Your search keyword '"Baiba Lace"' showing total 67 results

1. The phenotypic spectrum of PTCD3 deficiency

Author

Baiba Lace, Eissa Faqeih, Namik Kaya, Zita Krumina, Johannes A. Mayr, Ieva Micule, Nathan Thompson Wright, Melanie T. Achleitner, Hanan AlQudairy, Sander Pajusalu, Janis Stavusis, Pawel Zayakin, and Inna Inashkina

Subjects

Leigh‐like syndrome, pentatricopeptide repeat, PTCD3, Diseases of the endocrine glands. Clinical endocrinology, RC648-665, Genetics, QH426-470

Abstract

Abstract The PTCD3 gene product (protein PTCD3 or MRPS39) forms the entry channel of the mitochondrial small ribosomal subunit and binds to single‐stranded mRNA. Here, we expand on the clinical manifestations of PTCD3 pathogenic variants by describing an early‐onset patient with Leigh‐like syndrome and two patients with milder form of disease, with combined oxidative phosphorylation deficiency. A 34‐year‐old male and his 33‐year‐old sister both have horizontal nystagmus, pronounced rough tremor, truncal ataxia, dysmetria, spasticity and hyperreflexia. The basal respiration rate decreased significantly for the male patient and his mother (p A, p.(Tyr394Ter) and c.805C>T, p.(His269Tyr). Tyr394Ter variant ablates the C‐terminal half of the protein, including a significant portion of the central fold. In silico modelling for the variant His269Tyr shows that the inclusion of the slightly larger tyrosine sidechain is well tolerated, with no significant change in either the position or the movement of the surrounding area. The third case is a 9‐year‐old boy, who has a global developmental delay, central hypotonia, hyperreflexia and abnormal MRI. PTCD3 pathogenic variant c.538+4A>G was identified by whole exome sequencing. To test the variant's effect on splicing, an RT‐PCR experiment was performed, which revealed skipping of an out‐of‐frame exon 7.

Published

2024

2. Unraveling the Pathogenetic Mechanisms Underlying the Association between Specific Mitochondrial DNA Haplogroups and Parkinson’s Disease

Author

Min-Yu Lan, Tsu-Kung Lin, Baiba Lace, Algirdas Utkus, Birute Burnyte, Kristina Grigalioniene, Yu-Han Lin, Inna Inashkina, and Chia-Wei Liou

Subjects

Parkinson’s disease, mitochondrial haplogroup, cybrid, transcriptome, unfolding protein response, Cytology, QH573-671

Abstract

Variants of mitochondrial DNA (mtDNA) have been identified as risk factors for the development of Parkinson’s disease (PD). However, the underlying pathogenetic mechanisms remain unclear. Cybrid models carrying various genotypes of mtDNA variants were tested for resistance to PD-simulating MPP+ treatment. The most resistant line was selected for transcriptome profiling, revealing specific genes potentially influencing the resistant characteristic. We then conducted protein validation and molecular biological studies to validate the related pathways as the influential factor. Cybrids carrying the W3 mtDNA haplogroup demonstrated the most resistance to the MPP+ treatment. In the transcriptome study, PPP1R15A was identified, while further study noted elevated expressions of the coding protein GADD34 across all cybrids. In the study of GADD34-related mitochondrial unfolding protein response (mtUPR), we found that canonical mtUPR, launched by the phosphate eIF2a, is involved in the resistant characteristic of specific mtDNA to MPP+ treatment. Our study suggests that a lower expression of GADD34 in the late phase of mtUPR may prolong the mtUPR process, thereby benefitting protein homeostasis and facilitating cellular resistance to PD development. We herein demonstrate that GADD34 plays an important role in PD development and should be further investigated as a target for the development of therapies for PD.

Published

2024

3. Impact of the m.13513G>A Variant on the Functions of the OXPHOS System and Cell Retrograde Signaling

Author

Dita Kidere, Pawel Zayakin, Diana Livcane, Marina Makrecka-Kuka, Janis Stavusis, Baiba Lace, Tsu-Kung Lin, Chia-Wei Liou, and Inna Inashkina

Subjects

OXPHOS system, retrograde signaling, RNA sequencing, mitochondrial diseases, Leigh syndrome, Biology (General), QH301-705.5

Abstract

Mitochondria are involved in many vital functions in living cells, including the synthesis of ATP by oxidative phosphorylation (OXPHOS) and regulation of nuclear gene expression through retrograde signaling. Leigh syndrome is a heterogeneous neurological disorder resulting from an isolated complex I deficiency that causes damage to mitochondrial energy production. The pathogenic mitochondrial DNA (mtDNA) variant m.13513G>A has been associated with Leigh syndrome. The present study investigated the effects of this mtDNA variant on the OXPHOS system and cell retrograde signaling. Transmitochondrial cytoplasmic hybrid (cybrid) cell lines harboring 50% and 70% of the m.13513G>A variant were generated and tested along with wild-type (WT) cells. The functionality of the OXPHOS system was evaluated by spectrophotometric assessment of enzyme activity and high-resolution respirometry. Nuclear gene expression was investigated by RNA sequencing and droplet digital PCR. Increasing levels of heteroplasmy were associated with reduced OXPHOS system complex I, IV, and I + III activities, and high-resolution respirometry also showed a complex I defect. Profound changes in transcription levels of nuclear genes were observed in the cell lines harboring the pathogenic mtDNA variant, indicating the physiological processes associated with defective mitochondria.

Published

2023

4. Altered Splicing of LAMP2 in a Multigenerational Family from Latvia Affected by Danon Disease

Author

Janis Stavusis, Ieva Micule, Ieva Grinfelde, Anna Zdanovica, Janis Pudulis, Sandra Valeina, Svetlana Sepetiene, Baiba Lace, and Inna Inashkina

Subjects

LAMP2, Danon disease, altered splicing, Medicine (General), R5-920

Abstract

Background and Objectives: Danon disease is a multisystemic disorder associated with variants in the LAMP2 gene, mainly affecting the cardiac muscle. Here, we report a multigenerational family from Latvia with two male patients, hemizygous for a novel splice-affecting variant c.928+3A>G. Affected patients exhibit a cardiac phenotype, moderate mental disability, and mild retinal changes. Materials and Methods: Both patients underwent either exome or hypertrophic cardiomyopathy gene panel next-generation sequencing. The pathogenic variant effect was determined using reverse transcription, Sanger sequencing, and high-resolution electrophoresis. Results: Evaluation of the splicing process revealed that approximately 80% of the transcripts exhibited a lack of the entire exon 7. This alteration was predicted to cause a shift of the reading frame, consequently introducing a premature stop codon downstream in the sequence. Conclusions: Based on our data, we propose that c.928+3A>G is a pathogenic variant associated with Danon disease.

Published

2024

5. The most common European HINT1 neuropathy variant phenotype and its case studies

Author

Marija Rozevska, Dmitrijs Rots, Linda Gailite, Ronalds Linde, Stanislavs Mironovs, Maksims Timcenko, Viktors Linovs, Dzintra Locmele, Ieva Micule, Baiba Lace, and Viktorija Kenina

Subjects

HINT1, nerve USG, axonal polyneuropathy, population frequency, impaired mental performance, Neurology. Diseases of the nervous system, RC346-429

Abstract

HINT1 is an ubiquitous homodimeric purine phosphoramidase belonging to the histidine-triad superfamily. In neurons, HINT1 stabilizes the interaction of different receptors and regulates the effects of their signaling disturbances. Changes in HINT1 gene are associated with autosomal recessive axonal neuropathy with neuromyotonia. Aim of the study was detailed description of patients' phenotype with HINT1 homozygous NM_005340.7: c.110G>C (p.Arg37Pro) variant. Seven homozygous and three compound heterozygous patients were recruited and evaluated using standardized tests for CMT patients, in four patients' nerve ultrasonography was performed. The median age of symptom onset was 10 years (range 1–20), with initial complaints being distal lower limb weakness with gait impairment, combined with muscle stiffness, more pronounced in the hands than in the legs and worsened by cold. Arm muscles became involved later, presenting with distal weakness and hypotrophy. Neuromyotonia was present in all reported patients and is thus a diagnostic hallmark. Electrophysiological studies demonstrated axonal polyneuropathy. Impaired mental performance was observed in six out of ten cases. In all patients with HINT1 neuropathy, ultrasound examination showed significantly reduced muscle volume as well as spontaneous fasciculations and fibrillations. The nerve cross-sectional areas of the median and ulnar nerves were closer to the lower limits of the normal values. None of the investigated nerves had structural changes. Our findings broaden the phenotype of HINT1-neuropathy and have implications for diagnostics and ultrasonographic evaluation of HINT1-neuropathy patients.

Published

2023

6. A founder mutation in the PLPBP gene in families from Saguenay‐Lac‐St‐Jean region affected by a pyridoxine‐dependent epilepsy

Author

Maitou Pal, Baiba Lace, Yvan Labrie, Nathalie Laflamme, Nadie Rioux, Samarth Thonta Setty, Marc‐Andre Dugas, Louise Gosselin, Arnaud Droit, Nicolas Chrestian, and Serge Rivest

Subjects

PLPBP, PROSC, vitamin B6‐dependent early‐onset epilepsy, Diseases of the endocrine glands. Clinical endocrinology, RC648-665, Genetics, QH426-470

Abstract

Abstract Pyridoxine‐dependent epilepsy (PDE) is a relatively rare subgroup of epileptic disorders. They generally present in infancy as an early onset epileptic encephalopathy or seizures, refractory to standard treatments, with rapid and variable responses to vitamin B6 treatment. Whole exome sequencing of three unrelated families identified homozygous pathogenic mutation c.370_373del, p.Asp124fs in PLPBP gene in five persons. Haplotype analysis showed a single shared profile for the affected persons and their parents, leading to a hypothesis about founder effect of the mutation in Saguenay‐Lac‐St‐Jean region of French Canadians. All affected probands also shared one single mitochondrial haplotype T2b3 and two rare variations in the mitochondrial genome m.801A>G and m.5166A>G suggesting that a single individual female introduced PLPBP mutation c.370_373del, p.Asp124fs in Quebec. The mutation p.Asp124fs causes a severe disease phenotype with delayed myelination and cortical/subcortical brain atrophy. The most noteworthy radiological finding in this Quebec founder mutation is the presence of the temporal cysts that can be used as a marker of the disease. Also, both patients, who are alive, had a history of prenatal supplements taken by their mothers as antiemetic medication with high doses of pyridoxine. In the context of suspected PDE in patients with neonatal refractory seizures, treatment with pyridoxine and/or Pyridoxal‐5‐phophate has to be started immediately and continued until the results of genetic analysis received. Even with early appropriate treatment, neurological outcome of our patient is still poor.

Published

2021

7. Whole-exome sequencing identifies homozygous mutation in TTI2 in a child with primary microcephaly: a case report

Author

Vincent Picher-Martel, Yvan Labrie, Serge Rivest, Baiba Lace, and Nicolas Chrestian

Subjects

TTI2, Microcephaly, Whole-exome sequencing, Case report, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Background Primary microcephaly is defined as reduced occipital-frontal circumference noticeable before 36 weeks of gestation. Large amount of insults might lead to microcephaly including infections, hypoxia and genetic mutations. More than 16 genes are described in autosomal recessive primary microcephaly. However, the cause of microcephaly remains unclear in many cases after extensive investigations and genetic screening. Case presentation Here, we described the case of a boy with primary microcephaly who presented to a neurology clinic with short stature, global development delay, dyskinetic movement, strabismus and dysmorphic features. We performed microcephaly investigations and genetic panels. Then, we performed whole-exome sequencing to identify any genetic cause. Microcephaly investigations and genetic panels were negative, but we found a new D317V homozygous mutation in TELOE-2 interacting protein 2 (TTI2) gene by whole-exome sequencing. TTI2 is implicated in DNA damage response and mutation in that gene was previously described in mental retardation, autosomal recessive 39. Conclusions We described the first French Canadian case with primary microcephaly and global developmental delay secondary to a new D317V homozygous mutation in TTI2 gene. Our report also highlights the importance of TTI2 protein in brain development.

