ABSTRACT
BACKGROUND: Facial asymmetry when crying at birth (then called asymmetric crying facies or ACF) or when smiling or speaking loudly in adulthood is the consequence of the agenesis or hypoplasia of the muscle of one of the labial commissures. This developmental disorder of complex mechanism is well known by pediatricians to be a warning sign for underlying developmental disorders of variable severity. CASE REPORT: An 80-year-old man with medical history of renal agenesis was hospitalized for a transient motor deficit of the right face and arm revealing a lacunar stroke. Clinical examination showed an isolated left facial asymmetry upon smiling or talking out loud which had been known since childhood and was not related to the stroke, leading to the diagnosis of ACF. Cardiac ultrasound revealed a patent foramen. Chromosomal investigations could not be performed. DISCUSSION AND CONCLUSION: ACF is a rare disorder that may conceal associated congenital disorders such as heart, skeletal, or renal malformations. Its causing mechanisms are to this day still poorly understood but may include a genetic component as shown by familial cases and the identification of 22q11.2 deletions or trisomy 18 in some patients. Knowledge of this disorder seems highly relevant for adult neurologists, first because of the differential diagnosis with facial palsy, but mostly because it will allow them to screen patients for other congenital disorders such as heart malformations. Conversely, cardiologists and cardiac surgeon may search for an ACF when faced with a patient with a congruent heart defect.
Subject(s)
Facial Paralysis , Heart Defects, Congenital , Infant, Newborn , Male , Adult , Humans , Aged , Child , Aged, 80 and over , Facial Asymmetry/complications , Facial Asymmetry/congenital , Facial Asymmetry/genetics , Facial Paralysis/diagnosis , Facial Paralysis/etiology , Heart , Facial MusclesABSTRACT
OBJECTIVE: To resolve how the preferred chewing side (PCS) affects facial asymmetry in twins, whether there are differences between monozygotic (MZ) and dizygotic (DZ) twins, and whether the twins with PCS have more asymmetric faces compared to symmetrically chewing twins. MATERIAL AND METHODS: The study included 106 Lithuanian twin pairs of the same sex, 59 MZ and 47 DZ pairs. The data were analysed from facial 3D images and manually added landmarks. 3D images were analysed by Rapidform2006 software and statistical analyses were done by using the R software environment version 4.1.0. RESULTS: The contralateral effect of PCS and larger chin side was dominant among right and non-right side chewing twins. Being female increased the whole face symmetry. CONCLUSION: The volume of the chin becomes larger on the side opposite to the twins' habitual chewing side. As the results are quite similar in both twin types, functional factors are more prominent than heredity.
Subject(s)
Facial Asymmetry , Mastication , Face , Facial Asymmetry/genetics , Female , Humans , Twins, Dizygotic/genetics , Twins, Monozygotic/geneticsABSTRACT
BACKGROUND: Developmental instability is a component of non-genetic variation that results from random variation in developmental processes. It is considered a sensitive indicator of the physiological state of individuals. It is reflected in various ways, but in this study we focussed on its reflection in fluctuating asymmetry (FA) and morphological integration. AIM: To assess how, if at all, variations of facial morphology mirror developmental instability across childhood with respect to sex, growth rate and socioeconomic/environmental factors. SUBJECTS AND METHODS: A set of 210 three-dimensional facial models (of children aged between 6.3 and 14.3 years) originating from the FIDENTIS 3D Face Database was subjected to landmark-based methods of geometric morphometrics to quantify the degree of facial asymmetry and facial morphological integration. In addition, the association with age, sex, and socioeconomic factors was assessed. RESULTS: Our results showed a nonlinear increase of FA with age up to the age of 14 years. The pattern of sex-related variants in facial FA differed in relation to age, as girls exhibited higher values of FA than boys up to the age of 9 years. We found that a signal of modularity based on functional demands and organisation of the face is of particular importance. Here, girls exhibited higher morphological covariation among modules. During more rapid adolescence-related growth, however, covariation among modules at the asymmetrical level decreased in both sexes. CONCLUSION: We can conclude that facial morphology was shown to be strongly integrated, particularly until adolescence. This covariation can facilitate an increase of FA. In addition, the results of this study indicate there is a weak association between socioeconomic stress and facial asymmetries. In contrast, sex and growth rate are reflected in developmental instability.
