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4. CDK10 Mutations in Humans and Mice Cause Severe Growth Retardation, Spine Malformations, and Developmental Delays

Author

Windpassinger, Christian, Piard, Juliette, Bonnard, Carine, Alfadhel, Majid, Lim, Shuhui, Bisteau, Xavier, Blouin, Stéphane, Ali, Nur’Ain B., Ng, Alvin Yu Jin, Lu, Hao, Tohari, Sumanty, Talib, S. Zakiah A., van Hul, Noémi, Caldez, Matias J., Van Maldergem, Lionel, Yigit, Gökhan, Kayserili, Hülya, Youssef, Sameh A., Coppola, Vincenzo, de Bruin, Alain, Tessarollo, Lino, Choi, Hyungwon, Rupp, Verena, Roetzer, Katharina, Roschger, Paul, Klaushofer, Klaus, Altmüller, Janine, Roy, Sudipto, Venkatesh, Byrappa, Ganger, Rudolf, Grill, Franz, Ben Chehida, Farid, Wollnik, Bernd, Altunoglu, Umut, Al Kaissi, Ali, Reversade, Bruno, and Kaldis, Philipp

Published
2017
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9. Ischiopubic and odontoid synchondrosis in a boy with progressive pseudorheumatoid chondrodysplasia

Author

Ben Ghachem Maher, Ben Chehida Farid, Al Kaissi Ali, Grill Franz, and Klaushofer Klaus

Subjects
Pediatrics, RJ1-570, Diseases of the musculoskeletal system, RC925-935
Abstract

Abstract Purpose To present the case of a 14-year-old boy with clinical and radiographic features of pseudorheumatoid chondrodyspalsia with additional, potentially serious, cervical malformations. Methods Detailed clinical and radiological examinations were undertaken with emphasis on the usefulness of 3D-CT scanning. Results There was synchondrosis between the odontoid and the body of the axis and the cephalad part of the odontoid was detached. Bilateral ischiopubic ossification defects and ischiopubic and odontoid synchondroses were additional abnormalities. 3D-CT scan showed an orthotopic type of os odontoideum associated with an occult axial fracture. Conclusion Children who are younger than seven years of age are predisposed to develop odontoid fracture. The latter occur because of the presence of physiological odontoid synchondrosis, but fractures can result from trivial injuries as well as from high-energy trauma. The persistence of an infantile odontoid, with a large pre-adulthood head in children with skeletal dysplasias, is a major risk factor for sudden death or significant morbidity. Comprehensive orthopaedic management must follow early identification of these malformations.

Published
2007
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12. CDK10 Mutations in Humans and Mice Cause Severe Growth Retardation, Spine Malformations, and Developmental Delays

Author

Regenerative Medicine, Stem Cells & Cancer, Windpassinger, Christian, Piard, Juliette, Bonnard, Carine, Alfadhel, Majid, Lim, Shuhui, Bisteau, Xavier, Blouin, Stéphane, Ali, Nur'Ain B, Ng, Alvin Yu Jin, Lu, Hao, Tohari, Sumanty, Talib, S Zakiah A, van Hul, Noémi, Caldez, Matias J, Van Maldergem, Lionel, Yigit, Gökhan, Kayserili, Hülya, Youssef, Sameh A, Coppola, Vincenzo, de Bruin, Alain, Tessarollo, Lino, Choi, Hyungwon, Rupp, Verena, Roetzer, Katharina, Roschger, Paul, Klaushofer, Klaus, Altmüller, Janine, Roy, Sudipto, Venkatesh, Byrappa, Ganger, Rudolf, Grill, Franz, Ben Chehida, Farid, Wollnik, Bernd, Altunoglu, Umut, Al Kaissi, Ali, Reversade, Bruno, Kaldis, Philipp, Regenerative Medicine, Stem Cells & Cancer, Windpassinger, Christian, Piard, Juliette, Bonnard, Carine, Alfadhel, Majid, Lim, Shuhui, Bisteau, Xavier, Blouin, Stéphane, Ali, Nur'Ain B, Ng, Alvin Yu Jin, Lu, Hao, Tohari, Sumanty, Talib, S Zakiah A, van Hul, Noémi, Caldez, Matias J, Van Maldergem, Lionel, Yigit, Gökhan, Kayserili, Hülya, Youssef, Sameh A, Coppola, Vincenzo, de Bruin, Alain, Tessarollo, Lino, Choi, Hyungwon, Rupp, Verena, Roetzer, Katharina, Roschger, Paul, Klaushofer, Klaus, Altmüller, Janine, Roy, Sudipto, Venkatesh, Byrappa, Ganger, Rudolf, Grill, Franz, Ben Chehida, Farid, Wollnik, Bernd, Altunoglu, Umut, Al Kaissi, Ali, Reversade, Bruno, and Kaldis, Philipp