Published

2020

8. Case Report: Two Families With HPDL Related Neurodegeneration

Author

Ieva Micule, Baiba Lace, Nathan T. Wright, Nicolas Chrestian, Jurgis Strautmanis, Mikus Diriks, Janis Stavusis, Dita Kidere, Elfa Kleina, Anna Zdanovica, Nataly Laflamme, Nadie Rioux, Samarth Thonta Setty, Sander Pajusalu, Arnaud Droit, Monkol Lek, Serge Rivest, and Inna Inashkina

Subjects

spastic paraplegia, ataxia, citrate-synthase, mitochondrial diseases, brain diseases, Genetics, QH426-470

Abstract

There are recent reports of associations of variants in the HPDL gene with a hereditary neurological disease that presents with a wide spectrum of clinical severity, ranging from severe neonatal encephalopathy with no psychomotor development to adolescent-onset uncomplicated spastic paraplegia. Here, we report two probands from unrelated families presenting with severe and intermediate variations of the clinical course. A homozygous variant in the HPDL gene was detected in each proband; however, there was no known parental consanguinity. We also highlight reductions in citrate synthase and mitochondrial complex I activity detected in both probands in different tissues, reflecting the previously proposed mitochondrial nature of disease pathogenesis associated with HPDL mutations. Further, we speculate on the functional consequences of the detected variants, although the function and substrate of the HPDL enzyme are currently unknown.

Published

2022

9. Monogenic Versus Multifactorial Inheritance in the Development of Isolated Cleft Palate: A Whole Genome Sequencing Study

Author

Baiba Lace, Sander Pajusalu, Diana Livcane, Ieva Grinfelde, Ilze Akota, Ieva Mauliņa, Biruta Barkāne, Janis Stavusis, and Inna Inashkina

Subjects

isolated cleft palate, whole genome sequencing, rare monogenic diseases, recurrence risk, PCGF2, Genetics, QH426-470

Abstract

Craniofacial morphogenesis is highly complex, as is the anatomical region involved. Errors during this process, resulting in orofacial clefts, occur in more than 400 genetic syndromes. Some cases of cleft lip and/or palate (CLP) are caused by mutations in single genes; however, complex interactions between genetic and environmental factors are considered to be responsible for the majority of non-syndromic CLP development. The aim of the current study was to identify genetic risk factors in patients with isolated cleft palate (CP) by whole genome sequencing. Patients with isolated CP (n = 30) recruited from the Riga Cleft Lip and Palate Centre, Institute of Stomatology, Riga, were analyzed by whole genome sequencing. Pathogenic or likely pathogenic variants were discovered in genes associated with CP (TBX22, COL2A1, FBN1, PCGF2, and KMT2D) in five patients; hence, rare disease variants were identified in 17% of patients with non-syndromic isolated CP. Our results were relevant to routine genetic counselling practice and genetic testing recommendations. Based on our data, we propose that all newborns with orofacial clefts should be offered genetic testing, at least for a panel of known CLP genes. Only if the results are negative and there is no suggestive family history or additional clinical symptoms (which would support additional exome or genome-wide investigation), should multifactorial empiric recurrence risk prediction tools be applied for families.

Published

2022

10. A Homozygous Deep Intronic Mutation Alters the Splicing of Nebulin Gene in a Patient With Nemaline Myopathy

Author

Nathalie Laflamme, Baiba Lace, Samarth Thonta Setty, Nadie Rioux, Yvan Labrie, Arnaud Droit, Nicolas Chrestian, and Serge Rivest

Subjects

nemalin myopathy, neuromuscular disorder, alternative splicing, nebulin isoforms, nebulin, NEB, Neurology. Diseases of the nervous system, RC346-429

Abstract

Nemaline myopathy is a rare disorder affecting the muscle sarcomere. Mutations in nebulin gene (NEB) are known to be responsible for about 50% of nemaline myopathy cases. Nebulin is a giant protein which is formed integrally with the sarcomeric thin filament. This complex gene is under extensive alternative splicing giving rise to multiple isoforms. In this study, we report a 6-year-old boy presenting with general muscular weaknesses. Identification of rod-shaped structures in the patient' biopsy raised doubt about the presence of a nemaline myopathy. Next-generation sequencing was used to identify a causative mutation for the patient syndrome. A homozygous deep intronic substitution was found in the intron 144 of the NEB. The variant was predicted by in silico tools to create a new donor splice site. Molecular analysis has shown that the mutation could alter splicing events of the nebulin gene leading to a significant decrease of isoforms level. This change in the expression level of nebulin could give rise to functional consequences in the sarcomere. These results are consistent with the phenotypes observed in the patient. Such a discovery of variants in this gene will allow a better understanding of the involvement of nebulin in neuromuscular diseases and help find new treatments for the nemaline myopathy.

Published

2021

11. HSD10 mitochondrial disease: p.Leu122Val variant, mild clinical phenotype, and founder effect in French‐Canadian patients from Quebec

Author

Paula J. Waters, Baiba Lace, Daniela Buhas, Serge Gravel, Denis Cyr, Renée‐Myriam Boucher, Geneviève Bernard, Sébastien Lévesque, and Bruno Maranda

Subjects

2‐methyl‐3‐hydroxybutyryl‐CoA dehydrogenase, 17‐beta‐hydroxysteroid dehydrogenase X, HADH2, HSD10, HSD17B10, MHBD deficiency, Genetics, QH426-470

Abstract

Abstract Background HSD10 mitochondrial disease (HSD10MD), originally described as a deficiency of 2‐methyl‐3‐hydroxybutyryl‐CoA dehydrogenase (MHBD), is a rare X‐linked disorder of a moonlighting protein encoded by the HSD17B10. The diagnosis is usually first suspected on finding elevated isoleucine degradation metabolites in urine, reflecting decreased MHBD activity. However, it is now known that clinical disease pathogenesis reflects other independent functions of the HSD10 protein; particularly its essential role in mitochondrial transcript processing and tRNA maturation. The classical phenotype of HSD10MD in affected males is an infantile‐onset progressive neurodegenerative disorder associated with severe mitochondrial dysfunction. Patients, Methods, and Results In four unrelated families, we identified index patients with MHBD deficiency, which implied a diagnosis of HSD10MD. Each index patient was independently investigated because of neurological or developmental concerns. All had persistent elevations of urinary 2‐methyl‐3‐hydroxybutyric acid and tiglylglycine. Analysis of HSD17B10 identified a single missense variant, c.364C>G, p.Leu122Val, in each case. This rare variant (1/183336 alleles in gnomAD) was previously reported in one Dutch patient and was described as pathogenic. The geographic origins of our families and results of haplotype analysis together provide evidence of a founder effect for this variant in Quebec. Notably, we identified an asymptomatic hemizygous adult male in one family, while a second independent genetic disorder contributed substantially to the clinical phenotypes observed in probands from two other families. Conclusion The phenotype associated with p.Leu122Val in HSD17B10 currently appears to be attenuated and nonprogressive. This report widens the spectrum of phenotypic severity of HSD10MD and contributes to genotype–phenotype correlation. At present, we consider p.Leu122Val a “variant of uncertain significance.” Nonetheless, careful follow‐up of our patients remains advisable, to assess long‐term clinical course and ensure appropriate management. It will also be important to identify other potential patients in our population and to characterize their phenotype.

Published

2019

12. Duplication events downstream of IRX1 cause North Carolina macular dystrophy at the MCDR3 locus

Author

Valentina Cipriani, Raquel S. Silva, Gavin Arno, Nikolas Pontikos, Ambreen Kalhoro, Sandra Valeina, Inna Inashkina, Mareta Audere, Katrina Rutka, Bernard Puech, Michel Michaelides, Veronica van Heyningen, Baiba Lace, Andrew R. Webster, and Anthony T. Moore

Subjects

Medicine, Science

Abstract

Abstract Autosomal dominant North Carolina macular dystrophy (NCMD) is believed to represent a failure of macular development. The disorder has been linked to two loci, MCDR1 (chromosome 6q16) and MCDR3 (chromosome 5p15-p13). Recently, non-coding variants upstream of PRDM13 (MCDR1) and a duplication including IRX1 (MCDR3) have been identified. However, the underlying disease-causing mechanism remains uncertain. Through a combination of sequencing studies on eighteen NCMD families, we report two novel overlapping duplications at the MCDR3 locus, in a gene desert downstream of IRX1 and upstream of ADAMTS16. One duplication of 43 kb was identified in nine families (with evidence for a shared ancestral haplotype), and another one of 45 kb was found in a single family. Three families carry the previously reported V2 variant (MCDR1), while five remain unsolved. The MCDR3 locus is thus refined to a shared region of 39 kb that contains DNAse hypersensitive sites active at a restricted time window during retinal development. Publicly available data confirmed expression of IRX1 and ADAMTS16 in human fetal retina, with IRX1 preferentially expressed in fetal macula. These findings represent a major advance in our understanding of the molecular genetics of NCMD and provide insights into the genetic pathways involved in human macular development.

Published

2017

13. Human Mitochondrial HMG-CoA Synthase Deficiency: Role of Enzyme Dimerization Surface and Characterization of Three New Patients

Author

Beatriz Puisac, Iñigo Marcos-Alcalde, María Hernández-Marcos, Pilar Tobajas Morlana, Alina Levtova, Bernd C. Schwahn, Corinne DeLaet, Baiba Lace, Paulino Gómez-Puertas, and Juan Pié

Subjects

mitochondrial HMG-CoA synthase, deficiency, mutations, enzyme dimerization, ketone bodies, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Mitochondrial 3-hydroxy-3-methylglutaryl-CoA synthase deficiency (mitochondrial HMG-CoA synthase deficiency or mHS deficiency, OMIM #605911) is an inborn error of metabolism that affects ketone body synthesis. Acute episodes include vomiting, lethargy, hepatomegaly, hypoglycemia and dicarboxylic aciduria. The diagnosis is difficult due to the relatively unspecific clinical and biochemical presentation, and fewer than 30 patients have been described. This work describes three new patients with mHS deficiency and two missense mutations c.334C>T (p.R112W) and c.430G>T (p.V144L) previously not reported. We developed a new method to express and measure the activity of the enzyme and in this work the study is extended to ten new missense variants including those of our patients. Enzymatic assays showed that three of the mutant proteins retained some but seven completely lacked activity. The identification of a patient homozygous for a mutation that retains 70% of enzyme activity opens the door to a new interpretation of the disease by demonstrating that a modest impairment of enzyme function can actually produce symptoms. This is also the first study employing molecular dynamics modelling of the enzyme mutations. We show that the correct maintenance of the dimerization surface is crucial for retaining the structure of the active center and therefore the activity of the enzyme.

Published

2018

14. Dupuytren's Contracture Cosegregation with Limb-Girdle Muscle Dystrophy

Author

Baiba Lace, Inna Inashkina, Ieva Micule, Inta Vasiljeva, Maruta Solvita Naudina, Jurgis Strautmanis, Janis Stavusis, and Eriks Jankevics

Subjects

Neurology. Diseases of the nervous system, RC346-429

Abstract

Limb-girdle muscular dystrophies (LGMDs) is a heterogeneous group of muscular dystrophies that mostly affect the pelvic and shoulder girdle muscle groups. We report here a case of neuromuscular disease associated with Dupuytren's contracture, which has never been described before as cosegregating with an autosomal dominant type of inheritance. Dupuytren's contracture is a common disease, especially in Northern Europe. Comorbid conditions associated with Dupuytren's contracture are repetitive trauma to the hands, diabetes, and seizures, but it has never before been associated with neuromuscular disease. We hypothesize that patients may harbor mutations in genes with functions related to neuromuscular disease and Dupuytren's contracture development.