Subject(s)
Face , Facial Asymmetry , Adolescent , Child , Facial Asymmetry/genetics , Female , Head , Humans , Male , Socioeconomic FactorsABSTRACT
PURPOSE OF REVIEW: The current review aims to discuss the incorporation of facial recognition software into the clinical practice of dysmorphology and medical genetics. RECENT FINDINGS: Facial recognition software has improved the process of generating a differential diagnosis for rare genetic syndromes, and recent publications demonstrate utility in both research and clinical applications. Software programs are freely available to verified medical providers and can be incorporated into routine clinic encounters. SUMMARY: As facial recognition software capabilities improve, two-dimensional image capture with artificial intelligence interpretation may become a useful tool within many areas of medicine. Geneticists and researchers can use such software to enhance their differential diagnoses, to study similarities and differences between patient cohorts, and to improve the interpretation of genomic data. Pediatricians and subspecialists may use tools to identify patients who may benefit from a genetic evaluation, and educators can use these tools to interest students in the study of dysmorphoplogy and genetic syndromes.
Subject(s)
Congenital Abnormalities/diagnosis , Facial Asymmetry/diagnosis , Facial Recognition , Software , Diagnosis, Differential , Face/abnormalities , Facial Asymmetry/genetics , Humans , Image Processing, Computer-Assisted , PhenotypeABSTRACT
Hemifacial microsomia (HFM) is a rare, multisystemic congenital disease with estimated frequency of 1/26370 births in Europe. Most cases are sporadic and caused by unilateral abnormal morphogenesis of the first and second pharyngeal arches. The aim of this study is to define the types and frequency of maxillofacial and systemic malformations in HFM patients. This is a case series study of patients with HFM evaluated at a single institution. Data were acquired through history, physical examination, photographs, diagnostic radiology, and laboratory and analyzed by the FileMakerPro database on 95 patients (54F; 41M) of which 89 met the inclusion criteria. Mandibular hypoplasia was observed in 86 patients with right-side preponderance (50). One patient had bilateral mandibular hypoplasia. Seventy-four had external ear anomalies (anotia or microtia). Eleven had bilateral malformed ears. Hearing impairment, associated with stenosis or atresia of the external ear canal, was found in 69 patients (eight with bilateral canal defects). Ocular anomalies were seen in 41 (23 with dermoid cysts) and 39 had orbital malformations. Facial nerve paralysis was observed in 38 patients. Cleft lip/palate (10), preauricular tags (55), and macrostomia (41) were also described. A total of 73/86 had systemic malformations, mainly vertebral (40), genitourinary (25), and cardiovascular (28). Sixteen had cerebral anomalies (four with intellectual disability). All patients suspected of HFM should undergo a complete systematic clinical and imaging investigation to define the full scope of anomalies. Since the disease is rare and complex, affected patients should be monitored by specialized multidisciplinary team centers.
Subject(s)
Cleft Lip/genetics , Facial Asymmetry/genetics , Goldenhar Syndrome/genetics , Maxillofacial Abnormalities/genetics , Abnormalities, Multiple/diagnosis , Abnormalities, Multiple/genetics , Adolescent , Child , Child, Preschool , Cleft Lip/diagnosis , Cleft Lip/physiopathology , Cleft Palate/diagnosis , Cleft Palate/genetics , Cleft Palate/physiopathology , Ear, External/abnormalities , Facial Asymmetry/diagnosis , Facial Asymmetry/physiopathology , Female , Goldenhar Syndrome/diagnosis , Goldenhar Syndrome/physiopathology , Humans , Infant , Male , Mandible/abnormalities , Maxillofacial Abnormalities/diagnosis , Maxillofacial Abnormalities/physiopathology , Middle Aged , Young AdultABSTRACT
INTRODUCTION: We investigated whether ACTN3, ENPP1, ESR1, PITX1, and PITX2 genes which contribute to sagittal and vertical malocclusions also contribute to facial asymmetries and temporomandibular disorders (TMD) before and after orthodontic and orthognathic surgery treatment. METHODS: One hundred seventy-four patients with a dentofacial deformity were diagnosed as symmetric or subdivided into 4 asymmetric groups according to posteroanterior cephalometric measurements. TMD examination diagnosis and jaw pain and function (JPF) questionnaires assessed the presence and severity of TMD. RESULTS: Fifty-two percent of the patients were symmetric, and 48% were asymmetric. The asymmetry classification demonstrated significant cephalometric differences between the symmetric and asymmetric groups, and across the 4 asymmetric subtypes: group 1, mandibular body asymmetry; group 2, ramus asymmetry; group 3, atypical asymmetry; and group 4, C-shaped asymmetry. ENPP1 SNP-rs6569759 was associated with group 1 (P = 0.004), and rs858339 was associated with group 3 (P = 0.002). ESR1 SNP-rs164321 was associated with group 4 (P = 0.019). These results were confirmed by principal component analysis that showed 3 principal components explaining almost 80% of the variations in the studied groups. Principal components 1 and 2 were associated with ESR1 SNP-rs3020318 (P <0.05). Diagnoses of disc displacement with reduction, masticatory muscle myalgia, and arthralgia were highly prevalent in the asymmetry groups, and all had strong statistical associations with ENPP1 rs858339. The average JPF scores for asymmetric subjects before surgery (JPF, 7) were significantly higher than for symmetric subjects (JPF, 2). Patients in group 3 had the highest preoperative JPF scores, and groups 2 and 3 were most likely to be cured of TMD 1 year after treatment. CONCLUSIONS: Posteroanterior cephalometrics can classify asymmetry into distinct groups and identify the probability of TMD and genotype associations. Orthodontic and orthognathic treatments of facial asymmetry are effective at eliminating TMD in most patients.
