caused by dysregulation of the RAS/mitogen activated protein kinase (MAPK) pathway. Heterozygous, pathogenic variants in 11 known genes account for approximately 80% of cases. The identification of novel genes associated with Noonan syndrome has become increasingly challenging, since they might be responsible for very small fractions of the cases. Methods A cohort of 50 Brazilian probands negative for pathogenic variants in the known genes associated with Noonan syndrome was tested through whole-exome sequencing along with the relatives in the familial cases. Families from the USA and Poland with mutations in the newly identified genes were included subsequently. Results We identified rare, segregating or de novo missense variants in SOS2 and LZTR1 in 4% and 8%, respectively, of the 50 Brazilian probands. SOS2 and LZTR1 variants were also found to segregate in one American and one Polish family. Notably, SOS2 variants were identified in patients with marked ectodermal involvement, similar to patients with SOS1 mutations. Conclusions We identified two novel genes, SOS2 and LZTR1 , associated with Noonan syndrome, thereby expanding the molecular spectrum of RASopathies. Mutations in these genes are responsible for approximately 3% of all patients with Noonan syndrome. While SOS2 is a natural candidate, because of its homology with SOS1 , the functional role of LZTR1 in the RAS/MAPK pathway is not known, and it could not have been identified without the large pedigrees. Additional functional studies are needed to elucidate the role of LZTR1 in RAS/MAPK signalling and in the pathogenesis of Noonan syndrome.

Published

2015

35. Unusual Cyclin D1 Positive Marginal Zone Lymphoma of Mediastinum

Author

Ewa Paszkiewicz-Kozik, P. Janik, Jan Walewski, Konrad Ptaszyński, Renata Woroniecka, Małgorzata Czarnocka, Katarzyna Blachnio, Grzegorz Rymkiewicz, Paweł Swoboda, Barbara Pienkowska-Grela, and Monika Gos

Subjects

Adult, Cancer Research, medicine.medical_specialty, Pathology, Lymphoma, Mantle-Cell, Biology, Mediastinal Neoplasms, Models, Biological, Translocation, Genetic, Immunophenotyping, Cyclin D1, Internal medicine, medicine, Humans, In Situ Hybridization, Fluorescence, B cell, Hematology, medicine.diagnostic_test, Lymphoma, B-Cell, Marginal Zone, General Medicine, Flow Cytometry, medicine.disease, Immunohistochemistry, Lymphoma, Gene Expression Regulation, Neoplastic, medicine.anatomical_structure, Oncology, Cancer research, Female, Mantle cell lymphoma, Histopathology, Fluorescence in situ hybridization

Abstract

We report a case of 43-yr-old Caucasian female with an unusual, cyclin D1 positive marginal zone lymphoma (MZL) of mucosa-associated lymphoid tissue (MALT) type of the mediastinum. To date, only about 30 cases of this entity have been published. They occur mainly in Asian females with a history of coexisting autoimmune disease. To our knowledge, this is the first case of mediastinal MZL with cyclin D1 expression. In the span of 6 yr this patient's tumor recurred three times, was surgically treated, and initially diagnosed as paraganglioma. The diagnosis was based on histopathological examination only. Our final diagnosis of MZL was made by combined evaluation of histopathology (HP), immunohistochemistry (IH), flow cytometry (FCM), fluorescence in situ hybridization (FISH), and molecular biology studies. We found a positive cyclin D1 reaction by IH and cyclin D1 mRNA (CCND1) overexpression by reverse transcription polymerase chain reaction (RT-PCR). Very high cyclin D1 to beta-actin mRNA ratio in this case was comparable with the ratio, characteristic for mantle cell lymphoma (MCL). However, there was no translocation t(11;14) found by FISH and an immunophenotype by IH and FCM was consistent with MZL ruling out MCL diagnosis. In addition, our case differs from other, previously reported thymic MZL lymphoma cases by no autoimmune disease association, Caucasian origin, and the absence of the plasmacytic differentiation on both HP/IH.