Published
2017

13. CDK10 mutations in humans and mice cause severe growth retardation, spine malformations, and developmental delays

Author

Karabey, Hülya Kayserili; Wollnik, Bernd; Kaldis, Philipp, Windpassinger, Christian; Piard, Juliette; Bonnard, Carine; Alfadhel, Majid; Lim, Shuhui; Bisteau, Xavier; Blouin, Stéphane; Ali, Nur'Ain B.; Ng, Alvin Yu Jin; Lu, Hao; Tohari, Sumanty; Talib, S. Zakiah A.; van Hul, Noémi; Caldez, Matias J.; Van Maldergem, Lionel; Yiğit, Gökhan; Youssef, Sameh A.; Coppola, Vincenzo; de Bruin, Alain; Tessarollo, Lino; Choi, Hyungwon; Rupp, Verena; Roetzer, Katharina; Roschger, Paul; Klaushofer, Klaus; Altmüller, Janine; Roy, Sudipto; Venkatesh, Byrappa; Ganger, Rudolf; Grill, Franz; Ben Chehida, Farid; Altunoglu, Umut; Al Kaissi, Ali; Reversade, Bruno, School of Medicine, Department of Medical Genetics, Karabey, Hülya Kayserili; Wollnik, Bernd; Kaldis, Philipp, Windpassinger, Christian; Piard, Juliette; Bonnard, Carine; Alfadhel, Majid; Lim, Shuhui; Bisteau, Xavier; Blouin, Stéphane; Ali, Nur'Ain B.; Ng, Alvin Yu Jin; Lu, Hao; Tohari, Sumanty; Talib, S. Zakiah A.; van Hul, Noémi; Caldez, Matias J.; Van Maldergem, Lionel; Yiğit, Gökhan; Youssef, Sameh A.; Coppola, Vincenzo; de Bruin, Alain; Tessarollo, Lino; Choi, Hyungwon; Rupp, Verena; Roetzer, Katharina; Roschger, Paul; Klaushofer, Klaus; Altmüller, Janine; Roy, Sudipto; Venkatesh, Byrappa; Ganger, Rudolf; Grill, Franz; Ben Chehida, Farid; Altunoglu, Umut; Al Kaissi, Ali; Reversade, Bruno, School of Medicine, and Department of Medical Genetics

Abstract

In five separate families, we identified nine individuals affected by a previously unidentified syndrome characterized by growth retardation, spine malformation, facial dysmorphisms, and developmental delays. Using homozygosity mapping, array CGH, and exome sequencing, we uncovered bi-allelic loss-of-function CDK10 mutations segregating with this disease. CDK10 is a protein kinase that partners with cyclin M to phosphorylate substrates such as ETS2 and PKN2 in order to modulate cellular growth. To validate and model the pathogenicity of these CDK10 germline mutations, we generated conditional-knockout mice. Homozygous Cdk10-knockout mice died postnatally with severe growth retardation, skeletal defects, and kidney and lung abnormalities, symptoms that partly resemble the disease's effect in humans. Fibroblasts derived from affected individuals and Cdk10-knockout mouse embryonic fibroblasts (MEFs) proliferated normally; however, Cdk10-knockout MEFs developed longer cilia. Comparative transcriptomic analysis of mutant and wild-type mouse organs revealed lipid metabolic changes consistent with growth impairment and altered ciliogenesis in the absence of CDK10. Our results document the CDK10 loss-of-function phenotype and point to a function for CDK10 in transducing signals received at the primary cilia to sustain embryonic and postnatal development., NIH, the National Cancer Institute; Center for Cancer Research; Strategic Positioning Fund for the Genetic Orphan Diseases program; Industry Alignment Fund for the Singapore Childhood Undiagnosed Diseases program from the A*STAR (Agency for Science, Technology, and Research) Biomedical Research Council; A*STAR Biomedical Research Council