Published

2013

15. Interaction between IRF6 and TGFA genes contribute to the risk of nonsyndromic cleft lip/palate.

Author

Ariadne Letra, Walid Fakhouri, Renata F Fonseca, Renato Menezes, Inga Kempa, Joanne L Prasad, Toby G McHenry, Andrew C Lidral, Lina Moreno, Jeffrey C Murray, Sandra Daack-Hirsch, Mary L Marazita, Eduardo E Castilla, Baiba Lace, Ieda M Orioli, Jose M Granjeiro, Brian C Schutte, and Alexandre R Vieira

Subjects

Medicine, Science

Abstract

Previous evidence from tooth agenesis studies suggested IRF6 and TGFA interact. Since tooth agenesis is commonly found in individuals with cleft lip/palate (CL/P), we used four large cohorts to evaluate if IRF6 and TGFA interaction contributes to CL/P. Markers within and flanking IRF6 and TGFA genes were tested using Taqman or SYBR green chemistries for case-control analyses in 1,000 Brazilian individuals. We looked for evidence of gene-gene interaction between IRF6 and TGFA by testing if markers associated with CL/P were overtransmitted together in the case-control Brazilian dataset and in the additional family datasets. Genotypes for an additional 142 case-parent trios from South America drawn from the Latin American Collaborative Study of Congenital Malformations (ECLAMC), 154 cases from Latvia, and 8,717 individuals from several cohorts were available for replication of tests for interaction. Tgfa and Irf6 expression at critical stages during palatogenesis was analyzed in wild type and Irf6 knockout mice. Markers in and near IRF6 and TGFA were associated with CL/P in the Brazilian cohort (p

Published

2012

16. CAPN3 c.1746-20C>G variant is hypomorphic for LGMD R1 calpain 3-related

Author

Magdalena Mroczek, Inna Inashkina, Janis Stavusis, Pawel Zayakin, Andrey Khrunin, Ieva Micule, Victorija Kenina, Anna Zdanovica, Jana Zídková, Lenka Fajkusová, Svetlana Limborska, Anneke J. van der Kooi, Esther Brusse, Lea Leonardis, Ales Maver, Sander Pajusalu, Katrin Õunap, Sanna Puusepp, Paula Dobosz, Mateusz Sypniewski, Birute Burnyte, Baiba Lace, Neurology, ANS - Neuroinfection & -inflammation, and EURO-NMD

Subjects

Muscular Dystrophies, Limb-Girdle, CAPN3, Calpain, RNA Splicing, Mutation, Genetics, Humans, Muscle Proteins, LGMD R1 calpain 3-related, hypomorphic variant, Genetics (clinical), LGMD, calpainopathy

Abstract

The investigated intronic CAPN3 variant NM_000070.3:c.1746-20C>G occurs in the Central and Eastern Europe with a frequency of >1% and there are conflicting interpretations on its pathogenicity. We collected data on 14 patients carrying the CAPN3 c.1746-20C>G variant in trans position with another CAPN3 pathogenic/likely pathogenic variant. The patients compound heterozygous for the CAPN3 c.1746-20C>G variant presented a phenotype consistent with calpainopathy of mild/medium severity. This variant is most frequent in the North/West regions of Russia and may originate from that area. Molecular studies revealed that different splicing isoforms are produced in the muscle. We hypothesize that c.1746-20C>G is a hypomorphic variant with a reduction of RNA and protein expression and only individuals having a higher ratio of abnormal isoforms are affected. Reclassification of the CAPN3 variant c.1746-20C>G from variant with a conflicting interpretation of pathogenicity to hypomorphic variant explains many unidentified cases of limb girdle muscular dystrophy R1 calpain 3-related in Eastern and Central Europe.

Published

2022

17. EIF2AK2 Missense Variants Associated with Early Onset Generalized Dystonia

Author

Lena Sagi-Dain, Martje G. Pauly, Chiung C. Chen, Niccolo E. Mencacci, Shey Lin Wu, Inge A. Meijer, Aida M. Bertoli-Avella, Krishna Kumar Kandaswamy, Steven J. Lubbe, Celeste Panteghini, Wim Mandemakers, Christine Klein, Nicolas Marotta, Katja Lohmann, Peter Bauer, Andrea A. Kühn, Baiba Lace, Vincenzo Bonifati, Tu Hsueh Yeh, Chin Song Lu, Miryam Carecchio, Antonio E. Elia, Christina Fevga, Yah Huei Wu-Chou, Yi Hsin Weng, Vera Tadic, Bradley Osterman, Marialuisa Quadri, Barbara Garavaglia, Simone Olgiati, Guido J. Breedveld, Jens Volkmann, Hsiu Chen Chang, Demy J.S. Kuipers, and Clinical Genetics

Subjects

0301 basic medicine, Adult, Male, Adolescent, Mutation, Missense, Biology, White People, 03 medical and health sciences, symbols.namesake, Young Adult, eIF-2 Kinase, 0302 clinical medicine, Asian People, Genetic linkage, Exome Sequencing, medicine, Missense mutation, Humans, Age of Onset, Protein kinase A, Child, Exome, Research Articles, Dystonia, Sanger sequencing, Genetics, Kinase, Brain, Infant, Fibroblasts, Middle Aged, medicine.disease, Protein kinase R, Magnetic Resonance Imaging, Pedigree, 030104 developmental biology, Neurology, Dystonic Disorders, Child, Preschool, symbols, Female, Neurology (clinical), 030217 neurology & neurosurgery, Genome-Wide Association Study, Research Article

Abstract

Objective: The study was undertaken to identify a monogenic cause of early onset, generalized dystonia. Methods: Methods consisted of genome-wide linkage analysis, exome and Sanger sequencing, clinical neurological examination, brain magnetic resonance imaging, and protein expression studies in skin fibroblasts from patients. Results: We identified a heterozygous variant, c.388G>A, p.Gly130Arg, in the eukaryotic translation initiation factor 2 alpha kinase 2 (EIF2AK2) gene, segregating with early onset isolated generalized dystonia in 5 patients of a Taiwanese family. EIF2AK2 sequencing in 191 unrelated patients with unexplained dystonia yielded 2 unrelated Caucasian patients with an identical heterozygous c.388G>A, p.Gly130Arg variant, occurring de novo in one case, another patient carrying a different heterozygous variant, c.413G>C, p.Gly138Ala, and one last patient, born from consanguineous parents, carrying a third, homozygous variant c.95A>C, p.Asn32Thr. These 3 missense variants are absent from gnomAD, and are located in functional domains of the encoded protein. In 3 patients, additional neurological manifestations were present, including intellectual disability and spasticity. EIF2AK2 encodes a kinase (protein kinase R [PKR]) that phosphorylates eukaryotic translation initiation factor 2 alpha (eIF2α), which orchestrates the cellular stress response. Our expression studies showed abnormally enhanced activation of the cellular stress response, monitored by PKR-mediated phosphorylation of eIF2α, in fibroblasts from patients with EIF2AK2 variants. Intriguingly, PKR can also be regulated by PRKRA (protein interferon-inducible double-stranded RNA-dependent protein kinase activator A), the product of another gene causing monogenic dystonia. Interpretation: We identified EIF2AK2 variants implicated in early onset generalized dystonia, which can be dominantly or recessively inherited, or occur de novo. Our findings provide direct evidence for a key role of a dysfunctional eIF2α pathway in the pathogenesis of dystonia. ANN NEUROL 2021;89:485–497.

Published

2021

18. A founder mutation in the PLPBP gene in families from Saguenay‐Lac‐St‐Jean region affected by a pyridoxine‐dependent epilepsy

Author

Marc Andre Dugas, Arnaud Droit, Yvan Labrie, Maitou Pal, Nicolas Chrestian, Nadie Rioux, Nathalie Laflamme, Samarth Thonta Setty, Serge Rivest, Louise Gosselin, and Baiba Lace

Subjects

Proband, Research Report, PLPBP, Pediatrics, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, Context (language use), QH426-470, Biochemistry, Genetics and Molecular Biology (miscellaneous), Diseases of the endocrine glands. Clinical endocrinology, PROSC, Epilepsy, vitamin B6‐dependent early‐onset epilepsy, Genetics, Internal Medicine, Medicine, Pyridoxine-dependent epilepsy, Exome sequencing, business.industry, Haplotype, Research Reports, RC648-665, medicine.disease, Mutation (genetic algorithm), business, Founder effect

Abstract

Pyridoxine‐dependent epilepsy (PDE) is a relatively rare subgroup of epileptic disorders. They generally present in infancy as an early onset epileptic encephalopathy or seizures, refractory to standard treatments, with rapid and variable responses to vitamin B6 treatment. Whole exome sequencing of three unrelated families identified homozygous pathogenic mutation c.370_373del, p.Asp124fs in PLPBP gene in five persons. Haplotype analysis showed a single shared profile for the affected persons and their parents, leading to a hypothesis about founder effect of the mutation in Saguenay‐Lac‐St‐Jean region of French Canadians. All affected probands also shared one single mitochondrial haplotype T2b3 and two rare variations in the mitochondrial genome m.801A>G and m.5166A>G suggesting that a single individual female introduced PLPBP mutation c.370_373del, p.Asp124fs in Quebec. The mutation p.Asp124fs causes a severe disease phenotype with delayed myelination and cortical/subcortical brain atrophy. The most noteworthy radiological finding in this Quebec founder mutation is the presence of the temporal cysts that can be used as a marker of the disease. Also, both patients, who are alive, had a history of prenatal supplements taken by their mothers as antiemetic medication with high doses of pyridoxine. In the context of suspected PDE in patients with neonatal refractory seizures, treatment with pyridoxine and/or Pyridoxal‐5‐phophate has to be started immediately and continued until the results of genetic analysis received. Even with early appropriate treatment, neurological outcome of our patient is still poor.

Published

2021

19. A second cohort of CHD3 patients expands the molecular mechanisms known to cause Snijders Blok-Campeau syndrome

Author

Ann Seman, Rixa Woitschach, Duygu Selcen, Divya Nair, Lauren Gunderson, Mahim Jain, Sha Tang, Giuseppe Zampino, Julien L. Marcadier, Marielle Alders, Jason Pinner, Melanie Napier, Linda Hasadsri, Marina Macchiaiolo, Alyssa Blesson, Pavel N. Pichurin, Joseph T. Alaimo, Arjan Bouman, Philippe M. Campeau, Catherine Karimov, Chitra Prasad, Anne Dieux-Coeslier, Nicole L. Bertsch, Bernd Wollnik, Janine Altmüller, Zöe Powis, Holly Dubbs, Tahsin Stefan Barakat, Gregory M. Cooper, Kristen J. Rasmussen, Perrine Brunelle, Patrick R. Blackburn, Erica D. Smith, Jeff M. Milunsky, Katja Kloth, E. Martina Bebin, Lot Snijders Blok, Knut Brockmann, Karin Weiss, Xilma R. Ortiz-Gonzalez, Danna Gal, Dong Li, Francesca Clementina Radio, Joan M. Stoler, Elaine H. Zackai, Jiddeke M. van de Kamp, Deepali N. Shinde, Huifang Yan, Thomas Smol, Alejandro Ferrer, Dagmar Weise, Baiba Lace, Deborah L. Renaud, Lauren E. Bartik, Beth Keena, Michelle L. Thompson, Carol J Saunders, Theodore G. Drivas, Elizabeth J. Bhoj, Eric T. Rush, Marco Tartaglia, Eric W. Klee, Margit Burmeister, Jingmin Wang, Jonas Denecke, Clinical genetics, Amsterdam Neuroscience - Complex Trait Genetics, Amsterdam Gastroenterology Endocrinology Metabolism, Human Genetics, ACS - Pulmonary hypertension & thrombosis, ARD - Amsterdam Reproduction and Development, and Clinical Genetics

Subjects

Adult, Male, CHD3 variants, Genetic testing, Adolescent, Snijders Blok-Campeau syndrome, Developmental Disabilities, medicine.disease_cause, Pediatrics, Article, Chromodomain, Craniofacial Abnormalities, Catalytic Domain, Intellectual Disability, Genetics, medicine, Missense mutation, Humans, Child, Genetics (clinical), Mutation, medicine.diagnostic_test, biology, Significant difference, DNA Helicases, Helicase, Infant, Syndrome, Autism spectrum disorders, Phenotype, Settore MED/38 - PEDIATRIA GENERALE E SPECIALISTICA, Child, Preschool, Cohort, biology.protein, Female, Mi-2 Nucleosome Remodeling and Deacetylase Complex

Abstract

There has been one previous report of a cohort of patients with variants in Chromodomain Helicase DNA-binding 3 (CHD3), now recognized as Snijders Blok-Campeau syndrome. However, with only three previously-reported patients with variants outside the ATPase/helicase domain, it was unclear if variants outside of this domain caused a clinically similar phenotype. We have analyzed 24 new patients with CHD3 variants, including nine outside the ATPase/helicase domain. All patients were detected with unbiased molecular genetic methods. There is not a significant difference in the clinical or facial features of patients with variants in or outside this domain. These additional patients further expand the clinical and molecular data associated with CHD3 variants. Importantly we conclude that there is not a significant difference in the phenotypic features of patients with various molecular disruptions, including whole gene deletions and duplications, and missense variants outside the ATPase/helicase domain. This data will aid both clinical geneticists and molecular geneticists in the diagnosis of this emerging syndrome.

Published

2020

20. Whole-exome sequencing identifies homozygous mutation in TTI2 in a child with primary microcephaly: a case report

Author

Serge Rivest, Yvan Labrie, Nicolas Chrestian, Vincent Picher-Martel, and Baiba Lace

Subjects

Male, Microcephaly, Canada, Brain development, Primary microcephaly, Nervous System Malformations, Short stature, lcsh:RC346-429, 03 medical and health sciences, 0302 clinical medicine, Exome Sequencing, Case report, Medicine, Humans, Global developmental delay, Genetic Testing, Gene, Exome sequencing, lcsh:Neurology. Diseases of the nervous system, 030304 developmental biology, Genetics, 0303 health sciences, business.industry, Homozygote, Infant, General Medicine, TTI2, medicine.disease, 3. Good health, Child, Preschool, Whole-exome sequencing, Mutation, French canadian, Neurology (clinical), medicine.symptom, business, 030217 neurology & neurosurgery

Abstract

Background Primary microcephaly is defined as reduced occipital-frontal circumference noticeable before 36 weeks of gestation. Large amount of insults might lead to microcephaly including infections, hypoxia and genetic mutations. More than 16 genes are described in autosomal recessive primary microcephaly. However, the cause of microcephaly remains unclear in many cases after extensive investigations and genetic screening. Case presentation Here, we described the case of a boy with primary microcephaly who presented to a neurology clinic with short stature, global development delay, dyskinetic movement, strabismus and dysmorphic features. We performed microcephaly investigations and genetic panels. Then, we performed whole-exome sequencing to identify any genetic cause. Microcephaly investigations and genetic panels were negative, but we found a new D317V homozygous mutation in TELOE-2 interacting protein 2 (TTI2) gene by whole-exome sequencing. TTI2 is implicated in DNA damage response and mutation in that gene was previously described in mental retardation, autosomal recessive 39. Conclusions We described the first French Canadian case with primary microcephaly and global developmental delay secondary to a new D317V homozygous mutation in TTI2 gene. Our report also highlights the importance of TTI2 protein in brain development.