Published

2006

36. Cellular quiescence induced by contact inhibition or serum withdrawal in C3H10T1/2 cells

Author

H. Trembacz, P. Janik, Monika Gos, Paweł Swoboda, J. Skierski, and J. Miloszewska

Subjects

Ubiquitin-Protein Ligases, EGR1, Biology, Culture Media, Serum-Free, Cell Line, Mice, Antigen, Gene expression, Animals, Cell Proliferation, Oligonucleotide Array Sequence Analysis, Mice, Inbred C3H, Confluency, Contact Inhibition, Gene Expression Profiling, Tumor Suppressor Proteins, Cell Cycle, Contact inhibition, Original Articles, Cell Biology, General Medicine, Fibroblasts, Molecular biology, Gene expression profiling, Urokinase receptor, Ki-67 Antigen, Gene Expression Regulation, Von Hippel-Lindau Tumor Suppressor Protein, Cell culture

Abstract

Either confluence or serum withdrawal may cause growth arrest of cultured non‐transformed cells. Here, we compared sparsely populated and confluent C3H10T1/2 cells with and without serum‐containing medium. The following proliferation‐relevant end points were examined: cell‐cycle distribution, Ki‐67 antigen presence, the level of the von Hippel‐Lindau (VHL) protein, and gene expression, determined using a microarray approach. In sparse/logarithmic cultures, the fraction of cells in G(0)/G(1) phase increased from 55 to 85% following serum withdrawal. Moreover, the fraction of Ki‐67 positive cells dropped from 89 to 47%. In confluent cultures, the majority of cells (80%) were in G(0)/G(1) phase and only 25–30% were Ki‐67 positive, regardless of serum presence. In both serum‐deprived and contact‐inhibited cultures, significant and distinct changes in gene expression were observed. Serum deprivation of sparsely cultured cells resulted in significant over‐expression of several transcription factors, while confluent cells showed elevated expression of genes coding for Wnt6, uPar, Tdag51, Egr1, Ini1a and Mor1. These results indicate that contact inhibition and serum withdrawal lead to cellular quiescence through distinct genetic and molecular mechanisms.

Published

2005

37. Mantle Cell Lymphoma Presenting with Paraproteinemia

Author

Grzegorz Rymkiewicz, Paweł Swoboda, Monika Gos, P. Janik, Marika Kulińska, Katarzyna Blachnio, Renata Woroniecka, Barbara Pienkowska-Grela, Anna Borawska, and Jan Walewski

Subjects

Cancer Research, medicine.medical_specialty, Paraproteinemia, Pathology, Paraproteinemias, Lymphoma, Mantle-Cell, Flow cytometry, Diagnosis, Differential, Cyclin D1, immune system diseases, hemic and lymphatic diseases, Internal medicine, Humans, Medicine, Hematology, medicine.diagnostic_test, Reverse Transcriptase Polymerase Chain Reaction, business.industry, Macroglobulinemia, DNA, Neoplasm, General Medicine, Middle Aged, Flow Cytometry, medicine.disease, Immunoglobulin M, Oncology, Immunohistochemistry, Female, Mantle cell lymphoma, business, Fluorescence in situ hybridization

Abstract

Mantle cell lymphoma (MCL) is most frequently diagnosed by the routine histological (HP) and immunohistochemical (IH) examination. Herein we present a case of 47-yr-old female with general lymphadenopathy and leukemic blood picture. She was initially diagnosed with marginal zone lymphoma (MZL). This diagnosis was based not only on the HP/IH examination but also on the presence of IgM paraproteinemia. Flow cytometry (FCM) examination was helpful in making of the final diagnosis of MCL. Fluorescence in situ hybridization and cyclin D1 mRNA detection by RT-PCR additionally confirmed the MCL diagnosis. The IgM paraproteinemia is rare in MCL, although is a common feature of lymphoplasmacytoid lymphomas (LPL) and is considered a major characteristic of Waldenström's macroglobulinemia (WM).

