Diagnosing nail-patella syndrome: can it be so simple?

We describe here an interesting case of a 7-day-old male infant brought with parental concerns of inability to extend both knees. Clinical evaluation revealed dysplastic fingernails, bilateral abnormal patellae, triangular lunules in conjunction with pathognomic iliac horns on pelvic radiographs suggesting the possibility of nail-patella syndrome (NPS). Other competing diagnoses with similar phenotypic features were considered and sequentially excluded. A definitive diagnosis was established by the identification of the principal mutation at the LMX1B gene locus of chromosome 9. NPS is seldom diagnosed in neonates due to the heterogeneity of clinical presentations as well as the subtlety of clinical clues in this population. NPS is a dominantly inherited disorder that is predominantly familial in origin and thus carries important implications for the prenatal diagnosis of future pregnancies as well as pre-emptive surveillance of nephropathy in the index child.

Download Full-text

Novel differentiation antigens on late erythrocytic progenitor cells detected by alloantisera made between mouse strains congenic at the Fv-2 locus.

Journal of Experimental Medicine ◽

10.1084/jem.155.5.1491 ◽

1982 ◽

Vol 155 (5) ◽

pp. 1491-1500 ◽

Cited By ~ 2

Author(s):

D S Vaithilingam ◽

A A Axelrad

Keyword(s):

Bone Marrow ◽

Spleen Cell ◽

Progenitor Cells ◽

Gene Locus ◽

Cell Suspensions ◽

Chromosome 9 ◽

Mouse Strains ◽

Spleen Cells ◽

Linked Gene ◽

Differentiation Antigens

We have investigated the activities of alloantisera produced in B6 (C57BL/6) and B6.S strain mice reciprocally immunized with unwashed bone marrow and spleen cell suspensions from their respective Fv-2 congenic partner strains, B6.S and B6. These antisera inhibited the formation of colonies by the late erythrocytic progenitors (CFU-E) in plasma cultures seeded with unwashed bone marrow or spleen cells; washed cells were unaffected. Erythropoietic burst formation by the early progenitors (BFU-E) was not significantly inhibited by the antisera, whether the cells were washed or unwashed. We conclude (a) that the congenic antisera are capable of recognizing alloantigens controlled by alleles of Fv-2 or of a closely linked gene locus on chromosome 9; (b) that these alloantigens are situated on the surface of erythrocytic progenitor cells and can be removed by washing; and (c) that the expression of the alloantigens on these cells is influenced by their stage of differentiation.

Download Full-text

First-trimester prenatal diagnosis of cystic fibrosis using fibroblasts from a deceased index child to establish haplotypes

Prenatal Diagnosis ◽

10.1002/pd.1970080810 ◽

1988 ◽

Vol 8 (8) ◽

pp. 625-628 ◽

Cited By ~ 2

Author(s):

Ann Curtis ◽

Lisa Strain ◽

Moira Mennie ◽

Susan Holloway ◽

J. A. Raeburn ◽

...

Keyword(s):

Cystic Fibrosis ◽

Prenatal Diagnosis ◽

First Trimester ◽

Index Child

Download Full-text

Molecular Delineation of De Novo Small Supernumerary Marker Chromosomes in Prenatal Diagnosis, A Retrospective Study

10.21203/rs.3.rs-927187/v2 ◽

2021 ◽

Author(s):

Shuang Hu ◽

Xiangdong Kong

Keyword(s):

Genetic Counseling ◽

Prenatal Diagnosis ◽

De Novo ◽

Snp Array ◽

Chromosome 9 ◽

Marker Chromosomes ◽

Number Variation ◽

Low Coverage ◽

Small Supernumerary Marker Chromosomes ◽

Supernumerary Marker Chromosomes

Abstract Background To define the genotype-phenotype correlation of small supernumerary marker chromosomes (sSMCs) and conduct precise genetic counseling, we retrospectively searched and reviewed de novo sSMC cases detected during prenatal diagnosis at The First Affiliated Hospital of Zhengzhou University. Chromosome karyotypes of 20,314 cases of amniotic fluid from pregnant women were performed. For 16 samples with de novo sSMCs, 10 were subjected to single-nucleotide polymorphism (SNP) array or low-coverage massively parallel copy number variation sequencing (CNV-seq) analysis. Results Among the 10 sSMC cases, two sSMCs derived from chromosome 9, and three sSMCs derived from chromosomes 12, 18 and 22. The remaining 5 cases were not identified by SNP array or CNV-seq because they lacked euchromatin or had a low proportion of mosaicism. Four of them with a karyotype of 47,XN,+mar presented normal molecular cytogenetic results (seq[hg19] 46,XN), and the remaining patient with a karyotype of 46,XN,+mar presented with Turner syndrome (seq[hg19] 45,X). Five sSMC samples were mosaics of all 16 cases. Conclusion Considering the variable origins of sSMCs, further genetic testing of sSMCs should be performed by SNP array or CNV-seq. Detailed molecular characterization would allow precise genetic counseling for prenatal diagnosis.