Published

2020

21. Overview of Neuromuscular Disorder Molecular Diagnostic Experience for the Population of Latvia

Author

Baiba Lace, Ieva Micule, Viktorija Kenina, Signe Setlere, Jurgis Strautmanis, Inese Kazaine, Gita Taurina, Daiga Murmane, Ieva Grinfelde, Liene Kornejeva, Zita Krumina, Olga Sterna, Ilze Radovica-Spalvina, Inta Vasiljeva, Linda Gailite, Janis Stavusis, Diana Livcane, Dita Kidere, Ieva Malniece, and Inna Inashkina

Subjects

Neurology (clinical), Genetics (clinical)

Abstract

Background and ObjectivesGenetic testing has become an integral part of health care, allowing the confirmation of thousands of hereditary diseases, including neuromuscular disorders (NMDs). The reported average prevalence of individual inherited NMDs is 3.7–4.99 per 10,000. This number varies greatly in the selected populations after applying population-wide studies. The aim of this study was to evaluate the effect of genetic analysis as the first-tier test in patients with NMD and to calculate the disease prevalence and allelic frequencies for reoccurring genetic variants.MethodsPatients with NMD from Latvia with molecular tests confirming their diagnosis in 2008–2020 were included in this retrospective study.ResultsDiagnosis was confirmed in 153 unique cases of all persons tested. Next-generation sequencing resulted in a detection rate of 37%. Two of the most common childhood-onset NMDs in our population were spinal muscular atrophy and dystrophinopathies, with a birth prevalence of 1.01 per 10,000 newborns and 2.08 per 10,000 (male newborn population), respectively. The calculated point prevalence was 0.079 per 10,000 for facioscapulohumeral muscular dystrophy type 1, 0.078 per 10,000 for limb-girdle muscular dystrophy, 0.073 per 10,000 for nondystrophic congenital myotonia, 0.052 per 10,000 for spinobulbar muscular atrophy, and 0.047 per 10,000 for type 1 myotonic dystrophy.DiscussionDNA diagnostics is a successful approach. The carrier frequencies of the common CAPN3, FKRP, SPG11, and HINT1 gene variants as well as that of the SMN1 gene exon 7 deletion in the population of Latvia are comparable with data from Europe. The carrier frequency of the CLCN1 gene variant c.2680C>T p.(Arg894Ter) is 2.11%, and consequently, congenital myotonia is the most frequent NMD in our population.

Published

2021

22. Monogenic Versus Multifactorial Inheritance in the Development of Isolated Cleft Palate: A Whole Genome Sequencing Study

Author

Baiba Lace, Sander Pajusalu, Diana Livcane, Ieva Grinfelde, Ilze Akota, Ieva Mauliņa, Biruta Barkāne, Janis Stavusis, and Inna Inashkina

Subjects

Genetics, Molecular Medicine, Genetics (clinical)

Abstract

Craniofacial morphogenesis is highly complex, as is the anatomical region involved. Errors during this process, resulting in orofacial clefts, occur in more than 400 genetic syndromes. Some cases of cleft lip and/or palate (CLP) are caused by mutations in single genes; however, complex interactions between genetic and environmental factors are considered to be responsible for the majority of non-syndromic CLP development. The aim of the current study was to identify genetic risk factors in patients with isolated cleft palate (CP) by whole genome sequencing. Patients with isolated CP (n = 30) recruited from the Riga Cleft Lip and Palate Centre, Institute of Stomatology, Riga, were analyzed by whole genome sequencing. Pathogenic or likely pathogenic variants were discovered in genes associated with CP (TBX22, COL2A1, FBN1, PCGF2, and KMT2D) in five patients; hence, rare disease variants were identified in 17% of patients with non-syndromic isolated CP. Our results were relevant to routine genetic counselling practice and genetic testing recommendations. Based on our data, we propose that all newborns with orofacial clefts should be offered genetic testing, at least for a panel of known CLP genes. Only if the results are negative and there is no suggestive family history or additional clinical symptoms (which would support additional exome or genome-wide investigation), should multifactorial empiric recurrence risk prediction tools be applied for families.

Published

2021

23. Complete mtDNA sequencing reveals mutations m.9185T>C and m.13513G>A in three patients with Leigh syndrome

Author

Inna Inashkina, Eriks Jankevics, Irina Adomaitiene, Zita Krumina, Baiba Lace, Evelina Dagyte, Kristina Grigalioniene, Dita Pelnena, Janis Stavusis, Jolanta Rozentale, Liana Pliss, Birute Burnyte, and Algirdas Utkus

Subjects

Male, 0301 basic medicine, Mitochondrial DNA, Nuclear gene, Mitochondrial disease, Biology, medicine.disease_cause, DNA, Mitochondrial, 03 medical and health sciences, 0302 clinical medicine, Genetics, medicine, Humans, Leigh disease, Molecular Biology, Mutation, Genetic heterogeneity, Point mutation, Infant, medicine.disease, 030104 developmental biology, Child, Preschool, Lactic acidosis, Female, Leigh Disease, 030217 neurology & neurosurgery

Abstract

The most common mitochondrial disorder in children is Leigh syndrome, which is a progressive and genetically heterogeneous neurodegenerative disorder caused by mutations in nuclear genes or mitochondrial DNA (mtDNA). In the present study, a novel and robust method of complete mtDNA sequencing, which allows amplification of the whole mitochondrial genome, was tested. Complete mtDNA sequencing was performed in a cohort of patients with suspected mitochondrial mutations. Patients from Latvia and Lithuania (n = 92 and n = 57, respectively) referred by clinical geneticists were included. The de novo point mutations m.9185T>C and m.13513G>A, respectively, were detected in two patients with lactic acidosis and neurodegenerative lesions. In one patient with neurodegenerative lesions, the mutation m.9185T>C was identified. These mutations are associated with Leigh syndrome. The present data suggest that full-length mtDNA sequencing is recommended as a supplement to nuclear gene testing and enzymatic assays to enhance mitochondrial disease diagnostics.

Published

2017

24. Collagen VI-related limb-girdle syndrome caused by frequent mutation in COL6A3 gene with conflicting reports of pathogenicity

Author

Cristina Domínguez-González, Janis Stavusis, Volker Straub, Luísa Panadés-de Oliveira, Ana Töpf, Nicolas Chrestian, Nathan T. Wright, Dita Kidere, Ieva Micule, Baiba Lace, and Inna Inashkina

Subjects

0301 basic medicine, Adult, Male, Bethlem Myopathy 1, Contracture, Ullrich congenital muscular dystrophy, Collagen Type VI, Biology, Compound heterozygosity, Muscular Dystrophies, 03 medical and health sciences, 0302 clinical medicine, Von Willebrand factor, Collagen VI, Exome Sequencing, medicine, Humans, Myopathy, Genetics (clinical), Genetics, Sclerosis, Middle Aged, medicine.disease, Limb-Girdle Syndrome, Pedigree, 030104 developmental biology, Neurology, Pediatrics, Perinatology and Child Health, Mutation (genetic algorithm), biology.protein, Female, Neurology (clinical), medicine.symptom, 030217 neurology & neurosurgery

Abstract

Recently the scientific community has started to view Bethlem myopathy 1 and Ullrich congenital muscular dystrophy as two extremes of a collagen VI-related myopathy spectrum rather than two separate entities, as both are caused by mutations in one of the collagen VI genes. Here we report three individuals in two families who are homozygous for a COL6A3 mutation (c.7447A> G; p.Lys2483Glu), and compare their clinical features with seven previously published cases. Individuals carrying homozygous or compound heterozygous c.7447A> G, (p.Lys2483Glu) mutation exhibit mild phenotype without loss of ambulation, similar to the cases described previously as Collagen VI-related limb-girdle syndrome. The phenotype could arise due to an aberrant assembly of Von Willebrand factor A domains. Based on these data, we propose that c.7447A> G, (p.Lys2483Glu) is a common pathogenic mutation.

Published

2019

25. HSD10 mitochondrial disease: p.Leu122Val variant, mild clinical phenotype, and founder effect in French‐Canadian patients from Quebec

Author

Serge Gravel, Renee-Myriam Boucher, Bruno Maranda, Geneviève Bernard, Baiba Lace, Sébastien Lévesque, Daniela Buhas, Paula J. Waters, and Denis Cyr

Subjects

0301 basic medicine, Proband, Male, Mitochondrial Diseases, 030105 genetics & heredity, HSD17B10, MRPP2, Missense mutation, Age of Onset, Child, Genetics (clinical), Genetics, education.field_of_study, Genetic disorder, Quebec, 3-Hydroxyacyl CoA Dehydrogenases, Genetic Diseases, X-Linked, Middle Aged, Founder Effect, HADH2, Pedigree, mitochondrial disease, Child, Preschool, Original Article, Female, Adult, lcsh:QH426-470, HSD10, Mitochondrial disease, 2‐methyl‐3‐hydroxybutyryl‐CoA dehydrogenase, Population, Mutation, Missense, 03 medical and health sciences, Young Adult, 17‐beta‐hydroxysteroid dehydrogenase X, SDR5C1, medicine, Humans, MHBD deficiency, education, Molecular Biology, Hemizygote, business.industry, Haplotype, Infant, Original Articles, medicine.disease, lcsh:Genetics, 030104 developmental biology, Amino Acid Substitution, business, Founder effect

Abstract

Background HSD10 mitochondrial disease (HSD10MD), originally described as a deficiency of 2‐methyl‐3‐hydroxybutyryl‐CoA dehydrogenase (MHBD), is a rare X‐linked disorder of a moonlighting protein encoded by the HSD17B10. The diagnosis is usually first suspected on finding elevated isoleucine degradation metabolites in urine, reflecting decreased MHBD activity. However, it is now known that clinical disease pathogenesis reflects other independent functions of the HSD10 protein; particularly its essential role in mitochondrial transcript processing and tRNA maturation. The classical phenotype of HSD10MD in affected males is an infantile‐onset progressive neurodegenerative disorder associated with severe mitochondrial dysfunction. Patients, Methods, and Results In four unrelated families, we identified index patients with MHBD deficiency, which implied a diagnosis of HSD10MD. Each index patient was independently investigated because of neurological or developmental concerns. All had persistent elevations of urinary 2‐methyl‐3‐hydroxybutyric acid and tiglylglycine. Analysis of HSD17B10 identified a single missense variant, c.364C>G, p.Leu122Val, in each case. This rare variant (1/183336 alleles in gnomAD) was previously reported in one Dutch patient and was described as pathogenic. The geographic origins of our families and results of haplotype analysis together provide evidence of a founder effect for this variant in Quebec. Notably, we identified an asymptomatic hemizygous adult male in one family, while a second independent genetic disorder contributed substantially to the clinical phenotypes observed in probands from two other families. Conclusion The phenotype associated with p.Leu122Val in HSD17B10 currently appears to be attenuated and nonprogressive. This report widens the spectrum of phenotypic severity of HSD10MD and contributes to genotype–phenotype correlation. At present, we consider p.Leu122Val a “variant of uncertain significance.” Nonetheless, careful follow‐up of our patients remains advisable, to assess long‐term clinical course and ensure appropriate management. It will also be important to identify other potential patients in our population and to characterize their phenotype., HSD10 mitochondrial disease (HSD10MD) is a rare X‐linked disorder, with a classical phenotype of infantile‐onset progressive neurodegeneration associated with severe mitochondrial dysfunction. We describe patients from four unrelated families, showing an unusually mild clinical phenotype. All patients have the p.Leu122Val variant in the HSD17B10, reflecting a founder effect.

