Your search keyword '"Familial"' showing total 13 results

1. Familial 4p Interstitial Deletion Provides New Insights and Candidate Genes Underlying This Rare Condition.

Author

Di, Jing, Yenwongfai, Leonard, Rieger, Hillary T., Zhang, Shulin, and Wei, Sainan

Subjects

*CHROMOSOME analysis, *FAILURE to thrive syndrome, *MEDICAL personnel, *GENES, *CHROMOSOMES, *INTELLECTUAL disabilities

Abstract

Chromosome 4p deletions can lead to two distinct phenotypic outcomes: Wolf-–Hirschhorn syndrome (a terminal deletion at 4p16.3) and less frequently reported proximal interstitial deletions (4p11-p16). Proximal 4p interstitial deletions can result in mild to moderate intellectual disability, facial dysmorphisms, and a tall thin body habitus. To date, only 35 cases of proximal 4p interstitial deletions have been reported, and only two of these cases have been familial. The critical region for this syndrome has been narrowed down to 4p15.33-15.2, but the underlying causative genes remain unclear. In this study, we report the case of a 3-year-old female with failure to thrive, developmental and motor delays, and morphological features. The mother also had a 4p15.2-p14 deletion, and the proband was found to have a 13.4-Mb 4p15.2-p14 deletion by chromosome microarray analysis. The deleted region encompasses 16 genes, five of which have a high likelihood of contributing to the phenotype: PPARGC1A, DHX15, RBPJ, STIM2, and PCDH7. These findings suggest that multiple genes are involved in this rare proximal 4p interstitial deletion syndrome. This case highlights the need for healthcare providers to be aware of proximal 4p interstitial deletions and the potential phenotypic manifestations. [ABSTRACT FROM AUTHOR]

Published

2023

2. Influence of Parent-of-Origin on Intellectual Outcomes in the Chromosome 22q11.2 Deletion Syndrome.

Author

McGinn, Daniel E., Crowley, T. Blaine, Heung, Tracy, Tran, Oanh, Moss, Edward, Zackai, Elaine H., Emanuel, Beverly S., Chow, Eva W. C., Morrow, Bernice E., Swillen, Ann, Bassett, Anne S., and McDonald-McGinn, Donna M.

Subjects

*DIGEORGE syndrome, *CHROMOSOMES, *INTELLIGENCE tests, *INTELLECTUAL disabilities, *LEARNING disabilities

Abstract

Learning and intellectual disabilities are hallmark features of 22q11.2 deletion syndrome. Data are limited, however, regarding influences on full-scale IQ (FSIQ). Here, we investigated possible 22q11.2 deletion parent-of-origin effects. In 535 individuals, we compared FSIQ (≥50), 481 with de novo and 54 with inherited 22q11.2 deletions. In the subsets with data available, we examined parent-of-origin effects on FSIQ. We used linear regression models to account for covariates. Median FSIQ was significantly higher in de novo vs. inherited deletions (77; range 50–116 vs. 67; range 50–96, p < 0.0001). Results remained significant using a regression model accounting for age at IQ testing, sex and cohort site. No significant parent-of-origin differences in FSIQ were observed for de novo deletions (n = 81, 63.0% maternal; p = 0.6882). However, median FSIQ was significantly lower in maternally than in paternally inherited familial deletions (65, range 50–86 vs. 71.5, range 58–96, respectively, p = 0.0350), with the regression model indicating an ~8 point decrement in FSIQ for this variable (p = 0.0061). FSIQ is higher on average in de novo than in inherited 22q11.2 deletions, regardless of parental origin. However, parent-of-origin appears relevant in inherited deletions. The results have potential clinical implications with further research needed to delineate possible actionable mechanisms. [ABSTRACT FROM AUTHOR]

Published

2022

3. A Case Series of Familial ARID1B Variants Illustrating Variable Expression and Suggestions to Update the ACMG Criteria

Author

Claudia A. L. Ruivenkamp, Isabelle Maystadt, Scott E. Hickey, Bert B.A. de Vries, Marielle Alders, Stéphanie Moortgat, Bregje W.M. van Bon, Jill A. Rosenfeld, Kareesma Parbhoo, Catherine Vincent-Delorme, Johan T. den Dunnen, Thomas Smol, Debra S. Regier, Pleuntje J. van der Sluijs, Gijs W. E. Santen, Alexander J. M. Dingemans, Betsy Schmalz, Erica H. Gerkes, Bekim Sadikovic, Kyra E. Stuurman, Dan Doherty, Jennifer C. Dempsey, Ilana M. Milller, Human Genetics, ACS - Pulmonary hypertension & thrombosis, ARD - Amsterdam Reproduction and Development, and Clinical Genetics