Subject(s)
Dentofacial Deformities/classification , Dentofacial Deformities/genetics , Estrogen Receptor alpha/genetics , Facial Asymmetry/classification , Facial Asymmetry/genetics , Phosphoric Diester Hydrolases/genetics , Pyrophosphatases/genetics , Temporomandibular Joint Disorders/genetics , Adult , Dentofacial Deformities/complications , Dentofacial Deformities/surgery , Facial Asymmetry/complications , Facial Asymmetry/surgery , Female , Genotype , Humans , Male , Orthognathic Surgical Procedures , Postoperative Complications/etiology , Severity of Illness Index , Temporomandibular Joint Disorders/etiologyABSTRACT
Facial analysis systems are becoming available to healthcare providers to aid in the recognition of dysmorphic phenotypes associated with a multitude of genetic syndromes. These technologies automatically detect facial points and extract various measurements from images to recognize dysmorphic features and evaluate similarities to known facial patterns (gestalts). To evaluate such systems' usefulness for supporting the clinical practice of healthcare professionals, the recognition accuracy of the Cornelia de Lange syndrome (CdLS) phenotype was examined with FDNA's automated facial dysmorphology novel analysis (FDNA) technology. In the first experiment, 2D facial images of CdLS patients with either an NIPBL or SMC1A gene mutation as well as non-CdLS patients which were assessed by dysmorphologists in a previous study were evaluated by the FDNA technology; the average detection rate of experts was 77% while the system's detection rate was 87%. In the second study, when a new set of NIPBL, SMC1A and non-CdLS patient photos was evaluated, the detection rate increased to 94%. The results from both studies indicated that the system's detection rate was comparable to that of dysmorphology experts. Therefore, utilizing such technologies may be a useful tool in a clinical setting.
Subject(s)
De Lange Syndrome/genetics , Face/abnormalities , Facial Asymmetry/genetics , Image Processing, Computer-Assisted/methods , Cell Cycle Proteins/genetics , Chromosomal Proteins, Non-Histone/genetics , De Lange Syndrome/diagnosis , Diagnosis, Differential , Facial Asymmetry/diagnosis , Facies , Female , Humans , Male , Mutation , Phenotype , Proteins/genetics , Reproducibility of Results , Sensitivity and SpecificityABSTRACT
Cornelia de Lange syndrome is a multisystemic developmental disorder mainly related to de novo heterozygous NIPBL mutation. Recently, NIPBL somatic mosaicism has been highlighted through buccal cell DNA study in some patients with a negative molecular analysis on leukocyte DNA. Here, we present a series of 38 patients with a Cornelia de Lange syndrome related to a heterozygous NIPBL mutation identified by Sanger sequencing. The diagnosis was based on the following criteria: (i) intrauterine growth retardation and postnatal short stature, (ii) feeding difficulties and/or gastro-oesophageal reflux, (iii) microcephaly, (iv) intellectual disability, and (v) characteristic facial features. We identified 37 novel NIPBL mutations including 34 in leukocytes and 3 in buccal cells only. All mutations shown to have arisen de novo when parent blood samples were available. The present series confirms the difficulty in predicting the phenotype according to the NIPBL mutation. Until now, somatic mosaicism has been observed for 20 cases which do not seem to be consistently associated with a milder phenotype. Besides, several reports support a postzygotic event for those cases. Considering these elements, we recommend a first-line buccal cell DNA analysis in order to improve gene testing sensitivity in Cornelia de Lange syndrome and genetic counselling.