Published

2005

38. Evaluation of Encapsulation Potential of Selected Star-Hyperbranched Polyglycidol Architectures: Predictive Molecular Dynamics Simulations and Experimental Validation

Author

Mateusz Gosecki, Malgorzata Urbaniak, Nuno Martinho, Monika Gosecka, and Mire Zloh

Subjects

hydrophobic drug, encapsulation, molecular dynamics simulation, clotrimazole, unimolecular micelles, star-hyperbranched copolymer, Organic chemistry, QD241-441

Abstract

Polymers, including non-linear copolymers, have great potential in the development of drug delivery systems with many advantages, but the design requires optimizing polymer–drug interactions. Molecular dynamics (MD) simulations can provide insights into polymer–drug interactions for designing delivery systems, but mimicking formulation processes such as drying is often not included in in silico studies. This study demonstrates an MD approach to model drying of systems comprising either hydrophilic tinidazole or hydrophobic clotrimazole drugs with amphiphilic hyperbranched copolyethers. The simulated drying protocol was critical for elucidating drug encapsulation and binding mechanisms. Experimentally, two polymers were synthesized and shown to encapsulate clotrimazole with up to 83% efficiency, guided by interactions with the hydrophobic core observed in simulations. In contrast, tinidazole is associated with surface regions, indicating capacity differences between drug types. Overall, this work highlights MD simulation of the drying process as an important tool for predicting drug–polymer complex behaviour. The modelled formulation protocol enabled high encapsulation efficiency and opened possibilities for the design of delivery systems based on computationally derived binding mechanisms. This demonstrates a computational–experimental approach where simulated drying was integral to elucidating interactions and developing optimized complexes, emphasizing the value of molecular modelling for the development of drug delivery formulations.

Published

2023

39. Broad clinical spectrum observed in patients with scapuloperoneal spinal muscular atrophy (SPSMA) caused by an c.806G > A (p. Arg269His) mutation in the TRPV4 gene

Author

P. Halat, A. Jezela-Stanek, Monika Gos, M. Rydzanicz, E. Ciara, Piotr Gasperowicz, E. Dębek, Anna Kostera-Pruszczyk, and Maria Jędrzejowska

Subjects

Scapuloperoneal spinal muscular atrophy, Pathology, medicine.medical_specialty, Neurology, TRPV4 gene, business.industry, Pediatrics, Perinatology and Child Health, Mutation (genetic algorithm), Medicine, In patient, Neurology (clinical), business, Genetics (clinical)

Published

2017

40. P2.01-004 The Methylation Profiling of Multiple Tumor Suppressor Genes in Plasma Cell-Free DNA of Patients with NSCLC vs Benign Tumors

Author

Mateusz Florczuk, Kazimierz Roszkowski-Sliz, Dorota Giedronowicz, Michal Komorowski, Piotr Rudzinski, Wlodzimierz Kupis, Jolanta Zaleska, Joanna Chorostowska-Wynimko, Aleksandra Landowska, Monika Gos, Tadeusz Orłowski, Adam Szpechcinski, and Renata Langfort

Subjects

Pulmonary and Respiratory Medicine, business.industry, Cancer, Plasma cell, medicine.disease, Free dna, law.invention, medicine.anatomical_structure, Oncology, Methylation profiling, law, medicine, Cancer research, Suppressor, Multiple tumors, Topic analysis, business, Gene

Published

2017

41. Neurofibromin in neurofibromatosis type 1 - mutations in NF1gene as a cause of disease

Author

Anna, Abramowicz and Monika, Gos

Subjects

Neurofibromatosis 1, Neurofibromin 1, Cafe-au-Lait Spots, Mutation, ras Proteins, Humans, Point Mutation, Mitogen-Activated Protein Kinases, Gene Deletion, Signal Transduction