Subjects

Male, Inherited, Coffin–Siris syndrome, Intellectual disability, QH426-470, PHENOTYPE, Variable Expression, Familial, non-pathogenic, ARID1B, Loss of Function Mutation, Child, Genetics (clinical), Genetics, RISK, familial, Middle Aged, ACMG guidelines, DNA-Binding Proteins, intellectual disability, DNA methylation, Medical genetics, Female, Haploinsufficiency, Hand Deformities, Congenital, Adult, medicine.medical_specialty, GENES, Adolescent, Genomics, Biology, Non-pathogenic, Article, Young Adult, All institutes and research themes of the Radboud University Medical Center, medicine, Humans, Abnormalities, Multiple, Genetic Predisposition to Disease, AUTISM, Gene, Loss function, Sequence (medicine), COMPLEX, Neurodevelopmental disorders Donders Center for Medical Neuroscience [Radboudumc 7], DISABILITY, COFFIN-SIRIS SYNDROME, Variable expression, DNA Methylation, inherited, variable expression, Gene Expression Regulation, Face, Transcription Factors

Abstract

ARID1B is one of the most frequently mutated genes in intellectual disability (~1%). Most variants are readily classified, since they are de novo and are predicted to lead to loss of function, and therefore classified as pathogenic according to the American College of Medical Genetics and Genomics (ACMG) guidelines for the interpretation of sequence variants. However, familial loss-of-function variants can also occur and can be challenging to interpret. Such variants may be pathogenic with variable expression, causing only a mild phenotype in a parent. Alternatively, since some regions of the ARID1B gene seem to be lacking pathogenic variants, loss-of-function variants in those regions may not lead to ARID1B haploinsufficiency and may therefore be benign. We describe 12 families with potential loss-of-function variants, which were either familial or with unknown inheritance and were in regions where pathogenic variants have not been described or are otherwise challenging to interpret. We performed detailed clinical and DNA methylation studies, which allowed us to confidently classify most variants. In five families we observed transmission of pathogenic variants, confirming their highly variable expression. Our findings provide further evidence for an alternative translational start site and we suggest updates for the ACMG guidelines for the interpretation of sequence variants to incorporate DNA methylation studies and facial analyses.

Published

2021

4. Genetic Background of Congenital Erythrocytosis

Author

Mary Frances McMullin

Subjects

0301 basic medicine, Congenital erythrocytosis, Review, Polycythemia, QH426-470, Hematocrit, Bioinformatics, Infant, Newborn, Diseases, 03 medical and health sciences, 0302 clinical medicine, Elevated hemoglobin, Genetics, medicine, erythrocytosis, Humans, Genetics(clinical), Family history, Genetics (clinical), oxygen sensing pathway, medicine.diagnostic_test, Red Cell, business.industry, Clinical course, congenital, Infant, Newborn, familial, Young age, 030104 developmental biology, Erythropoietin, Mutation, erythropoietin, business, 030215 immunology, medicine.drug

Abstract

True erythrocytosis is present when the red cell mass is greater than 125% of predicted sex and body mass, which is reflected by elevated hemoglobin and hematocrit. Erythrocytosis can be primary or secondary and congenital or acquired. Congenital defects are often found in those diagnosed at a young age and with a family history of erythrocytosis. Primary congenital defects mainly include mutations in the Erythropoietin receptor gene but SH2B3 has also been implicated. Secondary congenital erythrocytosis can arise through a variety of genetic mechanisms, including mutations in the genes in the oxygen sensing pathway, with high oxygen affinity hemoglobin variants and mutations in other genes such as BPMG, where ultimately the production of erythropoietin is increased, resulting in erythrocytosis. Recently, mutations in PIEZ01 have been associated with erythrocytosis. In many cases, a genetic variant cannot be identified, leaving a group of patients with the label idiopathic erythrocytosis who should be the subject of future investigations. The clinical course in congenital erythrocytosis is hard to evaluate as these are rare cases. However, some of these patients may well present at a young age and with sometimes catastrophic thromboembolic events. There is little evidence to guide the management of congenital erythrocytosis but the use of venesection and low dose aspirin should be considered.