Published
2017

19. Persistent torticollis, facial asymmetry, grooved tongue, and dolicho-odontoid process in connection with atlas malformation complex in three family subjects.

Author

Al Kaissi, Ali, Chehida, Farid Ben, Gharbi, Hassan, Ghachem, Maher Ben, Grill, Franz, Varga, Franz, Klaushofer, Klaus, Ben Chehida, Farid, and Ben Ghachem, Maher

Subjects
ATLAS (Vertebra), WOUNDS & injuries, CERVICAL vertebrae, TORTICOLLIS, DYSPLASIA, PARALYSIS, APNEA
Abstract

Congenital clefts and other malformations of the atlas are incidental findings identified while investigating the cervical spine following trauma. A persistent bifid anterior and posterior arch of the atlas beyond the age of 3-4 years is observed in skeletal dysplasias, Goldenhar syndrome, Conradi syndrome, and Down's syndrome. There is a high incidence of both anterior and posterior spina bifida of the atlas in patients with metabolic disorders, such as Morquio's syndrome [Baraitser and Winter in London dysmorphology database, Oxford University Press, 2005; Torriani, Lourenco in Rev Hosp Clin Fac Med Sao Paulo 53: 73-76, 2002]. We report two siblings and their mother, with congenital, persistent torticollis, plagiocephaly, facial asymmetry, grooved tongues, and asymptomatic "dolicho-odontoid process". All are of normal intelligence. No associated Neurological dysfunction, paresis, apnoea, or failures to thrive were encountered. Radiographs of the cervical spine were non-contributory, but 3D CT scanning of this area allowed further visualisation of the cervico-cranial malformation complex in this family and might possibly explain the sudden early juvenile mortality. Agenesis of the posterior arch of the atlas and bifidity/clefting of anterior arch of the atlas associated with asymptomatic "dolicho-odontoid process" were the hallmark in the proband and his female sibling. Some of the features were present in the mother. All the family subjects were investigated. To the best of our knowledge the constellation of malformation complex in this family has not been previously reported. [ABSTRACT FROM AUTHOR]

Published
2007
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20. CDK10 Mutations in Humans and Mice Cause Severe Growth Retardation, Spine Malformations, and Developmental Delays

Author

Sudipto Roy, Noémi van Hul, Janine Altmüller, Hyungwon Choi, Nur'Ain Binte Ali, Xavier Bisteau, Shuhui Lim, Christian Windpassinger, Stéphane Blouin, Verena Rupp, Carine Bonnard, Franz Grill, Byrappa Venkatesh, Bruno Reversade, Rudolf Ganger, Vincenzo Coppola, S. Zakiah A. Talib, Klaus Klaushofer, Majid Alfadhel, Gökhan Yigit, Farid Ben Chehida, Paul Roschger, Ali Al Kaissi, Matias J. Caldez, Umut Altunoglu, Bernd Wollnik, Hülya Kayserili, Lionel Van Maldergem, Alvin Yu Jin Ng, Sameh A. Youssef, Lino Tessarollo, Katharina M. Roetzer, Hao Lu, Philipp Kaldis, Juliette Piard, Alain de Bruin, Sumanty Tohari, Karabey, Hülya Kayserili, Wollnik, Bernd, Kaldis, Philipp, Windpassinger, Christian, Piard, Juliette, Bonnard, Carine, Alfadhel, Majid, Lim, Shuhui, Bisteau, Xavier, Blouin, Stéphane, Ali, Nur'Ain B., Ng, Alvin Yu Jin, Lu, Hao, Tohari, Sumanty, Talib, S. Zakiah A., van Hul, Noémi, Caldez, Matias J., Van Maldergem, Lionel, Yiğit, Gökhan, Youssef, Sameh A., Coppola, Vincenzo, de Bruin, Alain, Tessarollo, Lino, Choi, Hyungwon, Rupp, Verena, Roetzer, Katharina, Roschger, Paul, Klaushofer, Klaus, Altmüller, Janine, Roy, Sudipto, Venkatesh, Byrappa, Ganger, Rudolf, Grill, Franz, Ben Chehida, Farid, Altunoglu, Umut, Al Kaissi, Ali, Reversade, Bruno, School of Medicine, Department of Medical Genetics, Regenerative Medicine, Stem Cells & Cancer, Amsterdam Cardiovascular Sciences, Amsterdam Reproduction & Development (AR&D), Center for Reproductive Medicine, ACS - Heart failure & arrhythmias, and ACS - Diabetes & metabolism