Published

2019

26. Novel Mutations in MYBPC1 Are Associated With Myogenic Tremor and Mild Myopathy

Author

Carsten G. Bönnemann, Janis Stavusis, Baiba Lace, Nathan T. Wright, Jochen Schäfer, Dietrich Haubenberger, Aikaterini Kontrogianni-Konstantopoulos, Annika Saak, Janelle Geist, Manja Weinhold, Dita Kidere, Sandra Jackson, Inna Inashkina, and Sander Pajusalu

Subjects

0301 basic medicine, Adult, Male, Mutation, Missense, Biology, medicine.disease_cause, Article, Protein Structure, Secondary, 03 medical and health sciences, 0302 clinical medicine, Muscular Diseases, Myosin, Tremor, medicine, Missense mutation, Humans, Myopathy, Exome, Genetics, Mutation, Muscle biopsy, medicine.diagnostic_test, Middle Aged, Phenotype, Pedigree, Protein Structure, Tertiary, 030104 developmental biology, Neurology, Myosin binding, Female, Neurology (clinical), medicine.symptom, Carrier Proteins, 030217 neurology & neurosurgery

Abstract

Objective To define a distinct, dominantly inherited, mild skeletal myopathy associated with prominent and consistent tremor in two unrelated, three-generation families. Methods Clinical evaluations as well as exome and panel sequencing analyses were performed in affected and nonaffected members of two families to identify genetic variants segregating with the phenotype. Histological assessment of a muscle biopsy specimen was performed in 1 patient, and quantitative tremor analysis was carried out in 2 patients. Molecular modeling studies and biochemical assays were performed for both mutations. Results Two novel missense mutations in MYBPC1 (p.E248K in family 1 and p.Y247H in family 2) were identified and shown to segregate perfectly with the myopathy/tremor phenotype in the respective families. MYBPC1 encodes slow myosin binding protein-C (sMyBP-C), a modular sarcomeric protein playing structural and regulatory roles through its dynamic interaction with actin and myosin filaments. The Y247H and E248K mutations are located in the NH2 -terminal M-motif of sMyBP-C. Both mutations result in markedly increased binding of the NH2 terminus to myosin, possibly interfering with normal cross-bridge cycling as the first muscle-based step in tremor genesis. The clinical tremor features observed in all mutation carriers, together with the tremor physiology studies performed in family 2, suggest amplification by an additional central loop modulating the clinical tremor phenomenology. Interpretation Here, we link two novel missense mutations in MYBPC1 with a dominant, mild skeletal myopathy invariably associated with a distinctive tremor. The molecular, genetic, and clinical studies are consistent with a unique sarcomeric origin of the tremor, which we classify as "myogenic tremor." ANN NEUROL 2019.

Published

2019

27. Mutations in PIGB Cause an Inherited GPI Biosynthesis Defect with an Axonal Neuropathy and Metabolic Abnormality in Severe Cases

Author

Praveen K. Raju, Areeg El-Gharbawy, Nissan V. Baratang, Adam C. Gunning, Eriko Koshimizu, Philippe M. Campeau, Naomichi Matsumoto, Anil Vasudev Israni, Tobias B. Haack, Peter Krawitz, Jurgis Strautmanis, Jessica Sebastian, Esther M. Maier, Pengfei Liu, Samarth Kulshrestha, Ishwar C. Verma, Justine Rousseau, Florian Erger, Nami Araya, Janis Stavusis, Satoko Miyatake, Marieke Joosten, Manami Akasaka, Jill A. Rosenfeld, Elsa Rossignol, Mais Hashem, Atsushi Kamei, Inna Inashkina, Maria Eugenia Rocha, Hesham Aldhalaan, Gaku Minase, Alexej Knaus, Norbert F. Ajeawung, Gabriela Jones, Jenneke van den Ende, Thi Tuyet Mai Nguyen, Julia Baptista, Yoshiko Murakami, Ratna Dua Puri, Baiba Lace, Zita Krumina, Taroh Kinoshita, Janine Altmüller, Sian Ellard, Fowzan S. Alkuraya, and Clinical Genetics

Subjects

0301 basic medicine, Adult, Male, Glycosylphosphatidylinositols, Hearing Loss, Sensorineural, Nails, Malformed, Biology, Mannosyltransferases, Severity of Illness Index, Article, Craniofacial Abnormalities, 03 medical and health sciences, Epilepsy, Young Adult, 0302 clinical medicine, Metabolic Diseases, DOOR syndrome, Seizures, Intellectual Disability, Intellectual disability, Genetics, medicine, Polymicrogyria, Humans, Child, Genetics (clinical), Neurogenesis, Infant, Newborn, Infant, Peripheral Nervous System Diseases, medicine.disease, Phenotype, 3. Good health, Elevated alkaline phosphatase, Pedigree, 030104 developmental biology, Peripheral neuropathy, Child, Preschool, Immunology, Mutation, Female, Human medicine, medicine.symptom, Hand Deformities, Congenital, 030217 neurology & neurosurgery

Abstract

Proteins anchored to the cell surface via glycosylphosphatidylinositol (GPI) play various key roles in the human body, particularly in development and neurogenesis. As such, many developmental disorders are caused by mutations in genes involved in the GPI biosynthesis and remodeling pathway. We describe ten unrelated families with bi-allelic mutations in PIGB, a gene that encodes phosphatidy-linositol glycan class B, which transfers the third mannose to the GPI. Ten different PIGB variants were found in these individuals. Flow cytometric analysis of blood cells and fibroblasts from the affected individuals showed decreased cell surface presence of GPI-anchored proteins. Most of the affected individuals have global developmental and/or intellectual delay, all had seizures, two had polymicrogyria, and four had a peripheral neuropathy. Eight children passed away before four years old. Two of them had a clinical diagnosis of DOORS syndrome (deafness, onychodystrophy, osteodystrophy, mental retardation, and seizures), a condition that includes sensorineural deafness, shortened terminal phalanges with small finger and toenails, intellectual disability, and seizures; this condition overlaps with the severe phenotypes associated with inherited GPI deficiency. Most individuals tested showed elevated alkaline phosphatase, which is a characteristic of the inherited GPI deficiency but not DOORS syndrome. It is notable that two severely affected individuals showed 2-oxoglutaric aciduria, which can be seen in DOORS syndrome, suggesting that severe cases of inherited GPI deficiency and DOORS syndrome might share some molecular pathway disruptions.

Published

2019

28. A New Baltic Population-Specific Human Genetic Marker in the PMCA4 Gene

Author

Dita Pelnena, Janis Stavusis, Linda Piekuse, Baiba Lace, Juris Erenpreiss, Branko Zorn, Inna Inashkina, Astrida Krumina, Margus Punab, Andrey Khrunin, Violeta Fodina, Vaidutis Kučinskas, and Svetlana A. Limborska

Subjects

0301 basic medicine, Genetics, education.field_of_study, Population, Biology, medicine.disease, Male infertility, 03 medical and health sciences, 030104 developmental biology, Genetic marker, medicine, Gene family, Allele, education, Gene, Genotyping, Genetics (clinical), Sperm motility

Abstract

Objectives: The PMCA gene family consists of 4 genes and at least 21 splice variants; among these, the Ca2+ ATPase 4 (PMCA4) gene encodes a plasma membrane protein abundantly expressed in several tissues, including the kidney, heart, and sperm. Knockout of PMCA4 causes infertility due to immotile sperm in mouse models. We therefore investigated variants in this gene for potential association with infertility in groups of Estonian (n = 191) and Latvian (n = 92) men with reduced sperm motility. Methods: All exons, exon-intron boundaries, 5′ and 3′ untranslated regions, and the promoter region of the PMCA4 gene were analysed by direct sequencing for a group of Estonian infertile men. Genotyping of guanine and adenine alleles of rs147729934 was performed, using a custom-designed TaqMan® probe for a group of Latvian infertile men as well as additional groups from Latvia and several groups of people with proven ethnicity from the Baltic region. Results: Although we did not identify any significant associations between variants in the gene and infertility, our results indicated that in all studied Latvian and Estonian groups the adenine allele of the variant rs147729934 was present at a higher frequency than expected. Analysis of additional samples indicated that the adenine allele of rs147729934 likely originated once in the modern-day Baltic or western Russia area, as the frequency of the minor adenine allele observed in this region is remarkably higher than that in the general European population. Conclusions: Our results revealed no significant difference in frequencies of genetic variants in PMCA4 gene between men with normal and those with reduced sperm motility. The adenine allele of the variant rs147729934 is potentially an informative tool for future population studies concerning ancient Baltic and Finno-Ugric history.

Published

2016

29. Analysis of possible genetic risk factors contributing to development of childhood acute lymphoblastic leukaemia in the Latvian population

Author

Zane Dobele, Madara Kreile, Linda Piekuse, Zhanna Kovalova, Baiba Lace, and Dmitrijs Rots

Subjects

0301 basic medicine, Genetics, education.field_of_study, Linkage disequilibrium, business.industry, Population, Single-nucleotide polymorphism, ARID5B, General Medicine, Environmental exposure, CEBPE, IKZF1, single nucleotide polymorphisms, 03 medical and health sciences, Basic Research, 030104 developmental biology, 0302 clinical medicine, 030220 oncology & carcinogenesis, Genetic predisposition, childhood acute lymphoblastic leukaemia, Medicine, Allele, business, education, Genetic association

Abstract

Introduction Childhood acute lymphoblastic leukaemia (ALL) is a complex disease caused by a combination of genetic susceptibility and environmental exposure. Previous genome-wide association studies have reported several single nucleotide polymorphisms (SNPs) associated with the incidence of ALL. Several variations in genes encoding enzymes involved in carcinogenesis are suggested as being associated with an increased risk of ALL development. Material and methods We enrolled 77 paediatric ALL patients and 122 healthy controls, and in addition parental DNA was also available for 45 probands. SNPs rs10821936 (ARID5B), rs4132601 (IKZF1), rs2239633 (CEBPE), rs3731217 (CDKN2A) and rs1800566 (NQO1) and the presence of GSTT1 and GSTM1 null variants were detected. For statistical analysis the hybrid method of two designs ‘Haplin’ was used as well as linkage disequilibrium for family-based association studies. Results We identified the SNP rs10821936 in the ARID5B gene as being statistically significantly associated with childhood ALL, especially if the C allele is in a homozygous state, relative risk (RR) 4.65, 95% CI: 2.03–10.6, p = 0.0006. Statistically significant differences were not found in other SNPs. We found risk combinations including all five variations, the strongest association being found in a combination where all five genetic variants are in a homozygous state, CCTTTTTTCC, p = 0.032. Conclusions The identified SNP rs10821936 could serve as a potential risk marker for childhood ALL development. Further studies in an independent population are needed for verification.

Published

2016

30. CONGENITAL MYOPATHIES 1 – NEMALINE

Author

Nicolas Chrestian, Y. Labrie, M. Dugas, S. Rivest, Baiba Lace, N. Laflamme, and N. Rioux

Subjects

Neurology, Pediatrics, Perinatology and Child Health, Neurology (clinical), Genetics (clinical)

Published

2020

31. Myosin Binding Protein-C Slow in Health and Disease

Author

Christopher W. Ward, Carsten G. Bönnemann, Aikaterini Kontrogianni-Konstantopou, Janelle Geist, Nathan T. Wright, Janis Stavusis, and Baiba Lace

Subjects

Myosin-binding protein C, Biochemistry, Chemistry, Biophysics, Disease

Published

2019

32. Y-Chromosomal Lineages of Latvians in the Context of the Genetic Variation of the Eastern-Baltic Region

Author

Inese Pelnena, Astrida Krumina, Baiba Lace, Sandra Rozane, Liana Pliss, Siiri Rootsi, Agrita Puzuka, Kristiina Tambets, Viesturs Baumanis, Līga Timša, Egija Zole, Renate Ranka, Areta Sabule, and Vaidutis Kučinskas

Subjects

Genetics, education.field_of_study, Lineage (evolution), Population, Latvian, Context (language use), Biology, Haplogroup, language.human_language, Evolutionary biology, Genetic variation, language, Biological dispersal, Gene pool, education, Genetics (clinical)

Abstract

Variations of the nonrecombining Y-chromosomal region were investigated in 159 unrelated Baltic-speaking ethnic Latvians from four different geographic regions, using 28 biallelic markers and 12 short tandem repeats. Eleven different haplogroups (hgs) were detected in a regionally homogeneous Latvian population, among which N1c, R1a, and I1 cover more than 85% of its paternal lineages. When compared its closest geographic neighbors, the composition of the Latvian Y-chromosomal gene pool was found to be very similar to those of Lithuanians and Estonians. Despite the comparable frequency distribution of hg N1c in Latvians and Lithuanians with the Finno-Ugric-speaking populations from the Eastern coast of the Baltic Sea, the observed differences in allelic variances of N1c haplotypes between these two groups are in concordance with the previously stated hypothesis of different dispersal ways of this lineage in the region. More than a third of Latvian paternal lineages belong specifically to a recently defined R1a-M558 hg, indicating an influence from a common source within Eastern Slavic populations on the formation of the present-day Latvian Y-chromosome gene pool.