Published

2021

5. ATTRv in Lazio-Italy: A High-Prevalence Region in a Non-Endemic Country

Author

Antonio Petrucci, Antonio Di Muzio, Roberto Massa, Vincenzo Di Lazzaro, Carlo Casali, Mariangela Goglia, Emanuela Proietti, Mario Sabatelli, Marco Luigetti, Maurizio Inghilleri, Maria Grazia Chiappini, Marco Di Girolamo, Giovanni Antonini, Luca Leonardi, Marco Ceccanti, Laura De Giglio, Elena Maria Pennisi, Marianna Gabriella Rispoli, and Valeria Guglielmino

Subjects

0301 basic medicine, Adult, Male, Population, prevalence, Disease, QH426-470, Amyloid Neuropathies, Settore MED/26, 03 medical and health sciences, 0302 clinical medicine, Familial, ATTRv, 80 and over, Genetics, Medicine, Effective treatment, Humans, Non endemic, education, Genetics (clinical), Aged, Aged, 80 and over, Amyloid Neuropathies, Familial, education.field_of_study, Amyloid, Prevalence, Female, Genetic Carrier Screening, Hospitals, Italy, Middle Aged, business.industry, Brief Report, Amyloidosis, amyloid, medicine.disease, 030104 developmental biology, Lazio region, 030220 oncology & carcinogenesis, business, Demography

Abstract

Hereditary transthyretin amyloidosis (ATTRv, v for variant) prevalence in Italy, a non-endemic region, has been established by ATTRv amyloidosis Italian Registry. However, values of prevalence were extremely heterogeneous, considering different regions. To properly establish the prevalence of the disease in the Lazio region, a survey was sent to university regional hospitals and to main regional hospitals, in order to collect all affected patients regularly followed. We identified 100 ATTRv patients and, considering a Lazio population of 5.8/million, we estimated a ATTRv prevalence of 17.2/million. The ATTRv amyloidosis Italian Registry reported a prevalence of 8.0/million in Lazio, while our survey showed a value of double this. Our survey documented a high-prevalence for a non-endemic country. The increased awareness of the disease among general practitioners and medical specialists is a fundamental step to reduce the diagnostic delay and start an effective treatment of this disease.

Published

2021

6. Hunting for Familial Parkinson’s Disease Mutations in the Post Genome Era

Author

Holly E. Sherman, Stephen A. Wood, Alex M. Sykes, Peter A. Silburn, Steven R. Bentley, Ilaria Guella, Hannah M. Neuendorf, Javed Fowdar, Matthew J. Farrer, and George D. Mellick

Subjects

0301 basic medicine, Male, Heterozygote, lcsh:QH426-470, Mutation, Missense, Disease, Biology, medicine.disease_cause, Article, 03 medical and health sciences, 0302 clinical medicine, Exome Sequencing, Genetics, medicine, Missense mutation, Humans, Genetic Predisposition to Disease, Family history, Potassium Channels, Inwardly Rectifying, Exome, Genetics (clinical), Exome sequencing, parkinsonism, Mutation, multi-incident, Parkinsonism, GTPase-Activating Proteins, High-Throughput Nucleotide Sequencing, familial, Parkinson Disease, medicine.disease, LRRK2, nervous system diseases, Pedigree, lcsh:Genetics, 030104 developmental biology, Female, movement disorder, mutation, 030217 neurology & neurosurgery, exome

Abstract

Parkinson’s disease (PD) is typically sporadic, however, multi-incident families provide a powerful platform to discover novel genetic forms of disease. Their identification supports deciphering molecular processes leading to disease and may inform of new therapeutic targets. The LRRK2 p.G2019S mutation causes PD in 42.5–68% of carriers by the age of 80 years. We hypothesise similarly intermediately penetrant mutations may present in multi-incident families with a generally strong family history of disease. We have analysed six multiplex families for missense variants using whole exome sequencing to find 32 rare heterozygous mutations shared amongst affected members. Included in these mutations was the KCNJ15 p.R28C variant, identified in five affected members of the same family, two elderly unaffected members of the same family, and two unrelated PD cases. Additionally, the SIPA1L1 p.R236Q variant was identified in three related affected members and an unrelated familial case. While the evidence presented here is not sufficient to assign causality to these rare variants, it does provide novel candidates for hypothesis testing in other modestly sized families with a strong family history. Future analysis will include characterisation of functional consequences and assessment of carriers in other familial cases.