Subject(s)
De Lange Syndrome/genetics , Face/abnormalities , Facial Asymmetry/genetics , Germ-Line Mutation , Mutation , Proteins/genetics , Cell Cycle Proteins , De Lange Syndrome/diagnosis , Facial Asymmetry/diagnosis , Facies , Female , Humans , Leukocytes/metabolism , Male , Mouth Mucosa/metabolism , Phenotype , Sequence Analysis, DNA/methodsABSTRACT
Cornelia de Lange syndrome (CdLS) is a clinically heterogeneous disorder characterized by typical facial dysmorphism, cognitive impairment and multiple congenital anomalies. Approximately 75% of patients carry a variant in one of the five cohesin-related genes NIPBL, SMC1A, SMC3, RAD21 and HDAC8. Herein we report on the clinical and molecular characterization of 11 patients carrying 10 distinct variants in HDAC8. Given the high number of variants identified so far, we advise sequencing of HDAC8 as an indispensable part of the routine molecular diagnostic for patients with CdLS or CdLS-overlapping features. The phenotype of our patients is very broad, whereas males tend to be more severely affected than females, who instead often present with less canonical CdLS features. The extensive clinical variability observed in the heterozygous females might be at least partially associated with a completely skewed X-inactivation, observed in seven out of eight female patients. Our cohort also includes two affected siblings whose unaffected mother was found to be mosaic for the causative mutation inherited to both affected children. This further supports the urgent need for an integration of highly sensitive sequencing technology to allow an appropriate molecular diagnostic, genetic counseling and risk prediction.
Subject(s)
De Lange Syndrome/genetics , Face/abnormalities , Facial Asymmetry/genetics , Histone Deacetylases/genetics , Mutation , Repressor Proteins/genetics , Amino Acid Sequence , Base Sequence , Child , De Lange Syndrome/pathology , Facial Asymmetry/pathology , Facies , Female , Genetic Counseling , Genotype , Humans , Male , Phenotype , Risk Factors , Sequence Analysis, DNA/methods , Sequence Homology, Amino Acid , Severity of Illness Index , X Chromosome InactivationABSTRACT
FBXL4 deficiency is a recently described disorder of mitochondrial maintenance associated with a loss of mitochondrial DNA in cells. To date, the genetic diagnosis of FBXL4 deficiency has been established in 28 individuals. This paper retrospectively reviews proxy-reported clinical and biochemical findings and evaluates brain imaging, morphological and genetic data in 21 of those patients. Neonatal/early-onset severe lactic acidosis, muscular hypotonia, feeding problems and failure to thrive is the characteristic pattern at first presentation. Facial dysmorphic features are present in 67% of cases. Seven children died (mean age 37 months); 11 children were alive (mean age at follow-up 46 months), three children were lost to follow-up. All survivors developed severe psychomotor retardation. Brain imaging was non-specific in neonates but a later-onset, rapidly progressive brain atrophy was noted. Elevated blood lactate and metabolic acidosis were observed in all individuals; creatine kinase was elevated in 45% of measurements. Diagnostic workup in patient tissues and cells revealed a severe combined respiratory chain defect with a general decrease of enzymes associated with mitochondrial energy metabolism and a relative depletion of mitochondrial DNA content. Mutations were detected throughout the FBXL4 gene albeit with no clear delineation of a genotype-phenotype correlation. Treatment with "mitochondrial medications" did not prove effective. In conclusion, a clinical pattern of early-onset encephalopathy, persistent lactic acidosis, profound muscular hypotonia and typical facial dysmorphism should prompt initiation of molecular genetic analysis of FBXL4. Establishment of the diagnosis permits genetic counselling, prevents patients undergoing unhelpful diagnostic procedures and allows for accurate prognosis.