Download Full-text

Pyoderma gangrenosum: An ulcerative variant developing at a paraincisional LSCS scar site

Our Dermatology Online ◽

10.7241/ourd.20212.11 ◽

2021 ◽

Vol 12 (2) ◽

pp. 153-155

Author(s):

Kritika Pandeyy ◽

Mansak Shishak ◽

Neeraj Yadav

Keyword(s):

Pyoderma Gangrenosum ◽

Multidisciplinary Approach ◽

Immunosuppressive Agents ◽

Scar Tissue ◽

Interesting Case ◽

Lower Segment ◽

Clinical Presentations ◽

Oral Corticosteroids ◽

Initiation Of Therapy ◽

Prompt Diagnosis

Pyoderma gangrenosum (PG) is an uncommon entity based on a diagnosis of exclusion. It can manifest itself mimicking various ulcerative cutaneous conditions and nonhealing wounds. With its less known etiology and presentation, there is a danger of mistreatment. Herein, we present an interesting case of pyoderma gangrenosum in a young woman, developing around the area of a lower segment Cesarean scar, but not involving the scar tissue. The PG was not associated with any underlying systemic ailments and responded well to a tapering dose of oral corticosteroids. Prompt diagnosis and initiation of therapy lead to a good response and favorable prognosis. Recognizing the atypical clinical presentations of PG is pertinent. Treatment with immunosuppressive agents and a multidisciplinary approach are recommended.

Download Full-text

Responding to Parental Concerns After a Prenatal Diagnosis of Trisomy 21

Journal of Developmental & Behavioral Pediatrics ◽

10.1097/00004703-200104001-00015 ◽

2001 ◽

Vol 22 (SUPPLEMENT) ◽

pp. S73-S76 ◽

Cited By ~ 1

Author(s):

&NA;

Keyword(s):

Prenatal Diagnosis ◽

Trisomy 21 ◽

Parental Concerns

Download Full-text

Familial intestinal degenerative neuropathy with chronic intestinal pseudo-obstruction linked to a gene locus with duplication in chromosome 9

Scandinavian Journal of Gastroenterology ◽

10.1080/00365521.2019.1697741 ◽

2019 ◽

Vol 54 (12) ◽

pp. 1441-1447

Author(s):

Hasse Abrahamsson ◽

Frida Ahlfors ◽

Susanne Fransson ◽

Staffan Nilsson ◽

Hans Linander ◽

...

Keyword(s):

Gene Locus ◽

Chromosome 9 ◽

Intestinal Pseudo Obstruction

Download Full-text

22q12.3-q13.1 microdeletion including SOX10 causes atypical Waardenburg syndrome

European Journal of Ophthalmology ◽

10.1177/1120672120944350 ◽

2020 ◽

pp. 112067212094435

Author(s):

Wenqiu Zhang ◽

Lirong Xiao ◽

Bingjie Chen ◽

Yingwen Xu ◽

Naihong Yan

Keyword(s):

Congenital Heart Disease ◽

Laboratory Tests ◽

Congenital Heart ◽

Heart Defects ◽

Male Infant ◽

Routine Laboratory ◽

Waardenburg Syndrome ◽

Whole Exome ◽

Clinical Presentations ◽

Severe Congenital Heart Disease

Purpose: To identify disease associated mutations in a male infant with congenital heart defects and heterochromia. Methods: A detailed clinical examination and routine laboratory tests were performed on the patient. We applied whole exome sequencing to identify the causal mutation on the proband and other family members. Results: The patient presented with severe congenital heart disease, strabismus, and pigment disturbances of the iris. We identified a deletion of 1.99 megabase [arr[hg19]22q12.3-13.1 (chr22:36656004-38643920) *1], including SOX10 and 13 RefSeq genes on this patient, which was associated with atypical Waardenburg syndrome. Conclusion: Our results suggest that a deletion of 1.99 megabase (including SOX10) acts as a dominant pathogenic variant on the clinical presentations of this patient with atypical Waardenburg syndrome.

Download Full-text