Published

2021

7. Ocular Involvement in Hereditary Amyloidosis

Author

Roberta Rissotto, Marco Luigetti, Elena Antoniazzi, Marco Di Girolamo, Laura Obici, Daniela Bacherini, Benedetto Falsini, Martina Maceroni, Stanislao Rizzo, and Angelo Maria Minnella

Subjects

Pathology, Eye Diseases, genetic structures, gelsolin, ocular amyloidosis, Review, Retinal Pigment Epithelium, QH426-470, Amyloid Neuropathies, chemistry.chemical_compound, Amyloid disease, Familial, 0302 clinical medicine, Transforming Growth Factor beta, Cornea, Prealbumin, Genetics (clinical), Extracellular Matrix Proteins, biology, keratoepithelin, Settore MED/30 - MALATTIE APPARATO VISIVO, Amyloidosis, amyloid, personalized medicine, Transport protein, medicine.anatomical_structure, vitreous opacities, Amyloidosis, Familial, medicine.medical_specialty, Amyloid, vitrectomy, ATTR, corneal lattice dystrophy, transthyretin, 03 medical and health sciences, Genetics, medicine, Humans, Genetic Predisposition to Disease, amyloidosis, Amyloid Neuropathies, Familial, business.industry, Retinal, medicine.disease, eye diseases, Transthyretin, chemistry, 030221 ophthalmology & optometry, biology.protein, sense organs, business, Gelsolin, 030217 neurology & neurosurgery

Abstract

The term amyloidosis describes a group of rare diseases caused by protein conformation abnormalities resulting in extracellular deposition and accumulation of insoluble fibrillar aggregates. So far, 36 amyloid precursor proteins have been identified, and each one is responsible for a specific disease entity. Transthyretin amyloidosis (ATTRv) is one of the most common forms of systemic and ocular amyloidosis, due to the deposition of transthyretin (TTR), which is a transport protein mainly synthesized in the liver but also in the retinal pigment epithelial cells. ATTRv amyloidosis may be misdiagnosed with several other conditions, resulting in a significant diagnostic delay. Gelsolin and keratoepithelin are other proteins that, when mutated, are responsible for a systemic amyloid disease with significant ocular manifestations that not infrequently appear before systemic involvement. The main signs of ocular amyloid deposition are in the cornea, irido-corneal angle and vitreous, causing complications related to vasculopathy and neuropathy at the local level. This review aims at describing the main biochemical, histopathological and clinical features of systemic amyloidosis associated with eye involvement, with particular emphasis on the inherited forms. We discuss currently available treatments, focusing on ocular involvement and specific ophthalmologic management and highlighting the importance of a prompt treatment for the potential sight-threatening complications derived from amyloid deposition in ocular tissues.

Published

2021

8. A Case Series of Familial ARID1B Variants Illustrating Variable Expression and Suggestions to Update the ACMG Criteria.

Author

van der Sluijs, Pleuntje J., Alders, Mariëlle, Dingemans, Alexander J. M., Parbhoo, Kareesma, van Bon, Bregje W., Dempsey, Jennifer C., Doherty, Dan, den Dunnen, Johan T., Gerkes, Erica H., Milller, Ilana M., Moortgat, Stephanie, Regier, Debra S., Ruivenkamp, Claudia A. L., Schmalz, Betsy, Smol, Thomas, Stuurman, Kyra E., Vincent-Delorme, Catherine, de Vries, Bert B. A., Sadikovic, Bekim, and Hickey, Scott E.