Subject(s)
F-Box Proteins/genetics , Mitochondrial Diseases/diagnosis , Mitochondrial Diseases/genetics , Mitochondrial Diseases/pathology , Mutation , Ubiquitin-Protein Ligases/genetics , Acidosis, Lactic/complications , Acidosis, Lactic/congenital , Acidosis, Lactic/genetics , Child , Child, Preschool , Disease Progression , Facial Asymmetry/complications , Facial Asymmetry/congenital , Facial Asymmetry/genetics , Family , Female , Genetic Association Studies , Humans , Infant , Infant, Newborn , Male , Mitochondrial Diseases/mortality , Muscle Hypotonia/complications , Muscle Hypotonia/congenital , Muscle Hypotonia/genetics , Neuroimaging , Prognosis , Retrospective StudiesABSTRACT
Fluctuating and directional asymmetry are aspects of morphological variation widely used to infer environmental and genetic factors affecting facial phenotypes. However, the genetic basis and environmental determinants of both asymmetry types is far from being completely known. The analysis of facial asymmetries in admixed individuals can be of help to characterize the impact of a genome's heterozygosity on the developmental basis of both fluctuating and directional asymmetries. Here we characterize the association between genetic ancestry and individual asymmetry on a sample of Latin-American admixed populations. To do so, three-dimensional (3D) facial shape attributes were explored on a sample of 4,104 volunteers aged between 18 and 85 years. Individual ancestry and heterozygosity was estimated using more than 730,000 genome-wide markers. Multivariate techniques applied to geometric morphometric data were used to evaluate the magnitude and significance of directional and fluctuating asymmetry (FA), as well as correlations and multiple regressions aimed to estimate the relationship between facial FA scores and heterozygosity and a set of covariates. Results indicate that directional and FA are both significant, the former being the strongest expression of asymmetry in this sample. In addition, our analyses suggest that there are some specific patterns of facial asymmetries characterizing the different ancestry groups. Finally, we find that more heterozygous individuals exhibit lower levels of asymmetry. Our results highlight the importance of including ancestry-admixture estimators, especially when the analyses are aimed to compare levels of asymmetries on groups differing on socioeconomic levels, as a proxy to estimate developmental noise.
Subject(s)
Facial Asymmetry/genetics , Hispanic or Latino/genetics , Adolescent , Adult , Aged , Aged, 80 and over , Analysis of Variance , Anthropometry , Face/anatomy & histology , Face/pathology , Humans , Middle Aged , Principal Component Analysis , Young AdultABSTRACT
Velo-Cardio-Facial syndrome (VCFS), also called 22q11.2 microdeletion syndrome, is a rare pathology. The syndrome is caused by 22q11.2 deletion, recognized as one of the most frequent pathogenic human microdeletions. The scope and severity of the phenotypic expression of 22q11.2 microdeletion is characterised by high variability, although cleft palate and congenital conotruncal malformations are among the clinical features often associated with that syndrome. In the presented case of a boy patient with submucous cleft palate and congenital cardiac defect, 22q11.2 microdeletion was identified at the age of 13 months. In the presented paper particular emphasis was placed on the issue of dental and orthodontic care in patients with changes in the oral cavity and the craniofacial area, as well as on the possibilities of treatment and prophylaxis. The necessity to perform a thorough examination of the oral cavity in infants was also underlined as a vital element of clinical assessment, in particular in the case of co-occurring structural defects of internal organs.
Subject(s)
Abnormalities, Multiple/diagnosis , Chromosome Deletion , Chromosomes, Human, Pair 22 , Cleft Palate/diagnosis , Facial Asymmetry/diagnosis , Malocclusion/diagnosis , Abnormalities, Multiple/genetics , Child , Cleft Palate/genetics , Facial Asymmetry/genetics , Humans , Male , Malocclusion/genetics , Phenotype , SyndromeABSTRACT
Family relatives of children with nonsyndromic cleft lip with or without cleft palate (NSCL/P) who presumably carry a genetic risk yet do not manifest overt oral clefts, often present with distinct facial morphology of unknown genetic etiology. This study investigates distinct facial morphology among unaffected relatives and examines whether candidate genes previously associated with overt NSCL/P and left-right body patterning are correlated with such facial morphology. Cases were unaffected relatives of individuals with NSCL/P (n = 188) and controls (n = 194) were individuals without family history of NSCL/P. Cases and controls were genotyped for 20 SNPs across 13 candidate genes for NSCL/P (PAX7, ABCA4-ARHGAP29, IRF6, MSX1, PITX2, 8q24, FOXE1, TGFB3 and MAFB) and left-right body patterning (LEFTY1, LEFTY2, ISL1 and SNAI1). Facial shape and asymmetry phenotypes were obtained via principal component analyses and Procrustes analysis of variance from 32 coordinate landmarks, digitized on 3D facial images. Case-control comparisons of phenotypes obtained were performed via multivariate regression adjusting for age and gender. Phenotypes that differed significantly (P < 0.05) between cases and controls were regressed on the SNPs one at a time. Cases had significantly (P < 0.05) more profile concavity with upper face retrusion, upturned noses with obtuse nasolabial angles, more protrusive chins, increased lower facial heights, thinner and more retrusive lips and more protrusive foreheads. Furthermore, cases showed significantly more directional asymmetry compared to controls. Several of these phenotypes were significantly associated with genetic variants (P < 0.05). Facial height and width were associated with SNAI1. Midface antero-posterior (AP) projection was associated with LEFTY1. The AP position of the chin was related to SNAI1, IRF6, MSX1 and MAFB. The AP position of the forehead and the width of the mouth were associated with ABCA4-ARHGAP29 and MAFB. Lastly, facial asymmetry was related to LEFTY1, LEFTY2 and SNAI1. This study demonstrates that, genes underlying lip and palate formation and left-right patterning also contribute to facial features characteristic of the NSCL/P spectrum.