Published

2015

33. Lack of Association between Polymorphisms in Genes MTHFR and MDR1 with Risk of Childhood Acute Lymphoblastic Leukemia

Author

Zhanna Kovalova, Madara Kreile, Linda Piekuse, Dmitrijs Rots, Elizabete Cebura, Baiba Lace, and Marika Grutupa

Subjects

Male, Proband, Cancer Research, Linkage disequilibrium, ATP Binding Cassette Transporter, Subfamily B, Adolescent, Genotype, Epidemiology, Risk Factors, Humans, Medicine, Genetic Predisposition to Disease, Allele, Risk factor, Child, Childhood Acute Lymphoblastic Leukemia, Gene, Methylenetetrahydrofolate Reductase (NADPH2), Neoplasm Staging, Genetics, Polymorphism, Genetic, biology, business.industry, Public Health, Environmental and Occupational Health, Infant, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Prognosis, Oncology, Genetic marker, Case-Control Studies, Child, Preschool, Methylenetetrahydrofolate reductase, Immunology, biology.protein, Female, business, Follow-Up Studies

Abstract

Background: Acute lymphoblastic leukemia (ALL) is a complex disease caused by interactions between hazardous exogenous or/and endogenous agents and many mild effect inherited susceptibility mutations. Some of them are known, but their functional roles still requireinvestigation. Age is a recognized risk factor; children with disease onset after the age of ten have worse prognosis, presumably also triggered by inherited factors. Materials and Methods: The MDR1 gene polymorphisms rs1045642, rs2032582 and MTHFR gene polymorphisms rs1801131 and rs1801133 were genotyped in 68 ALL patients in remission and 102 age and gender matched controls; parental DNA samples were also available for 42 probands. Results: No case control association was found between analyzed polymorphisms and a risk of childhood ALL development. Linkage disequilibrium was not observed in a family-based association study either. Only marginal association was observed between genetic marker rs2032582A and later disease onset (p=0.04). Conclusions: Our data suggest that late age of ALL onset could be triggered by mild effect common alleles.

Published

2014

34. Duplication events downstream of IRX1 cause North Carolina macular dystrophy at the MCDR3 locus

Author

Michel Michaelides, Valentina Cipriani, Sandra Valeina, Nikolas Pontikos, Andrew R. Webster, Gavin Arno, Bernard Puech, Inna Inashkina, Veronica van Heyningen, Raquel S. Silva, Mareta Audere, Baiba Lace, Anthony T. Moore, Katrina Rutka, and Ambreen Kalhoro

Subjects

Male, Gene Expression, Neurodegenerative, Eye, Macular Degeneration, ADAMTS Proteins, Gene duplication, Chromosome Duplication, 2.1 Biological and endogenous factors, Aetiology, Tomography, Corneal Dystrophies, Hereditary, Genetics, Hereditary, Chromosomes, Human, Pair 5, Medicine, Chromosomes, Human, Pair 6, Female, Pair 6, Pair 5, NORTH CAROLINA MACULAR DYSTROPHY, Sequence Analysis, Tomography, Optical Coherence, Human, IRX1, Adult, medicine.medical_specialty, Corneal Dystrophies, Science, Genomics, Locus (genetics), Biology, Article, Retina, Chromosomes, Fetus, Molecular genetics, medicine, Humans, Family, Eye Proteins, Gene, Eye Disease and Disorders of Vision, Homeodomain Proteins, Base Sequence, Haplotype, Human Genome, Sequence Analysis, DNA, DNA, Haplotypes, Optical Coherence, Genetic Loci, Transcription Factors

Abstract

Autosomal dominant North Carolina macular dystrophy (NCMD) is believed to represent a failure of macular development. The disorder has been assigned by linkage to two loci, MCDR1 on chromosome 6q16 and MCDR3 on chromosome 5p15-p13. Recently, noncoding variants upstream ofPRDM13and a large duplication includingIRX1have been identified. However, the underlying disease-causing mechanism remains uncertain. Through a combination of sequencing studies, we report two novel overlapping duplications at the MCDR3 locus, in a gene desert downstream ofIRX1and upstream ofADAMTS16.One duplication of 43 kb was identified in nine NCMD families (with evidence for a shared ancestral haplotype), and another one of 45 kb was found in a single family. The MCDR3 locus is thus refined to a shared region of 39 kb that contains DNAse hypersensitive sites active at a restricted time window during retinal development. Publicly available data confirmed expression ofIRX1andADAMTS16in human fetal retina, withIRX1preferentially expressed in fetal macula. These findings represent a major advance in our understanding of the molecular genetics of NCMD at the MCDR3 locus and provide insights into the genetic pathways involved in human macular development.Abbreviations listaCGHarray comparative genomic hybridizationCNVCopy number variantIBDIdentical-by-descentiPSCInduced pluripotent stem cellDHSDNase hypersensitive siteHHHomozygosity HaplotypeMCDRMacular dystrophy regionNCMDNorth Carolina macular dystrophyPCRPolymerase chain reactionRCHHRegion with a Conserved Homozygosity HaplotypeSNPSingle-nucleotide polymorphismSNVSingle nucleotide variantSVStructural variantWGSWhole-genome sequencing

Published

2017

35. Novel MYBPC1 Mutations in Myopathy with Tremor

Author

Carsten G. Bönnemann, Baiba Lace, Christopher W. Ward, Janis Stavusis, Janelle Geist, and Aikaterini Kontrogianni-Konstantopou

Subjects

Pathology, medicine.medical_specialty, business.industry, Biophysics, Medicine, medicine.symptom, business, Myopathy

Published

2019

36. Impact of the genes UGT1A1, GSTT1, GSTM1, GSTA1, GSTP1 and NAT2 on acute alcohol-toxic hepatitis

Author

Valentina Sondore, Zanda Daneberga, Lilite Sadovska, Madara Kreile, Ieva Micule, Astrida Krumina, Baiba Lace, J. Keiss, Inga Kempa, and Linda Piekuse

Subjects

Toxic hepatitis, medicine.medical_specialty, QH301-705.5, Biology, medicine.disease_cause, General Biochemistry, Genetics and Molecular Biology, GSTP1, Internal medicine, Genotype, medicine, oxidative stress, hepatitis, Biology (General), Allele, Gene, pharmacogenetics, Hepatitis, General Immunology and Microbiology, General Neuroscience, medicine.disease, Endocrinology, Biochemistry, Alkaline phosphatase, medicine.symptom, General Agricultural and Biological Sciences, Oxidative stress, alcoholic

Abstract

Alcohol metabolism causes cellular damage by changing the redox status of cells. In this study, we investigated the relationship between genetic markers in genes coding for enzymes involved in cellular redox stabilization and their potential role in the clinical outcome of acute alcohol-induced hepatitis. Study subjects comprised 60 patients with acute alcohol-induced hepatitis. The control group consisted of 122 healthy non-related individuals. Eight genetic markers of the genes UGT1A1, GSTA1, GSTP1, NAT2, GSTT1 and GSTM1 were genotyped. GSTT1 null genotype was identified as a risk allele for alcohol-toxic hepatitis progression (OR 2.146, P=0.013). It was also found to correlate negatively with the level of prothrombin (β= −11.05, P=0.037) and positively with hyaluronic acid (β=170.4, P=0.014). NAT2 gene alleles rs1799929 and rs1799930 showed opposing associations with the activity of the biochemical markers γ-glutamyltransferase and alkaline phosphatase; rs1799929 was negatively correlated with γ-glutamyltransferase (β=−261.3, P=0.018) and alkaline phosphatase (β= −270.5, P=0.032), whereas rs1799930 was positively correlated with Γ-glutamyltransferase (β=325.8, P=0.011) and alkaline phosphatase (β=374.8, P=0.011). Enzymes of the glutathione S-transferase family and NAT2 enzyme play an important role in the detoxification process in the liver and demonstrate an impact on the clinical outcome of acute alcohol-induced hepatitis.

Published

2013

37. Sequencing the GRHL3 Coding Region Reveals Rare Truncating Mutations and a Common Susceptibility Variant for Nonsyndromic Cleft Palate

Author

Khalid Aldhorae, Franz-Josef Kramer, Hannah Schuenke, Gül Schmidt, Elisabeth Mangold, Johanna Klamt, Janis Stavusis, Heiko Reutter, Rudolf Reiter, Pinar Gültepe, Guntram Borck, Markus M. Nöthen, Andrea Hofmann, Miho Ishida, Bert Braumann, Ruth Raff, Philip Stanier, Nina Ishorst, Baiba Lace, Anne C. Böhmer, Michael Knapp, Alexander Hemprich, Sibylle Brosch, Lina Gölz, Gudrun E. Moore, Ann-Kathrin Hoebel, Peter Tessmann, Rimante Seselgyte, Stefanie Nowak, Kerstin U. Ludwig, Andreas Jäger, Rudolf H. Reich, and Thomas Kreusch

Subjects

0301 basic medicine, Genetic counseling, Cleft Lip, Genome-wide association study, 030105 genetics & heredity, Biology, medicine.disease_cause, Polymorphism, Single Nucleotide, 03 medical and health sciences, Open Reading Frames, Polymorphism (computer science), Report, medicine, Genetics, Coding region, Humans, Van der Woude syndrome, Genetics(clinical), Abnormalities, Multiple, Genetic Predisposition to Disease, Allele, Genetics (clinical), Alleles, Mutation, Cysts, Racial Groups, medicine.disease, Lip, Minor allele frequency, Cleft Palate, DNA-Binding Proteins, 030104 developmental biology, Case-Control Studies, Transcription Factors

Abstract

Nonsyndromic cleft lip with/without cleft palate (nsCL/P) and nonsyndromic cleft palate only (nsCPO) are the most frequent subphenotypes of orofacial clefts. A common syndromic form of orofacial clefting is Van der Woude syndrome (VWS) where individuals have CL/P or CPO, often but not always associated with lower lip pits. Recently, ∼5% of VWS-affected individuals were identified with mutations in the grainy head-like 3 gene (GRHL3). To investigate GRHL3 in nonsyndromic clefting, we sequenced its coding region in 576 Europeans with nsCL/P and 96 with nsCPO. Most strikingly, nsCPO-affected individuals had a higher minor allele frequency for rs41268753 (0.099) than control subjects (0.049; p = 1.24 × 10(-2)). This association was replicated in nsCPO/control cohorts from Latvia, Yemen, and the UK (pcombined = 2.63 × 10(-5); ORallelic = 2.46 [95% CI 1.6-3.7]) and reached genome-wide significance in combination with imputed data from a GWAS in nsCPO triads (p = 2.73 × 10(-9)). Notably, rs41268753 is not associated with nsCL/P (p = 0.45). rs41268753 encodes the highly conserved p.Thr454Met (c.1361C>T) (GERP = 5.3), which prediction programs denote as deleterious, has a CADD score of 29.6, and increases protein binding capacity in silico. Sequencing also revealed four novel truncating GRHL3 mutations including two that were de novo in four families, where all nine individuals harboring mutations had nsCPO. This is important for genetic counseling: given that VWS is rare compared to nsCPO, our data suggest that dominant GRHL3 mutations are more likely to cause nonsyndromic than syndromic CPO. Thus, with rare dominant mutations and a common risk variant in the coding region, we have identified an important contribution for GRHL3 in nsCPO.

Published

2015

38. FMR1 Linked haplotype analysis in a mentally retarded male population

Author

Natalija Pronina, Zanda Daneberga, Rita Lugovska, and Baiba Lace

Subjects

Genetics, congenital, hereditary, and neonatal diseases and abnormalities, education.field_of_study, Population, Haplotype, General Medicine, Biology, medicine.disease, FMR1, Fragile X syndrome, medicine, Dynamic mutation, Microsatellite, Allele, education, Founder effect

Abstract

Fragile X syndrome is caused by dynamic mutation of FMR1 gene CpG island CGG repeats. The underlying mutational mechanism is not fully understood. Different microsatellite markers and SNP have previously been reported as markers associated with FMR1 CGG repeat instability. The aim of the present study was to identify specific haplotypes among Latvian FXS patients and the control group with respect to allelic stability. Eleven male FXS patients and 122 control male patients participated in the study. In total, 27 different DXS548-FRAXAC1-ATL1-FRAXAC2 haplotypes were found. The prevalent haplotype in the control group was 7-4-A-5+ (rel. frequency 0.327). The prevalent haplotype associated with the FXS group was 2-2-G-4 (rel. frequency 0.818; p < 0.0001). Grey zone alleles with a long uninterrupted CGG tract at the 3’ end were significantly associated with the 2-2-G-4 haplotype (p = 0.0022). Our findings suggest that, for the Latvian population, the haplotype 2-2-G-4 is a marker of CGG tract instability. We conclude that a founder effect could not be an explanation for our findings on the basis of heterogeneity exhibited by the Latvian population and lack of studies throughout this geographical region. This data may provide evidence of different mutational pathways of expansion in the Baltic States region.