Subjects

*MEDICAL genetics, *MEDICAL genomics, *DNA methylation, *PHENOTYPES, *INTELLECTUAL disabilities

Abstract

ARID1B is one of the most frequently mutated genes in intellectual disability (~1%). Most variants are readily classified, since they are de novo and are predicted to lead to loss of function, and therefore classified as pathogenic according to the American College of Medical Genetics and Genomics (ACMG) guidelines for the interpretation of sequence variants. However, familial loss-of-function variants can also occur and can be challenging to interpret. Such variants may be pathogenic with variable expression, causing only a mild phenotype in a parent. Alternatively, since some regions of the ARID1B gene seem to be lacking pathogenic variants, loss-of-function variants in those regions may not lead to ARID1B haploinsufficiency and may therefore be benign. We describe 12 families with potential loss-of-function variants, which were either familial or with unknown inheritance and were in regions where pathogenic variants have not been described or are otherwise challenging to interpret. We performed detailed clinical and DNA methylation studies, which allowed us to confidently classify most variants. In five families we observed transmission of pathogenic variants, confirming their highly variable expression. Our findings provide further evidence for an alternative translational start site and we suggest updates for the ACMG guidelines for the interpretation of sequence variants to incorporate DNA methylation studies and facial analyses. [ABSTRACT FROM AUTHOR]

Published

2021

9. Molecular Pathways Involved in the Development of Congenital Erythrocytosis.

Author

Tomc, Jana and Debeljak, Nataša

Subjects

*POLYCYTHEMIA, *BIOLOGICAL transport, *CELLULAR signal transduction, *IRON metabolism, *POST-translational modification, *GENETIC testing, *ERYTHROCYTES, *HOMEOSTASIS

Abstract

Patients with idiopathic erythrocytosis are directed to targeted genetic testing including nine genes involved in oxygen sensing pathway in kidneys, erythropoietin signal transduction in pre-erythrocytes and hemoglobin-oxygen affinity regulation in mature erythrocytes. However, in more than 60% of cases the genetic cause remains undiagnosed, suggesting that other genes and mechanisms must be involved in the disease development. This review aims to explore additional molecular mechanisms in recognized erythrocytosis pathways and propose new pathways associated with this rare hematological disorder. For this purpose, a comprehensive review of the literature was performed and different in silico tools were used. We identified genes involved in several mechanisms and molecular pathways, including mRNA transcriptional regulation, post-translational modifications, membrane transport, regulation of signal transduction, glucose metabolism and iron homeostasis, which have the potential to influence the main erythrocytosis-associated pathways. We provide valuable theoretical information for deeper insight into possible mechanisms of disease development. This information can be also helpful to improve the current diagnostic solutions for patients with idiopathic erythrocytosis. [ABSTRACT FROM AUTHOR]

Published

2021

10. Genetic Background of Congenital Erythrocytosis.

Author

McMullin, Mary Frances

Subjects

*POLYCYTHEMIA, *GENETIC variation, *HEMOGLOBIN polymorphisms, *ERYTHROCYTES, *HUMAN abnormalities, *ERYTHROPOIETIN receptors

Abstract

True erythrocytosis is present when the red cell mass is greater than 125% of predicted sex and body mass, which is reflected by elevated hemoglobin and hematocrit. Erythrocytosis can be primary or secondary and congenital or acquired. Congenital defects are often found in those diagnosed at a young age and with a family history of erythrocytosis. Primary congenital defects mainly include mutations in the Erythropoietin receptor gene but SH2B3 has also been implicated. Secondary congenital erythrocytosis can arise through a variety of genetic mechanisms, including mutations in the genes in the oxygen sensing pathway, with high oxygen affinity hemoglobin variants and mutations in other genes such as BPMG, where ultimately the production of erythropoietin is increased, resulting in erythrocytosis. Recently, mutations in PIEZ01 have been associated with erythrocytosis. In many cases, a genetic variant cannot be identified, leaving a group of patients with the label idiopathic erythrocytosis who should be the subject of future investigations. The clinical course in congenital erythrocytosis is hard to evaluate as these are rare cases. However, some of these patients may well present at a young age and with sometimes catastrophic thromboembolic events. There is little evidence to guide the management of congenital erythrocytosis but the use of venesection and low dose aspirin should be considered. [ABSTRACT FROM AUTHOR]

Published

2021

11. At the X-Roads of Sex and Genetics in Pulmonary Arterial Hypertension

Author

Samuel M. Brown, Greg Elliott, Tim Lahm, Meghan M. Cirulis, Lynn M. Brown, and Mark W. Dodson