Abstract

Neurofibromatosis type I (NF1) is a disease associated with the presence of benign neurofibromas and malignant tumours of the central and peripheral nervous system, that are accompanied by characteristic changes in the skin, such as café-au-lait spots or axillary freckling. In 50% of NF1 patients, the clinical symptoms become apparent below 1st year and in 97%, before the age of 8 years. The disease is mainly caused by the presence of mutation in the NF1 gene that encodes neurofibromin - a protein involved in the regulation of several cellular signaling pathways responsible for cell proliferation and differentiation. Neurofibromin is necessary for embryonic development and involved mainly in the differentiation of neural crest derived cells, mesenchymal cells, neural cells, melanocytes and bone cells. Type I neurofibromatosis is inherited in autosomal dominant manner, nevertheless about 50% of detected mutations are de novo ones. The mutations have full penetrance, although they also have significant pleiotropic effect. Over 1485 different mutations have been identified in the NF1 gene so far, most of which lead to a synthesis of truncated, non-functional protein. It is estimated that the point mutations are responsible for approximately 90% of cases of NF1. The remaining 5-7% of NF1 cases are associated with the presence of a single exon or whole NF1 gene deletion (17q11.2 microdeletion syndrome). The article discusses the role of neurofibromin in cell signaling with the special attention to RAS/MAPK pathway regulation as well as in organism development. Also the basic methods of molecular analysis of NF1 gene are presented in the context of their application in the diagnosis and clinical differentiation of the disease.

Published

2014

42. The RASopathies as an example of RAS/MAPK pathway disturbances - clinical presentation and molecular pathogenesis of selected syndromes

Author

Natalia, Bezniakow, Monika, Gos, and Ewa, Obersztyn

Subjects

Heart Defects, Congenital, Neurofibromatosis 1, MAP Kinase Signaling System, Costello Syndrome, Noonan Syndrome, Port-Wine Stain, Facies, Capillaries, Failure to Thrive, Arteriovenous Malformations, Craniofacial Abnormalities, Ectodermal Dysplasia, LEOPARD Syndrome, ras Proteins, Humans, Mitogen-Activated Protein Kinases, Germ-Line Mutation, Signal Transduction

Abstract

The RASopathies are a class of developmental syndromes. Each of them exhibits distinctive phenotypic features, although there are numerous overlapping clinical manifestations that include: dysmorphic craniofacial features, congenital cardiac defects, skin abnormalities, varying degrees of intellectual disability and increased risk of malignancies. These disorders include: Noonan syndrome, Costello syndrome, LEOPARD syndrome, cardio-facio-cutaneous syndrome (CFC), capillary malformation-arteriovenous malformation syndrome (CM-AVM), Legius syndrome and neurofibromatosis type 1 (NF1). The RASopathies are associated with the presence of germline mutation in genes encoding specific proteins of the RAS/mitogen - activated protein kinase (MAPK) pathway that plays a crucial role in embryonic and postnatal development. In this review, we present the clinical and molecular features of selected syndromes from the RASopathies group.

Published

2014

43. Rett-like onset in late-infantile neuronal ceroid lipofuscinosis (CLN7) caused by compound heterozygous mutation in the MFSD8 gene and review of the literature data on clinical onset signs

Author

Dorota Hoffman-Zacharska, Nahid Nahavandi, Mihaela Gherghiceanu, Monika Gos, Catrinel Iliescu, Alice Dica, Mihai Craiu, Dana Craiu, Octavia Dragostin, Alexandra Bastian, and Arndt Rolfs

Subjects

Parents, Pediatrics, medicine.medical_specialty, Microcephaly, Heterozygote, Developmental Disabilities, Rett syndrome, Gene mutation, Compound heterozygosity, Blindness, MECP2, Neuronal Ceroid-Lipofuscinoses, Seizures, medicine, Rett Syndrome, Humans, Age of Onset, Child, Genetics, business.industry, Membrane Transport Proteins, Electroencephalography, General Medicine, medicine.disease, Magnetic Resonance Imaging, Pediatrics, Perinatology and Child Health, Mutation, Disease Progression, Neuronal ceroid lipofuscinosis, Ataxia, Female, Neurology (clinical), Age of onset, business, Lysosomes, Developmental regression