Published

2011

39. Association studies of candidate genes and cleft lip and palate taking into consideration geographical origin

Author

Linda Piekuse, Inga Kempa, Ieva Grinfelde, Janis Klovins, Liana Pliss, Astrida Krumina, Alexandre R. Vieira, and Baiba Lace

Subjects

Genetics, Candidate gene, education.field_of_study, Mitochondrial DNA, Population, Haplotype, Biology, Haplogroup, stomatognathic diseases, education, General Dentistry, Gene, Genotyping, Genetic association

Abstract

Isolated cleft lip and/or palate (CL/CLP) is a complex congenital anomaly with many contributing factors. There are several genes involved in the aetiology of CL/CLP, they are different in selected populations. In a previous study, the mitochondrial haplotypes of Latvian subjects with CL/CLP were characterized. Latvian subjects with CL/CLP have mostly mitochondrial haplogroups U4/U5 compared with the ethnic population of Latvia. The aim of this study was to stratify the results of genotyping based on European mitochondrial DNA (mtDNA) haplotypes. DNA samples from 108 patients with CL/CLP and from 182 unrelated and unaffected individuals selected randomly in Latvia (used as controls) were obtained for investigation. In this study, we analysed the data taking into consideration mitochondrial haplogroups and found that gene associations depended on the genetic origin of the population. The phenotype of patients with non-U haplotypes was associated with markers in wingless-type MMTV integration site family, member 3 (WNT3), collagen, type XI, alpha 2 (COL11A2), and fibroblast growth factor receptor 1 (FGFR1), whereas patients with U4 and U5 haplotypes showed significant association with WNT3 and COL11A2. It is unlikely that mtDNA variants play a direct role in the development of CL/CLP; rather, they may be a surrogate for population substructure and provide a tool to increase homogeneity and statistical power.

Published

2011

40. Variation in FGF1, FOXE1, and TIMP2genes is associated with nonsyndromic cleft lip with or without cleft palate

Author

Mare Saag, Kaarel Krjutškov, Andres Metspalu, Vaidutis Kučinskas, Linda Piekuse, Biruta Barkane, Triin Jagomägi, Inga Kempa, Aušra Matulevičienė, Tiit Nikopensius, Laima Ambrozaitytė, Veronika Tammekivi, Algirdas Utkus, Janis Klovins, Ilze Akota, Astrida Krumina, and Baiba Lace

Subjects

Estonia, Male, Embryology, Candidate gene, Cleft Lip, LIM-Homeodomain Proteins, Nectins, Single-nucleotide polymorphism, Biology, Polymorphism, Single Nucleotide, 03 medical and health sciences, Humans, SNP, Allele, Gene, 030304 developmental biology, Homeodomain Proteins, Genetics, Tissue Inhibitor of Metalloproteinase-2, 0303 health sciences, 030305 genetics & heredity, Haplotype, Wnt signaling pathway, Epistasis, Genetic, Forkhead Transcription Factors, Lithuania, General Medicine, Latvia, 3. Good health, Cleft Palate, Wnt Proteins, Haplotypes, Genetic Loci, Case-Control Studies, Pediatrics, Perinatology and Child Health, Fibroblast Growth Factor 1, Female, Cell Adhesion Molecules, Signal Transduction, Transcription Factors, Developmental Biology, FOXE1

Abstract

BACKGROUND: Nonsyndromic cleft lip with or without cleft palate (CL/P) is a common complex birth defect caused by the interaction between multiple genes and environmental factors. METHODS: Five hundred and eighty-seven single nucleotide polymorphisms in 40 candidate genes related to orofacial clefting were tested for association with CL/P in a clefting sample composed of 300 patients and 606 controls from Estonian, Latvian, and Lithuanian populations. RESULTS: In case-control comparisons, the minor alleles of FGF1 rs34010 (p 5 4.56 3 10 24 ), WNT9B rs4968282 (p 5 0.0013), and FOXE1 rs7860144 (p 5 0.0021) were associated with a decreased risk of CL/P. Multiple haplotypes in FGF1, FOXE1, and TIMP2 and haplotypes in WNT9B, PVRL2, and LHX8 were associated with CL/P. The strongest association was found for protective haplotype rs250092/rs34010 GT in the FGF1 gene (p 5 5.01 3 10 24 ). The strongest epistatic interaction was observed between the COL2A1 and WNT3 genes. CONCLUSIONS: Our results provide for the first time evidence implicating FGF1 in the occurrence of CL/P, and support TIMP2 and WNT9B as novel loci predisposing to CL/P. We have also replicated recently reported significant associations between variants in or near FOXE1 and CL/P. It is likely that variation in FOXE1, TIMP2, and the FGF and Wnt signaling pathway genes confers susceptibility to nonsyndromic CL/P in Northeastern European populations. Birth Defects Research (Part A) 91:218–225, 2011. 2011 Wiley-Liss, Inc.

Published

2011

41. Genetic variants in COL2A1, COL11A2, and IRF6 contribute risk to nonsyndromic cleft palate

Author

Zita Aušrelė Kučinskienė, Astrida Krumina, Laima Ambrozaitytė, Tiit Nikopensius, Veronika Tammekivi, Biruta Barkane, Linda Piekuse, Mare Saag, Ilze Akota, Kaarel Krjutškov, Vaidutis Kučinskas, Inga Prane, Aušra Matulevičienė, Triin Jagomägi, Andres Metspalu, and Baiba Lace

Subjects

Baltic States, Genetic Markers, Male, Embryology, Candidate gene, Cleft Lip, Population, Single-nucleotide polymorphism, Biology, Collagen Type XI, Polymorphism, Single Nucleotide, 03 medical and health sciences, Risk Factors, Humans, Genetic Predisposition to Disease, Allele, education, Collagen Type II, Gene, Genetic Association Studies, 030304 developmental biology, Genetics, 0303 health sciences, education.field_of_study, 030305 genetics & heredity, Haplotype, Gene Expression Regulation, Developmental, Epistasis, Genetic, General Medicine, 3. Good health, Cleft Palate, Haplotypes, Case-Control Studies, Interferon Regulatory Factors, Pediatrics, Perinatology and Child Health, Epistasis, Female, IRF6, Signal Transduction, Developmental Biology

Abstract

BACKGROUND: Orofacial clefts are among the most common birth defects with a strong genetic component. Nonsyndromic cleft palate (NSCP) is a complex malformation determined by the interaction between multiple genes and environmental risk factors. METHODS: We conducted a case-control association study to investigate the role of 40 candidate genes in predisposition to orofacial clefting. Five hundred ninety-one haplotype tagging single nucleotide polymorphism (tagSNPs) were genotyped in a clefting sample from the Baltic region, composed of 104 patients with nonsyndromic cleft palate and 606 controls from an Estonian, Latvian, and Lithuanian population. RESULTS: In case-control comparisons, the minor alleles of IRF6 rs17389541 (p 5 5.45 3 10 24 ) and COL2A1 rs1793949 (p 5 7.26 3 10 24 ) were associated with increased risk of NSCP. Multiple haplotypes in COL2A1 and COL11A2 and haplotypes in WNT3, FGFR1, and CLPTM1were associated with NSCP. The strongest associations were found for IRF6 haplotype rs17389541/rs9430018 GT (p 5 2.23 3 10 24 ) and COL2A1 haplotype rs12822608/rs6823 GC (p 5 3.68 3 10 24 ). The strongest epistatic interactions were observed between MSX1 and BMP2, FGF1 and PVRL2, and COL2A1 and FGF2 genes. CONCLUSIONS: This study provides for the first time evidence of the implication of IRF6, COL2A1, and WNT3 in the occurrence of NSCP. It is likely that variation in cartilage collagen II and XI genes, IRF6, and the Wnt and FGF signaling pathway genes contributes susceptibility to nonsyndromic cleft palate in Northeastern European populations. Birth Defects Research (Part A) 88:748– 756, 2010. 2010 Wiley-Liss, Inc.

Published

2010

42. Whole Xp Deletion in a Girl with Mental Retardation, Epilepsy, and Biochemical Features of OTC Deficiency

Author

Inga Talvik, Baiba Lace, Pille Tammur, Riina Zordania, Maire Peters, Rita Teek, Olga Zilina, Katrin Õunap, Madara Kreile, and Kairit Joost

Subjects

Genetics, Urea cycle disorder, business.industry, Ornithine transcarbamylase, medicine.disease, Epilepsy, Turner syndrome, medicine, Original Article, business, Haploinsufficiency, Skewed X-inactivation, Genetics (clinical), X chromosome, SNP array

Abstract

Background: Females with a total or partial deletion of the short arm of the X chromosome have variable features of Turner syndrome, but mental retardation (MR) rarely occurs. The haploinsufficiency of deleted genes that escape X-inactivation may explain the occurrence of MR and autism. Ornithine transcarbamylase (OTC) deficiency is the most common urea cycle disorder and is inherited in an X-linked semi-dominant trait, and the OTC gene maps to Xp21. Methods: We report on a girl with MR, epilepsy and biochemical changes characteristic of OTC deficiency but no identifiable point mutation in the OTC gene. Standard G-banding cytogenetic analysis, whole genome karyotyping, and X-inactivation studies were performed to determine the genetic etiology of the OTC deficiency in the patient. Results: Cytogenetic analysis and molecular karyotyping using SNP array revealed a deletion of the whole short arm of the X chromosome (Xp22.33–p11.1). Inactivation studies also revealed a completely skewed X-inactivation. Conclusion: Our patient presented with MR, epilepsy, and some evidence of reduced OTC activity, but performed genetic studies gave no explanation for this phenotype. We hope that this case report contributes to the understanding of the underlying genetic factors of the manifestation of X-linked disorders in female patients.

Published

2010

43. Age of SERPINA1 Gene PI Z Mutation: Swedish and Latvian Population Analysis

Author

Baiba Lace, G. Cernevska, Tomas Sveger, A. Krams, and Astrida Krumina

Subjects

Genetics, education.field_of_study, Population, Alpha (ethology), Single-nucleotide polymorphism, Biology, medicine.disease, Liver disease, Mutation (genetic algorithm), medicine, Allele, education, Gene, Allele frequency, Genetics (clinical)

Abstract

Alpha 1-antitrypsin (A1AT) deficiency, one of the most common inborn errors of metabolism in Caucasians, is characterized by a low serum concentration of A1AT and a high risk of pulmonary emphysema and liver disease. The allelic frequency for the most common protease inhibitor (PI) Z mutation in the SERPINA1 gene is 2-5% in Caucasians of European descent. The objective of our study was to estimate the PI Z mutation age using molecular analysis in Latvian and Swedish populations, which have the highest frequency of PI Z mutation. DNA samples of heterozygous and homozygous PI Z allele carriers from Latvia (n = 21) and Sweden (n = 65) were analysed; 113 unrelated healthy donors from Latvia were used as a control group. MALDI-TOF analysis was performed on all samples. Pairwise Fst was computed to compare the PI Z mutation ages between the two populations and controls. A p value less than 0.05 was considered significant. Analysis of non-recombinant SNPs revealed that the PI Z mutation age was 2902 years in Latvia (SD 1983) and 2362 years in Sweden (SD 1614) which correlates with previous studies based on microsatellite analysis.

Published

2008

44. Y-Chromosomal Lineages of Latvians in the Context of the Genetic Variation of the Eastern-Baltic Region

Author

Liana, Pliss, Līga, Timša, Siiri, Rootsi, Kristiina, Tambets, Inese, Pelnena, Egija, Zole, Agrita, Puzuka, Areta, Sabule, Sandra, Rozane, Baiba, Lace, Vaidutis, Kucinskas, Astrida, Krumina, Renate, Ranka, and Viesturs, Baumanis

Subjects

Genetic Markers, Male, Chromosomes, Human, Y, Genotype, Genetic Variation, Gene Pool, Latvia, Polymorphism, Single Nucleotide, White People, Phylogeography, Genetics, Population, Haplotypes, Humans, Phylogeny, Microsatellite Repeats

Abstract

Variations of the nonrecombining Y-chromosomal region were investigated in 159 unrelated Baltic-speaking ethnic Latvians from four different geographic regions, using 28 biallelic markers and 12 short tandem repeats. Eleven different haplogroups (hgs) were detected in a regionally homogeneous Latvian population, among which N1c, R1a, and I1 cover more than 85% of its paternal lineages. When compared its closest geographic neighbors, the composition of the Latvian Y-chromosomal gene pool was found to be very similar to those of Lithuanians and Estonians. Despite the comparable frequency distribution of hg N1c in Latvians and Lithuanians with the Finno-Ugric-speaking populations from the Eastern coast of the Baltic Sea, the observed differences in allelic variances of N1c haplotypes between these two groups are in concordance with the previously stated hypothesis of different dispersal ways of this lineage in the region. More than a third of Latvian paternal lineages belong specifically to a recently defined R1a-M558 hg, indicating an influence from a common source within Eastern Slavic populations on the formation of the present-day Latvian Y-chromosome gene pool.