Subjects
0301 basic medicine, Male, Developmental Disabilities, medicine.disease_cause, Mice, 0302 clinical medicine, Phosphorylation, Child, Genetics (clinical), Exome sequencing, Cells, Cultured, Growth Disorders, Mice, Knockout, Mutation, Cultured, Cilium, Cell Cycle, Disease gene identification, Phenotype, Cyclin-Dependent Kinases, Pedigree, Embryo, 030220 oncology & carcinogenesis, Child, Preschool, Female, Signal Transduction, medicine.medical_specialty, Cells, Knockout, Biology, Article, 03 medical and health sciences, Germline mutation, Internal medicine, Ciliogenesis, Journal Article, Genetics, medicine, Animals, Humans, Star syndrome, Genome browser, Protein-kinase, Cdk10/Cyclin M, Family, Gene, Pisslre, DNA, Melanoma, Member, Cilia, Preschool, Cell Proliferation, Medicine, Genetics and heredity, Mammalian, Infant, Fibroblasts, medicine.disease, Embryo, Mammalian, Spine, 030104 developmental biology, Endocrinology, Congenital disorder, Al Kaissi syndrome knockout mice, CDK10, ETS2, cilia, congenital disorder, growth retardation, metabolism, spine malformation
Abstract

In five separate families, we identified nine individuals affected by a previously unidentified syndrome characterized by growth retardation, spine malformation, facial dysmorphisms, and developmental delays. Using homozygosity mapping, array CGH, and exome sequencing, we uncovered bi-allelic loss-of-function CDK10 mutations segregating with this disease. CDK10 is a protein kinase that partners with cyclin M to phosphorylate substrates such as ETS2 and PKN2 in order to modulate cellular growth. To validate and model the pathogenicity of these CDK10 germline mutations, we generated conditional-knockout mice. Homozygous Cdk10-knockout mice died postnatally with severe growth retardation, skeletal defects, and kidney and lung abnormalities, symptoms that partly resemble the disease's effect in humans. Fibroblasts derived from affected individuals and Cdk10-knockout mouse embryonic fibroblasts (MEFs) proliferated normally; however, Cdk10-knockout MEFs developed longer cilia. Comparative transcriptomic analysis of mutant and wild-type mouse organs revealed lipid metabolic changes consistent with growth impairment and altered ciliogenesis in the absence of CDK10. Our results document the CDK10 loss-of-function phenotype and point to a function for CDK10 in transducing signals received at the primary cilia to sustain embryonic and postnatal development., NIH, the National Cancer Institute; Center for Cancer Research; Strategic Positioning Fund for the Genetic Orphan Diseases program; Industry Alignment Fund for the Singapore Childhood Undiagnosed Diseases program from the A*STAR (Agency for Science, Technology, and Research) Biomedical Research Council; A*STAR Biomedical Research Council

Published
2017
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21. Broad spectrum of skeletal malformation complex in patients with cleidocranial dysplasia syndrome: radiographic and tomographic study.