Abstract

Background We present clinical and molecular findings of a patient with ceroid-lipofuscinosis CLN7, with a compound heterozygous mutation of the MFSD8 gene, with Rett syndrome clinical signs onset and a later development of full picture of vLINCL. Case presentation A 7 years-old female patient with normal development until the age 12 months, developed Rett like clinical picture (psychomotor regression, microcephaly, stereotypic hands movements in the midline, hyperventilation episodes) present at the onset of her condition (age 18 months), features still present at the initial evaluation in our clinic at age 5 years. Results MECP2 (methyl CpG binding protein 2) gene mutation was negative. At age 6 years she was readmitted for severe ataxia and blindness, seizures, and severe developmental regression leading to NCL (neuronal ceroid lipofuscinosis) suspicion. EEG showed slow background with IRDA (intermittent rhythmic delta activity). A conjunctive biopsy showed abnormal curvilinear and fingerprint lysosomal deposits, and genetic analysis revealed two heterozygous mutations of MFSD8 gene (c.881C > A p.Thr294Lys and c.754 + 2T > A) each inherited from carrier parents and a heterozygous variant (c.470A>C p.Asp157Ala) of CLN5 gene. Conclusion NCL should be suspected and MFSD8 genetic testing should also be considered in patients with Rett like phenotype at onset and negative MECP2 mutation. Such cases should be carefully and frequently re-evaluated in order to avoid delayed diagnosis and offer proper genetic advice to the family. In our knowledge, this might be the first case of CLN7 disease with Rett like onset described in the literature, which developed typical vLINCL clinical phenotype after age 5.5 years. A short review of the literature showing NCL onset modalities is presented.

Published

2014

44. Severe phenotypes of SMARD1 associated with novel mutations of the IGHMBP2 gene and nuclear degeneration of muscle and Schwann cells

Author

Tomasz Kmieć, Ewa Pronicka, Iwona Walczak-Wojtkowska, Monika Gos, Maciej Pronicki, Elżbieta Konopka, Maria Jędrzejowska, Hanna Mierzewska, Magdalena Mierzewska-Schmidt, Irena Hausmanowa-Petrusewicz, Ewa Obersztyn, Marek Migdał, Anna Fidziańska, and Agnieszka Madej-Pilarczyk

Subjects

Male, Pathology, medicine.medical_specialty, Nonsense mutation, Degeneration (medical), medicine.disease_cause, Polymerase Chain Reaction, Muscular Atrophy, Spinal, medicine, Missense mutation, Myocyte, Humans, Muscle, Skeletal, Cell Nucleus, Mutation, Respiratory Distress Syndrome, Newborn, Muscle biopsy, medicine.diagnostic_test, business.industry, Infant, Newborn, General Medicine, Spinal muscular atrophy, medicine.disease, Hypotonia, Pedigree, DNA-Binding Proteins, Pediatrics, Perinatology and Child Health, Female, Neurology (clinical), Schwann Cells, medicine.symptom, business, Transcription Factors

Abstract

Spinal muscular atrophy with respiratory distress type 1 (SMARD1) is a very rare autosomal recessive form of spinal muscular atrophy manifested in low birth weight, diaphragmatic palsy and distal muscular atrophy. Caused by a mutation in the IGHMBP2 gene, the disease is addressed here by reference to five Polish patients in which SMARD1 has been confirmed genetically. All presented a severe form of the disease and had evident symptoms during the second month of life; with four displaying weak cries, feeding difficulties and hypotonia from birth. Two were afflicted by severe dysfunction of the autonomic nervous system. Ultrastructural analysis of a muscle biopsy revealed progressive degeneration within the nuclei of the muscle cells and Schwann cells. Neuromuscular junctions were also defective. It proved possible to identify in our patients 6 novel IGHMBP2 mutations: three missense (c.595G>C, c.1682T>C and c.1794C>A), two nonsense (c.94C>T and c.1336C>T) and one in-frame deletion (c.1615_1623del). One nonsense mutation (c.429C>T) that had been described previously was also identified. Observation of our patients makes it clear that clinical picture is still the most important factor suggesting diagnosis of SMARD1, though further investigations concerning some of the symptoms are required. As the IGHMBP2 gene is characterized by significant heterogeneity, genetic counseling of affected families is rendered more complex. IGHMBP2 protein deficiency can lead to the degeneration of nuclei, in both muscle and Schwann cells.