Published

2014

45. Association of BMP4 polymorphisms with non-syndromic cleft lip with or without cleft palate and isolated cleft palate in Latvian and Lithuanian populations

Author

Inga, Kempa, Laima, Ambrozaitytė, Janis, Stavusis, Ilze, Akota, Biruta, Barkane, Astrida, Krumina, Aušra, Matulevičienė, Algirdas, Utkus, Vaidutis, Kučinskas, and Baiba, Lace

Subjects

Genetic Markers, Male, Guanine, Genotype, Genetic Linkage, Adenine, Cleft Lip, Lithuania, Bone Morphogenetic Protein 4, Exons, Latvia, Polymorphism, Single Nucleotide, Introns, Linkage Disequilibrium, Cleft Palate, Cytosine, Gene Frequency, Haplotypes, Case-Control Studies, Humans, Female, Thymine

Abstract

Cleft lip with or without cleft palate (CLP and CL, respectively) and isolated cleft palate (CP) represent one of the most common human birth defects, with a prevalence of approximately 1 in 300-2500 depending on the population. Formation of non-syndromic CL/CLP and CP arises from the interaction of environmental and genetic factors. The objective of this study was to investigate the association between the BMP4 gene (encoding bone morphogenetic protein 4) and non-syndromic CL/CLP and CP in order to clarify the role of this gene in the aetiology of the malformation in Latvian and Lithuanian populations. We genotyped three markers of the BMP4 gene (rs17563, rs2071047 and rs1957860) in order to perform single marker and haplotype association analyses for Latvian and Lithuanian non-syndromic CL/CLP and CP patients and controls. Transmission disequilibrium test was also conducted for Latvian and Lithuanian proband-parent trios. The case-control analysis revealed that SNP rs2071047 allele A was associated with a decreased risk of CL/CLP in the Latvian population, which was confirmed by the haplotype analysis. A modest association was detected between SNP rs1957860 and CP in the Lithuanian population, where allele C was associated with a decreased risk of this cleft phenotype, corroborating haplotype analysis data. Our findings support a role of the BMP4 gene in the aetiology of non-syndromic CL/CLP and CP in the studied populations.

Published

2014

46. Contents Vol. 82, 2016

Author

Branko Zorn, Vaidutis Kučinskas, Baiba Lace, Inna Inashkina, Susanne Rospleszcz, Linda Piekuse, Juris Erenpreiss, Andrey Khrunin, Jonathan T. L. Kang, Satz Mengensatzproduktion, Margus Punab, Noah A. Rosenberg, Amy Goldberg, Janis Stavusis, Violeta Fodina, Svetlana A. Limborska, Markus Brugger, Druckerei Stückle, Michael D. Edge, Konstantin Strauch, Dita Pelnena, Doron M. Behar, and Astrida Krumina

Subjects

Genetics, Genetics (clinical)

Published

2016

47. CAV3 gene sequence variations: National Genome Database and clinics

Author

Baiba Lace, Inna Inashkina, Janis Stavusis, Birute Burnyte, Algirdas Utkus, Jurgis Strautmanis, Ilze Radovica, Eriks Jankevics, Maruta Solvita Naudina, and Ieva Micule

Subjects

Adult, Male, Caveolin 3, Gene mutation, Biology, Bioinformatics, Exon, symbols.namesake, medicine, Missense mutation, Coding region, Humans, Muscular dystrophy, Gene, Creatine Kinase, Genetics, Muscle biopsy, medicine.diagnostic_test, General Medicine, Neuromuscular Diseases, Middle Aged, medicine.disease, Neurology, Muscular Dystrophies, Limb-Girdle, Mutation, Mendelian inheritance, symbols, Female, Neurology (clinical), Cardiomyopathies

Abstract

Introduction Caveolinopathies are a group of untreatable, degenerative muscle diseases associated with caveolin 3 (CAV3) gene mutations. Objectives The goal of this study was to characterize the role of the CAV3 gene in patients with limb-girdle muscular dystrophy, hyperCKemia, cardiomyopathies, as well as utilization of the National Genome Database in clinical applications. Materials and methods We sequenced the coding region and exon/intron boundaries of CAV3 gene in 81 neuromuscular disorder patients, a sample group from the National Genome Database, consisting of 97 individuals with cardiomyopathies, and also random selection of 100 persons. Immunohistochemical staining of muscle biopsy was performed to verify findings in one case, as the setup for the project was to use less invasive molecular biology methods. Results We identified three novel sequence variations (c.183C>G, p.S61R; c.220C>A, p.R74S; c.220C>T, p.R74C) and found evidence that one was associated with hypercreatine kinase-emia. Two previously reported mutations in families with limb-girdle muscular dystrophy were found. No mutations were identified in the cohort of patients with cardiomyopathies. Discussion CAV3 gene encodes muscle-specific protein with dominant negative type of missense mutations in it causing various phenotypes. Our study confirmed CAV3 gene involvement in neuromuscular disorders, but found no evidence in the group of patients with cardiomyopathies. Persons included in the National Genome Database could be screened for late onset Mendelian diseases.

Published

2014

48. Association between inherited monogenic liver disorders and chronic hepatitis C

Author

Valentina Sondore, Linda Piekuse, Baiba Lace, Zane Steinberga, Madara Kreile, Astrida Krumina, J. Keiss, and Agnese Zarina

Subjects

education.field_of_study, Hepatology, medicine.diagnostic_test, Brief Article, business.industry, Ribavirin, Population, Odds ratio, Hepatitis C, medicine.disease, chemistry.chemical_compound, chemistry, Pegylated interferon, Liver biopsy, Immunology, Medicine, Mutation frequency, business, education, Viral load, medicine.drug

Abstract

AIM: To determine the frequencies of mutations that cause inherited monogenic liver disorders in patients with chronic hepatitis C. METHODS: This study included 86 patients with chronic hepatitis C (55 men, 31 women; mean age at diagnosis, 38.36 ± 14.52 years) who had undergone antiviral therapy comprising pegylated interferon and ribavirin. Viral load, biochemical parameter changes, and liver biopsy morphological data were evaluated in all patients. The control group comprised 271 unrelated individuals representing the general population of Latvia for mutation frequency calculations. The most frequent mutations that cause inherited liver disorders [gene (mutation): ATP7B (H1069Q), HFE (C282Y, H63D), UGT1A1 (TA)7, and SERPINA1 (PiZ)] were detected by polymerase chain reaction (PCR), bidirectional PCR allele-specific amplification, restriction fragment length polymorphism analysis, and sequencing. RESULTS: The viral genotype was detected in 80 of the 86 patients. Viral genotypes 1, 2, and 3 were present in 61 (76%), 7 (9%), and 12 (15%) patients, respectively. Among all 86 patients, 50 (58%) reached an early viral response and 70 (81%) reached a sustained viral response. All 16 patients who did not reach a sustained viral response had viral genotype 1. Case-control analysis revealed a statistically significant difference in only the H1069Q mutation between patients and controls (patients, 0.057; controls, 0.012; odds ratio, 5.514; 95%CI: 1.119-29.827, P = 0.022). However, the H1069Q mutation was not associated with antiviral treatment outcomes or biochemical indices. The (TA) 7 mutation of the UGT1A1 gene was associated with decreased ferritin levels (beta regression coefficient = -295.7, P = 0.0087). CONCLUSION: Genetic mutations that cause inherited liver diseases in patients with hepatitis C should be studied in detail.

Published

2014

49. Clinical and biochemical features guiding the diagnostics in neurometabolic cutis laxa

Author

Michel Leão, Livia Garavelli, Dirk Lefeber, Miski Mohamed, Ron A. Wevers, Björn Fischer, Johannes Häberle, Michael W. Parker, Ariana Kariminejad, Byung Chan Lim, Martin Lammens, Deanna Guerra, Uwe Kornak, Sujatha Jagadeesh, Baiba Lace, Bert van den Heuvel, Han G. Brunner, Riikka Keski-Filppula, Thatjana Gardeitchik, Ki Joong Kim, Eva Morava, and Leo G.J. Nijtmans

Subjects

Proband, Male, Pathology, medicine.medical_specialty, Glycosylation, Adolescent, Biology, medicine.disease_cause, Article, Cutis Laxa, Epilepsy, Genetics, medicine, Guanine Nucleotide Exchange Factors, Humans, Prospective Studies, Prospective cohort study, Child, Genetics (clinical), Mutation, Neurodevelopmental disorders Donders Center for Medical Neuroscience [Radboudumc 7], Psychomotor retardation, Genetic heterogeneity, Metabolic Disorders Radboud Institute for Molecular Life Sciences [Radboudumc 6], Aldehyde Dehydrogenase, Mitochondrial Proton-Translocating ATPases, medicine.disease, Disorders of movement Donders Center for Medical Neuroscience [Radboudumc 3], Hypotonia, Renal disorders Radboud Institute for Molecular Life Sciences [Radboudumc 11], Child, Preschool, Female, Pyrroline Carboxylate Reductases, medicine.symptom, Agenesis of Corpus Callosum, Carrier Proteins, Cutis laxa

Abstract

Contains fulltext : 137634.pdf (Publisher’s version ) (Open Access) Patients with cutis laxa (CL) have wrinkled, sagging skin with decreased elasticity. Skin symptoms are associated with variable systemic involvement. The most common, genetically highly heterogeneous form of autosomal recessive CL, ARCL2, is frequently associated with variable metabolic and neurological symptoms. Progeroid symptoms, dysmorphic features, hypotonia and psychomotor retardation are highly overlapping in the early phase of these disorders. This makes the genetic diagnosis often challenging. In search for discriminatory symptoms, we prospectively evaluated clinical, neurologic, metabolic and genetic features in our patient cohort referred for suspected ARCL. From a cohort of 26 children, we confirmed mutations in genes associated with ARCL in 16 children (14 probands), including 12 novel mutations. Abnormal glycosylation and gyration abnormalities were mostly, but not always associated with ATP6V0A2 mutations. Epilepsy was most common in ATP6V0A2 defects. Corpus callosum dysgenesis was associated with PYCR1 and ALDH18A1 mutations. Dystonic posturing was discriminatory for PYCR1 and ALDH18A1 defects. Metabolic markers of mitochondrial dysfunction were found in one patient with PYCR1 mutations. So far unreported white matter abnormalities were found associated with GORAB and RIN2 mutations. We describe a large cohort of CL patients with neurologic involvement. Migration defects and corpus callosum hypoplasia were not always diagnostic for a specific genetic defect in CL. All patients with ATP6V0A2 defects had abnormal glycosylation. To conclude, central nervous system and metabolic abnormalities were discriminatory in this genetically heterogeneous group, although not always diagnostic for a certain genetic defect in CL.

Published

2014

50. Dupuytren's Contracture Cosegregation with Limb-Girdle Muscle Dystrophy

Author

Inta Vasiljeva, Inna Inashkina, Ieva Micule, Baiba Lace, Eriks Jankevics, Janis Stavusis, Maruta Solvita Naudina, and Jurgis Strautmanis

Subjects

medicine.medical_specialty, Neuromuscular disease, Cosegregation, business.industry, Case Report, Limb girdle, Muscle dystrophy, medicine.disease, Dermatology, lcsh:RC346-429, Surgery, body regions, medicine.anatomical_structure, Diabetes mellitus, medicine, Shoulder girdle, Contracture, medicine.symptom, Dupuytren's contracture, General Agricultural and Biological Sciences, business, lcsh:Neurology. Diseases of the nervous system

Abstract

Limb-girdle muscular dystrophies (LGMDs) is a heterogeneous group of muscular dystrophies that mostly affect the pelvic and shoulder girdle muscle groups. We report here a case of neuromuscular disease associated with Dupuytren's contracture, which has never been described before as cosegregating with an autosomal dominant type of inheritance. Dupuytren's contracture is a common disease, especially in Northern Europe. Comorbid conditions associated with Dupuytren's contracture are repetitive trauma to the hands, diabetes, and seizures, but it has never before been associated with neuromuscular disease. We hypothesize that patients may harbor mutations in genes with functions related to neuromuscular disease and Dupuytren's contracture development.

Published

2013