Author

Al Kaissi A, Ben Chehida F, Kenis V, Ganger R, Radler C, Hofstaetter JG, Klaushofer K, and Grill F

Abstract

Purpose: Cleidocranial dysplasia is an autosomal dominant disorder characterized by defective ossification of the intramembraneous ossification (primarily the clavicles, cranium, and pelvis), and it is caused by mutations in the RUNX2 gene that is responsible for osteoblast differentiation. Spine deformities were of progressive nature and considered to be the major orthopedic abnormalities encountered in our practice in patients with cleidocranial dysplasia. We aimed to further delineate the underlying spine pathology and its etiological understanding. Extraspinal deformities were dealt with respectively., Material and Methods: In this paper, we describe 7 patients who were consistent with the phenotypic and the genotypic characterization of cleidocranial dysplasia. Reformatted computed tomography (CT) scans have been applied in several instances to further understand the underlying pathology of progressive spine tilting. Radiographs were sufficient to illustrate other skeletal malformations., Results: Anatomical survey demonstrates that a broad spectrum of frequently unrecognized orthopedic aberrations were encountered. We believe that torticollis has evolved in connection with the persistence of synchondrosis of the skull base and the upper cervical spine and these are strongly correlated to the well-known pathology of posterior occipital synchondrosis. Similarly, scoliosis and kyphoscoliosis resulted from the pathologic aberration of the cartilaginous stage of disrupted embryological development. All our results are discussed for the first time. Coxa vara, patellar dysplasia, and genu valgum were observed as extraspinal deformities., Conclusion: This paper includes for the first time the anatomical analysis of the malformation complex of the craniocervical and the entire spine in patients with cleidocranial dysplasia. Reformatted CT scan was the modality of choice. We were able to illustrate that the persistence of skull base and the cervical spine synchondrosis were correlated with the pathological mechanism of the posterior occipital synchondrosis. Therefore, injuries to the craniocervical region in these patients might lead to a wide range of dreadful complications, ranging from complete atlanto-occipital or atlanto-axial dislocation to nondisplaced occipital condyle avulsion fractures with the possibility of morbid and or mortal outcome. On the other hand, the persistence of a cartilaginous spine was the reason behind the progressive spine tilting. This pathological form can be considered as a notoriously unpredictable malformation complex. The value of presenting these patients is to demonsterate that the genotype is not a precise index to assess the severity and the natural history of the phenotype.

Published
2013
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22. Dysmorphic facies and diffuse posterior spine ankylosis in a patient with unusual form of spondyloenchondrodysplasia (Spranger type IV).

Author

Al Kaissi A, Ben Chehida F, Ben Ghachem M, Klaushofer K, and Grill F

Subjects
Adolescent, Age of Onset, Ankylosis etiology, Ankylosis pathology, Autoimmune Diseases complications, Child, Facies, Humans, Male, Osteochondrodysplasias complications, Radiography, Spinal Diseases etiology, Spine pathology, Ankylosis diagnostic imaging, Autoimmune Diseases diagnostic imaging, Autoimmune Diseases pathology, Osteochondrodysplasias diagnostic imaging, Osteochondrodysplasias pathology, Spinal Diseases diagnostic imaging, Spinal Diseases pathology
Abstract

We describe a male patient, who was seen for the first time at the age of 8 years because of short trunk dwarfism. Spine radiographs showed platyspondyly with irregular areas of increased and decreased mineralization (irregular spotted appearance within lytic lesions located along the posterior vertebral bodies of the entire spine). Skeletal survey showed no enchondromatous lesions of the short/long tubular bones. At the age of 17, progressive spine stiffness associated with stooping posture developed. 3DCT scanning showed pathological transformation of the spinal enchondromas into generalized ossification and thickening of the posterior vertebral elements (vertebral laminae, supraspinal, and interspinal ligaments, respectively) causing effectively the development of a diffuse posterior spinal ankylosis. We report what might be a unique subtype of spondyloenchondrodysplasia (Spranger type IV).

Published
2013
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23. Diffuse skull base/cervical fusion syndromes in two siblings with spondylocostal dysostosis syndrome: analysis via three dimensional computed tomography scanning.