Subject(s)
Brain/abnormalities , Cleft Lip/genetics , Cleft Palate/genetics , Facial Asymmetry/genetics , Family , Genetic Association Studies , Adolescent , Adult , Case-Control Studies , Child , Child, Preschool , Face , Female , Humans , Male , Middle Aged , Polymorphism, Single Nucleotide , Principal Component Analysis , Young AdultABSTRACT
PURPOSE: Facial asymmetry is a common comorbid condition in patients with jaw deformation malocclusion. Heritability of malocclusion is advancing rapidly, but very little is known regarding genetic contributions to asymmetry. This study identifies differences in expression of key asymmetry-producing genes that are down-regulated in patients with facial asymmetry. METHODS: Masseter muscle samples were collected during bilateral sagittal split osteotomy orthognathic surgery to correct skeletal-based malocclusion. Patients were classified as class II or III and open or deep bite malocclusion with or without facial asymmetry. Muscle samples were analyzed for gene expression differences on Affymetrix HT2.0 microarray global expression chips. RESULTS: Overall gene expression was different for asymmetric patients compared with other malocclusion classifications by principal component analysis (P < 0.05). We identified differences in the nodal signaling pathway, which promotes development of mesoderm and endoderm and left-right patterning during embryogenesis. Nodal and Lefty expression was 1.39- to 1.84-fold greater (P < 3.41 × 10), whereas integral membrane Nodal modulators Nomo1,2,3 were -5.63 to -5.81 (P < 3.05 × 10) less in asymmetry subjects. Fold differences among intracellular pathway members were negative in the range of -7.02 to -2.47 (P < 0.003). Finally Pitx2, an upstream effector of Nodal known to influence the size of type II skeletal muscle fibers was also significantly decreased in facial asymmetry (P < 0.05). CONCLUSIONS: When facial asymmetry is part of skeletal malocclusion, there are decreases in nodal signaling pathway genes in masseter muscle. This data suggest that the nodal signaling pathway is down-regulated to help promote development of asymmetry. Pitx2 expression differences also contributed to both skeletal and muscle development in this condition.
Subject(s)
Down-Regulation/genetics , Facial Asymmetry/genetics , Nodal Protein/genetics , Signal Transduction/genetics , Adult , Facial Asymmetry/pathology , Female , Homeodomain Proteins/genetics , Humans , Intracellular Signaling Peptides and Proteins/genetics , Left-Right Determination Factors/genetics , Male , Malocclusion/genetics , Malocclusion/pathology , Masseter Muscle/metabolism , Masseter Muscle/pathology , Membrane Proteins/genetics , Transcription Factors/genetics , Homeobox Protein PITX2ABSTRACT
Craniofacial microsomia (CFM) is a complex condition associated with microtia, mandibular hypoplasia, and preauricular tags. It is the second most common congenital facial condition treated in many craniofacial centers and requires longitudinal multidisciplinary patient care. The purpose of this article is to summarize current recommendations for clinical management and discuss opportunities to advance clinical research in CFM.