Published

2013

45. [RAS/MAPK signal transduction pathway and its role in the pathogenesis of Noonan syndrome]

Author

Monika, Gos, Monika, Leszkiewicz, and Anna, Abramowicz

Subjects

Genes, ras, MAP Kinase Signaling System, Mutation, Noonan Syndrome, Humans

Abstract

Noonan syndrome (NS) is one of the most frequent dysmorphic syndromes in children with a frequency of 1/1000-1/2500 of newborns. Noonan syndrome is a multi-organ disease with a broad spectrum of clinical symptoms. The most characteristic features of NS are: craniofacial dysmorphy, short stature, cardiovascular defects, bone and skeletal defects and delayed puberty (cryptorchidism in males). Noonan syndrome has a genetic background and is inherited in autosomal dominant manner. The recent studies have shown that it is due to the presence of mutation in one of the genes encoding proteins of RAS/MAPK signalling pathway responsible for cell proliferation and differentiation. Till now, NS causing mutations were identified in PTPN11, SOS1, RAF1, KRAS, BRAF, SHOC2 and NRAS genes, and this may partially explain the broad phenotypic spectrum observed in patients. Noonan syndrome is one of the RAS-opathies, therefore the molecular analysis of RAS/ MAPK genes might be a very useful tool in clinical differentiation of the disease.

Published

2013

46. [Inherited skin diseases - a review of selected genodermatoses]

Author

Katarzyna, Wertheim-Tysarowska, Monika, Gos, Katarzyna, Niepokój, and Cezary, Kowalewski

Subjects

Neurofibromatosis 1, Skin Neoplasms, Mutation, Humans, Apoptosis, Skin Pigmentation, Epidermolysis Bullosa, Pigmentation Disorders, Skin Diseases, Cell Proliferation

Abstract

Inherited distubances in skin structure and its function are the main cause of diseases classified as genodermatoses. The following clinical entities are classified as genodermatoses: epidermolysis bullosa, keratotic disorders, disorders of skin color, ectodermal genodermatoses, genodermatoses associated with connective tissue, vascular genodermatoses and genodermatoses with skin manifestation and elevated cancer risk. One of the most clinically heterogenous group of genodermatoses, is epidermolysis bullosa. Four main subtypes were described: simplex, dystrophic, junctional and Kindler syndrome. These diseases are caused by mutations in the genes encoding proteins forming junctions between the dermis and epidermis (eg. COL7A1, COL17A1, KRT14, KRT5 or genes coding for 332 laminin). They are inherited in an autosomal recessive or dominant manner. The disease that is inherited as a dominant, sex dependent trait, is incontinenia pigmenti (Bloch-Sulzberger syndrome) characterized by the presence of extensive pigmentation changes already in the neonatal period. In patients with incontinenia pigmenti, mutations in the NEMO gene are found. The protein encoded by NEMO is involved in the negative regulation of activity of the NFκB transcription factor that is responsible for apoptosis and cell proliferation control. In the regulation of cell proliferation, the neurofibromin (NF1) - the suppressor of RAS/MAPK signaling pathway activity, is also involved. The mutations in the NF1 gene are identified in neurofibromatosis type I - a genodermatosis with higher risk of cancer development and tumor formation. Herein, a review of selected genodermatoses in the context of their molecular pathology is presented.

Published

2013

47. A novel COL12A1 variant expands the clinical picture for a collagen XII-related myopathy

Author

Maria Jędrzejowska, Monika Gos, Anna Kamińska, Eric P. Hoffman, Jaya Punetha, Carsten G. Bönnemann, Yaqun Zou, Anna Kostera-Pruszczyk, Ying Hu, and Akanchha Kesari

Subjects

Pathology, medicine.medical_specialty, Collagen xii, Neurology, business.industry, Pediatrics, Perinatology and Child Health, medicine, Neurology (clinical), medicine.symptom, Myopathy, business, Genetics (clinical)

Published

2016

48. Introduction

Author

Monika Gosin

Published

2019

49. Title Page, Copyright

Author

Monika Gosin

Published

2019

50. Acknowledgments

Author

Monika Gosin

Published

2019