Author

Al Kaissi A, Ben Chehida F, Ben Ghachem M, Klaushofer K, and Grill F

Subjects
Adolescent, Cervical Vertebrae abnormalities, Child, Preschool, Humans, Male, Siblings, Skull Base abnormalities, Syndrome, Abnormalities, Multiple diagnostic imaging, Ankylosis diagnostic imaging, Cervical Vertebrae diagnostic imaging, Dysostoses diagnostic imaging, Imaging, Three-Dimensional, Radiographic Image Interpretation, Computer-Assisted, Skull Base diagnostic imaging, Tomography, X-Ray Computed
Abstract

Study Design: A study on a pair of male sibs to reach for the etiological understanding of unusual skull base/spine maldevelopment., Objective: Previously, radiographs alone were used to formulate this diagnosis. Here, three-dimensional computed tomography (3D CT) studies further clarified the typical diagnostic findings associated with spondylocostal dysostosis (SCD). Interestingly, patients with SCD are at increased risk for diffuse skull base/cervical fusion syndromes and can result in severe neurologic deficits associated with any degree of trauma., Summary of Background Data: Classically SCD is defined as a skeletal dysplasia with clinical and radiologic manifestations, consisting of short neck and trunk, nonprogressive scoliosis and abnormalities of vertebral segmentation and of the ribs. Radiograms have been adopted as the only modality for the classification and prognostication of patients with SCD., Methods: Detailed clinical and radiographic examinations were undertaken with emphasis on the significance of the 3D CT scanning., Results: We observed extensive fusion of the clivus with the cervical/entire spine, resulting in a remarkable solid, immobile, and fixed bony ankylosis of extremely serious outcome., Conclusion: Patients with spondylcostal dysostosis are predisposed to develop extensive skull-base-cervical spine fusion. The latter might lead to the development of a solid, immobile, and fixed bony ankylosis. In children/adults trivial injuries and/or high-energy trauma can lead to serious intracranial and spinal cord injury. Comprehensive orthopedic and neurosurgeons management must follow the recognition of these anomalies. To the best of our knowledge, no previous CT studies of the spine have been published in patients with SCD.

Published
2008
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24. Craniocervical junction malformation in a child with Oromandibular-limb hypogenesis-Möbius syndrome.

Author

Al Kaissi A, Grill F, Safi H, Ben Ghachem M, Ben Chehida F, and Klaushofer K

Subjects
Abnormalities, Multiple genetics, Abnormalities, Multiple physiopathology, Child Development, Child, Preschool, Craniofacial Abnormalities genetics, Craniofacial Abnormalities physiopathology, Humans, Infant, Infant, Newborn, Limb Deformities, Congenital genetics, Limb Deformities, Congenital physiopathology, Male, Mobius Syndrome genetics, Mobius Syndrome physiopathology, Phenotype, Abnormalities, Multiple diagnosis, Craniofacial Abnormalities diagnosis, Limb Deformities, Congenital diagnosis, Mobius Syndrome diagnosis
Abstract

We report a male child with Oromandibular-limb hypogenesis (OMLH), the main features being bilateral sixth and seventh nerve palsies, limb anomalies and hypoplasia of the tongue. Additional features were shortness of the neck associated with torticollis. Radiographs of the cervical spine were non-contributory, but 3D computed tomography (CT) scanning of this area identified: a) congenital hypoplasia of the atlas; b) the simultaneous development of occiput-atlas malformation/developmental defect. To our knowledge, this is the first clinical report assessing the cervico-cranium malformation in a child with OMLH-Möbius syndrome.

Published
2007
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25. Progressive congenital torticollis in VATER association syndrome.