Subject(s)
Congenital Abnormalities/therapy , Ear/abnormalities , Facial Asymmetry/therapy , Goldenhar Syndrome/therapy , Congenital Abnormalities/genetics , Congenital Abnormalities/pathology , Congenital Microtia , Ear/pathology , Facial Asymmetry/genetics , Facial Asymmetry/pathology , Goldenhar Syndrome/genetics , Goldenhar Syndrome/pathology , HumansABSTRACT
CHARGE (coloboma of the eye, heart defects, choanal atresia, retarded growth and development, genital hypoplasia and ear anomalies and/or hearing loss) syndrome is a rare genetic, multiple-malformation syndrome. About 80% of patients with a clinical diagnose, have a mutation or a deletion in the gene encoding chromodomain helicase DNA-binding protein 7 (CHD7). Genotype-phenotype correlation is only partly known. In this nationwide study, phenotypic characteristics of 18 Danish CHD7 mutation positive CHARGE individuals (N = 18) are presented. We studied patient records, clinical photographs, computed tomography, and magnetic resonance imaging (MRI). Information was not available for all traits in all subjects. Therefore, the results are presented as fractions. The following prevalence of cardinal symptoms were found: coloboma, 16/17; heart defects, 14/18; choanal atresia, 7/17; retarded growth and development, 11/13; genital abnormalities, 5/18; ear anomalies, 15/17 and sensorineural hearing loss, 14/15. Vestibular dysfunction (10/13) and swallowing problems (12/15) were other frequent cranial nerve dysfunctions. Three-dimensional reconstructions of MRI scans showed temporal bone abnormalities in >85%. CHARGE syndrome present a broad phenotypic spectrum, although some clinical features are more frequently occurring than others. Here, we suggest that genetic testing for CHD7 mutation should be considered in neonates with a specific combination of several clinical symptoms.
Subject(s)
CHARGE Syndrome/pathology , DNA Helicases/genetics , DNA-Binding Proteins/genetics , Genetic Association Studies , Adolescent , Bone Diseases, Developmental/genetics , Bone Diseases, Developmental/pathology , CHARGE Syndrome/genetics , Child , Child, Preschool , Coloboma/genetics , Coloboma/pathology , Denmark/epidemiology , Developmental Disabilities/genetics , Developmental Disabilities/pathology , Ear, External/abnormalities , Ear, External/pathology , Facial Asymmetry/genetics , Facial Asymmetry/pathology , Female , Hearing Loss, Sensorineural/genetics , Hearing Loss, Sensorineural/pathology , Heart Defects, Congenital/genetics , Heart Defects, Congenital/pathology , Humans , Infant , Male , Mouth Abnormalities/genetics , Mouth Abnormalities/pathology , Mutation , Retrospective Studies , Urogenital Abnormalities/genetics , Urogenital Abnormalities/pathologyABSTRACT
This study explored the role of TCOF1 insertion mutations in Taiwanese patients with craniofacial anomalies. Twelve patients with single or multiple, asymmetrical congenital craniofacial anomalies were enrolled. Genomic DNA was prepared from leukocytes; the coding regions of TCOF1 were analyzed by polymerase chain reaction and direct sequencing. Clinical manifestations were correlated to the TCOF1 mutation. Six of 12 patients diagnosed with hemifacial microsomia exhibited a novel insertion mutation 4127 ins G (frameshift) in exon 24 in the TCOF1 gene. All six patients were diagnosed with anomalies on the left side. In addition, four of these six patients had hearing impairment; three had other major anomalies; and two had developmental delay. The insertion caused a frameshift, an early truncation, the loss of two putative nuclear localization signals (residues 1404-1420 and 1424-1440), and the loss of coiled coil domain (1406-1426) in treacle protein. These findings support the existence of two regulators of growth of the mandibular condyles.
Subject(s)
Facial Asymmetry/genetics , Mutagenesis, Insertional , Nuclear Proteins/genetics , Phosphoproteins/genetics , Adult , Child , Child, Preschool , Craniofacial Abnormalities/genetics , Craniofacial Abnormalities/pathology , Exons , Female , Frameshift Mutation , Genome, Human/genetics , Humans , Infant , Infant, Newborn , Male , Nuclear Localization Signals/genetics , Nuclear Proteins/metabolism , Phenotype , Phosphoproteins/metabolism , Polymorphism, Single Nucleotide , Sequence Analysis, DNA , TaiwanABSTRACT
Transient knock-down of the gap junction protein Cx43 by antisense and siRNA, or gap junction block with mimetic peptides, have been shown to enhance epidermal wound healing. However, patients with oculodentodigital dysplasia (ODDD) express mutant Cx43 that leads to a chronic reduction in gap junctional intercellular communication. To determine whether mutant Cx43 in keratinocytes would impact upon the wound healing process, we localized Cx43 in human and mouse skin tissue expressing mutant Cx43 and assessed the ability of primary keratinocytes derived from a mouse model of ODDD to proliferate, migrate and differentiate. In the epidermis from an ODDD patient and in the epidermis of mice expressing the G60S mutant or in keratinocytes obtained from mutant mice, Cx43 was frequently found within intracellular compartments and rarely localized to punctate sites of cell-cell apposition. Primary keratinocytes derived from G60S mutant mice proliferated faster but migrated similarly to keratinocytes derived from wild-type control mice. Keratinocytes derived from mutant mice expressed abundant Cx43 and higher levels of involucrin and loricrin under low calcium conditions. However, after calcium-induced differentiation, similar levels of Cx43, involucrin and loricrin were observed. Thus, we conclude that during wound healing, mutant Cx43 may enhance keratinocyte proliferation and promote early differentiation of keratinocytes.