Subjects

Male, lcsh:QH426-470, medicine.drug_class, Review, 030204 cardiovascular system & hematology, Bone Morphogenetic Protein Receptors, Type II, Bone morphogenetic protein, Bioinformatics, 03 medical and health sciences, 0302 clinical medicine, Mediator, estradiol, bone morphogenetic protein receptor type 2, gender, estrogen, Genetics, medicine, Animals, Humans, Bone morphogenetic protein receptor, penetrance, Receptor, Genetics (clinical), Pulmonary Arterial Hypertension, business.industry, familial, Estrogens, PAH, heritable, medicine.disease, Pulmonary hypertension, BMPR2, lcsh:Genetics, medicine.anatomical_structure, 030228 respiratory system, Estrogen, Vascular resistance, Female, business, Signal Transduction

Abstract

Group 1 pulmonary hypertension (pulmonary arterial hypertension; PAH) is a rare disease characterized by remodeling of the small pulmonary arteries leading to progressive elevation of pulmonary vascular resistance, ultimately leading to right ventricular failure and death. Deleterious mutations in the serine-threonine receptor bone morphogenetic protein receptor 2 (BMPR2; a central mediator of bone morphogenetic protein (BMP) signaling) and female sex are known risk factors for the development of PAH in humans. In this narrative review, we explore the complex interplay between the BMP and estrogen signaling pathways, and the potentially synergistic mechanisms by which these signaling cascades increase the risk of developing PAH. A comprehensive understanding of these tangled pathways may reveal therapeutic targets to prevent or slow the progression of PAH.

Published

2020

12. Hunting for Familial Parkinson's Disease Mutations in the Post Genome Era.

Author

Bentley, Steven R., Guella, Ilaria, Sherman, Holly E., Neuendorf, Hannah M., Sykes, Alex M., Fowdar, Javed Y., Silburn, Peter A., Wood, Stephen A., Farrer, Matthew J., Mellick, George D., and Koks, Sulev

Subjects

*PARKINSON'S disease, *EXOMES, *FAMILY history (Medicine), *GENETIC disorders, *GENOMES

Abstract

Parkinson's disease (PD) is typically sporadic; however, multi-incident families provide a powerful platform to discover novel genetic forms of disease. Their identification supports deciphering molecular processes leading to disease and may inform of new therapeutic targets. The LRRK2 p.G2019S mutation causes PD in 42.5–68% of carriers by the age of 80 years. We hypothesise similarly intermediately penetrant mutations may present in multi-incident families with a generally strong family history of disease. We have analysed six multiplex families for missense variants using whole exome sequencing to find 32 rare heterozygous mutations shared amongst affected members. Included in these mutations was the KCNJ15 p.R28C variant, identified in five affected members of the same family, two elderly unaffected members of the same family, and two unrelated PD cases. Additionally, the SIPA1L1 p.R236Q variant was identified in three related affected members and an unrelated familial case. While the evidence presented here is not sufficient to assign causality to these rare variants, it does provide novel candidates for hypothesis testing in other modestly sized families with a strong family history. Future analysis will include characterisation of functional consequences and assessment of carriers in other familial cases. [ABSTRACT FROM AUTHOR]

Published

2021

13. At the X-Roads of Sex and Genetics in Pulmonary Arterial Hypertension.

Author

Cirulis, Meghan M., Dodson, Mark W., Brown, Lynn M., Brown, Samuel M., Lahm, Tim, and Elliott, Greg

Subjects

*PULMONARY hypertension, *BONE morphogenetic proteins, *GENETICS, *BONE morphogenetic protein receptors, *PERSISTENT fetal circulation syndrome, *VASCULAR resistance, *PULMONARY circulation

Abstract

Group 1 pulmonary hypertension (pulmonary arterial hypertension; PAH) is a rare disease characterized by remodeling of the small pulmonary arteries leading to progressive elevation of pulmonary vascular resistance, ultimately leading to right ventricular failure and death. Deleterious mutations in the serine-threonine receptor bone morphogenetic protein receptor 2 (BMPR2; a central mediator of bone morphogenetic protein (BMP) signaling) and female sex are known risk factors for the development of PAH in humans. In this narrative review, we explore the complex interplay between the BMP and estrogen signaling pathways, and the potentially synergistic mechanisms by which these signaling cascades increase the risk of developing PAH. A comprehensive understanding of these tangled pathways may reveal therapeutic targets to prevent or slow the progression of PAH. [ABSTRACT FROM AUTHOR]

Published

2020