Author

Al Kaissi A, Ben Chehida F, Safi H, Nassib N, Ben Ghachem M, Gharbi H, and Grill F

Subjects
Cervical Vertebrae diagnostic imaging, Child, Female, Humans, Image Processing, Computer-Assisted, Skull Base diagnostic imaging, Syndrome, Tomography, X-Ray Computed, Abnormalities, Multiple diagnosis, Anus, Imperforate complications, Cervical Vertebrae abnormalities, Radial Artery abnormalities, Skull Base abnormalities, Torticollis congenital, Torticollis etiology, Tracheoesophageal Fistula complications
Abstract

Study Design: A family study to reach the diagnosis of a multiple malformation syndrome., Objective: To determine the cause of torticollis, in a patient with the VATER association., Summary of Background Data: The VATER association is a combination of vertebral anomalies, anal stenosis, tracheo-esophageal fistula, and radial anomalies. It needs a multidisciplinary approach with a major input from orthopedic surgeons. Torticollis in this condition has not been reported before., Methods: Detailed family history and radiologic study using plain radiographs and three-dimensional-reconstruction., Results: Bony abnormalities at the base of the skull and upper cervical vertebrae were found., Conclusions: It is postulated that the bony abnormalities were the underlying cause of the neurologic problem.

Published
2006
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26. Craniovertebral malformation complex in a child with Weismann-Netter-Stuhl syndrome.

Author

Al Kaissi A, Ben Chehida F, Gharbi H, Jinziri M, Safi H, Ben Ghachem M, Grill F, Varga F, and Klaushofer K

Subjects
Abnormalities, Multiple etiology, Child, Preschool, Fibula abnormalities, Humans, Leg Length Inequality etiology, Male, Syndrome, Tomography, X-Ray Computed, Vitamin D Deficiency complications, Abnormalities, Multiple diagnostic imaging, Atlanto-Axial Joint abnormalities, Leg Length Inequality diagnostic imaging, Musculoskeletal Abnormalities diagnostic imaging, Skull abnormalities
Abstract

Objective: Bowing of the legs is usually thrown into the basket of vitamin D deficiency rickets; therefore, a significant number of affected children can be misdiagnosed and improperly managed. This case illustrates how the careful clinical and radiological assessment of such a case can lead to the adequate understanding of its etiology., Description: We report a sporadic case of a 2-year-old male child who presented with radiological features that were compatible with Weismann-Netter-Stuhl syndrome. In addition, we observed craniovertebral malformation complex. He was of normal intelligence. To our knowledge, the combination of Weismann-Netter-Stuhl syndrome and presence of a hypoplastic occipitalized atlas and further C2-C3 fusion has not been reported before. The diagnosis of Weismann-Netter-Stuhl is discussed. Classically, Weismann-Netter-Stuhl syndrome is characterized by short stature, mental retardation (in some individuals), dural calcification, and anterior bowing of the tibiae. However, we believe that careful clinical and radiological examinations can reveal more striking data which might positively reflect on the whole process of management., Comments: We postulate that the congenital limitations in neck movements in our patient developed because of the marked fusion of the hypoplastic and occipitalized atlas and simultaneous C2-C3 fusion. Therefore, if this form of malformation is disregarded, there may be involvement of the atlantoaxial structure, and this can possibly lead to serious neurological and even life-threatening complications. The use of CT scanning for the detection of such abnormalities can be remarkably important.

Published
2006
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27. Subtotal amelia in a child with autosomal recessive hypohidrotic ectodermal dysplasia.

Author

Al Kaissi A, Ben Chehida F, Nassib N, Safi H, Djnziri M, Ben Ghachem M, and Gharbi H

Subjects
Child, Ectodermal Dysplasia, Hypohidrotic, Autosomal Recessive physiopathology, Humans, Male, Tunisia, Ectodermal Dysplasia, Hypohidrotic, Autosomal Recessive genetics, Ectromelia genetics, Genetic Diseases, Inborn physiopathology
Abstract

We report an inbred Tunisian family, in which the proband manifested signs of hypohidrotic ectodermal dysplasia, subtotal amelia, scoliosis and left renal agenesis. Two other family members had the full clinical criteria of hypohidrotic ectodermal dysplasia, characterized by deficient sweat glands, hypodontia, hypoplasia of the mucous glands, and fine hair. Nine family subjects had variable clinical expression of the disorder.

Published
2005
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