Subject(s)
Cell Differentiation , Cell Proliferation , Connexin 43/genetics , Connexin 43/metabolism , Dental Enamel Hypoplasia/genetics , Facial Asymmetry/genetics , Keratinocytes/metabolism , Keratinocytes/pathology , Microphthalmos/genetics , Mutation/genetics , Syndactyly/genetics , Abnormalities, Multiple/genetics , Abnormalities, Multiple/metabolism , Abnormalities, Multiple/pathology , Animals , Biopsy , Calcium/pharmacology , Cell Differentiation/drug effects , Cell Movement/drug effects , Cell Proliferation/drug effects , Cells, Cultured , Dental Enamel Hypoplasia/metabolism , Dental Enamel Hypoplasia/pathology , Disease Models, Animal , Face/abnormalities , Face/pathology , Facial Asymmetry/metabolism , Facial Asymmetry/pathology , Humans , Intercellular Junctions/metabolism , Intercellular Junctions/pathology , Membrane Proteins/metabolism , Mice , Mice, Mutant Strains , Microphthalmos/metabolism , Microphthalmos/pathology , Protein Precursors/metabolism , Skin/pathology , Syndactyly/metabolism , Syndactyly/pathology , Wound Healing/physiologyABSTRACT
Oculoauriculovertebral spectrum or Goldenhar syndrome is a phenotypically and probably genetically heterogeneous disorder characterized by hemifacial microsomia (unilateral ear abnormalities and ipsilateral mandibular hypoplasia) as well as vertebral anomalies and epibulbar dermoid/lipodermoids. Although most cases of the Goldenhar syndrome are sporadic, both autosomal recessive and dominant inheritance have been reported so far. In this report, we describe the clinical aspects of two familial cases with evidence of autosomal dominant inheritance and a non-familial case, and compare them with the reports in the literature. One of our familial cases was a ten day old female infant of a mother with left hemifacial microsomia. She had multiple bilateral preauricular tags and a "fleshy masse" on her right cheek. The other familial case was a two months old male infant whose father had hemifacial asymmetry. He had unilateral microtia, and abnormal antihelix, a skin tag in the contralateral ear associated with bilateral sensorineural hearing loss. The third case was a sporadic case who was 2 years old boy with preauricular skin tag, right hemifacial microsomia and limbal dermoid at the temporal limbus of the right eye. As there were no other associated defects, the cases we presented here were thought to be mild variations of the Goldenhar spectrum. The most commonly encountered mutations of thrombophilia genes were studied. We believe that the interfamilial and intrafamilial clinical variabilities observed in these cases reinforce the necessity of a careful examination for the whole family with regards to the stigmata of Goldenhar syndrome.
Subject(s)
Facial Asymmetry/genetics , Factor V/genetics , Goldenhar Syndrome/genetics , Methylenetetrahydrofolate Reductase (NADPH2)/genetics , Prothrombin/genetics , Female , Humans , Infant , Infant, Newborn , Male , Mutation , Severity of Illness IndexABSTRACT
For decades the relationships of twinning and alterations in body patterning, such as laterality and asymmetry, have been investigated. However, the tools to define and quantify these relationships have been limited and the majority of these studies have relied on associations with subjectively defined phenotypes. The emerging technologies of 3-dimensional (3D) facial scanning and geometric morphometrics are providing the means to establish objective criteria, including measures of asymmetry, which can be used for phenotypic classification and investigations. Additionally, advances in molecular epigenetics provide new opportunities for novel investigations of mechanisms central to early developmental processes, twinning and related phenotypes. We review the evidence for overlapping etiologies of twinning, asymmetry and selected monogenic and complex diseases, and we suggest that the combination of epigenetic investigations with detailed and objective phenotyping, utilizing 3D facial analysis tools, can reveal insights into the genesis of these phenomena.