A novel missense mutation Ile538Val in the fibroblast growth factor receptor 3 in hypochondroplasia

Grigelioniené, G.; Hagenäs, Lars; Eklöf, O.; Neumeyer, Lo; Haereid, PE; Anvret, Maria

doi:10.1002/(sici)1098-1004(1998)11:4<333::aid-humu17>3.3.co;2-a

Cited by 11 publications

(13 citation statements)

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“…The known mutation p.Ile538Val found in our patient is located in the highly conserved tyrosine kinase domain of FGFR3 (Supplementary Figure S1). This mutation has been previously reported in a Swedish family with typical HCH (Grigelioniene et al, ). The p.Ile538Val mutation in the FGFR3 gene was expected to cause weak FGFR3 activation and aberrant RAS/ERK pathway (Krejci, ; Ornitz & Legeai‐Mallet, ).…”

Section: Discussionsupporting

confidence: 57%

Monoallelic FGFR3 and Biallelic ALPL mutations in a Thai girl with hypochondroplasia and hypophosphatasia

Porntaveetus

Srichomthong

Suphapeetiporn

et al. 2017

American J of Med Genetics Pt A

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Skeletal dysplasias are a complex group of more than 350 disorders with phenotypic and genotypic heterogeneity affecting bone and cartilage growth. We studied a 2-year-old girl and her 21-year-old mother with disproportionate short stature. In addition to typical features of hypochondroplasia found in both patients, the child had deformities of the extremity bones, metaphyseal flares, and bilateral transverse (Bowdler) fibular spurs with overlying skin dimples detected at birth. Intravenous pamidronate was started in the child since the age of 17 days, and then every two months. Exome sequencing revealed that the girl was heterozygous for a missense mutation (c.1651A>G, p.Ile538Val) in exon 13 of FGFR3, a known mutation for hypochondroplasia, inherited from her mother. Interestingly, the child also harbored compound heterozygous missense mutations in exon 12 of ALPL, c.1460C>T (p.Ala487Val) inherited from her mother and c.1479C>A (p.Asn493Lys) inherited from her healthy father. The former mutation was previously reported in perinatal hypophosphatasia while the latter was novel. Constantly reduced serum alkaline phosphatase levels including the one before the pamidronate administration and a substantially elevated level of plasma pyridoxal 5'-phosphate detected at age 28 months supported the diagnosis of hypophosphatasia. After a definite diagnosis was achieved, pamidronate was withdrawn at the age of 28 months. No adverse events were observed during pamidronate therapy. In conclusion, we describe a unique case with monoallelic FGFR3 and biallelic ALPL mutations leading to features of both hypochondroplasia and hypophosphatasia.

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Section: Discussionsupporting

confidence: 57%

Monoallelic FGFR3 and Biallelic ALPL mutations in a Thai girl with hypochondroplasia and hypophosphatasia

Porntaveetus

Srichomthong

Suphapeetiporn

et al. 2017

American J of Med Genetics Pt A

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“…Genetic heterogeneity has been found in some families by excluding linkage to 4p16.3 [Stoilov et al, 1995; Rousseau et al, 1996a; Grigelioniene et al, 1998]. Other mutations have been found in isolated families, including Ile538Val [Grigelioniene et al, 1998], Asn540Thr [Deutz‐Terlouw et al, 1998], Asn328Ile [Winterpacht et al, 2000], and Asn540Ser [Mortier et al, 2000] (Table XXIII).…”

Section: Fgfs/fgfrs Fgfr3 Skeletal Dysplasias Craniosynostosis Andmentioning

confidence: 99%

The new bone biology: Pathologic, molecular, and clinical correlates

Cohen

2006

American J of Med Genetics Pt A

285

197

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Bone and cartilage and their disorders are addressed under the following headings: functions of bone; normal and abnormal bone remodeling; osteopetrosis and osteoporosis; epithelial-mesenchymal interaction, condensation and differentiation; osteoblasts, markers of bone formation, osteoclasts, components of bone, and pathology of bone; chondroblasts, markers of cartilage formation, secondary cartilage, components of cartilage, and pathology of cartilage; intramembranous and endochondral bone formation; RUNX genes and cleidocranial dysplasia (CCD); osterix; histone deacetylase 4 and Runx2; Ligand to receptor activator of NFkappaB (RANKL), RANK, osteoprotegerin, and osteoimmunology; WNT signaling, LRP5 mutations, and beta-catenin; the role of leptin in bone remodeling; collagens, collagenopathies, and osteogenesis imperfecta; FGFs/FGFRs, FGFR3 skeletal dysplasias, craniosynostosis, and other disorders; short limb chondrodysplasias; molecular control of the growth plate in endochondral bone formation and genetic disorders of IHH and PTHR1; ANKH, craniometaphyseal dysplasia, and chondrocalcinosis; transforming growth factor beta, Camurati-Engelmann disease (CED), and Marfan syndrome, types I and II; an ACVR1 mutation and fibrodysplasia ossificans progressiva; MSX1 and MSX2: biology, mutations, and associated disorders; G protein, activation of adenylyl cyclase, GNAS1 mutations, McCune-Albright syndrome, fibrous dysplasia, and Albright hereditary osteodystrophy; FLNA and associated disorders; and morphological development of teeth and their genetic mutations.

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“…Nine different FGFR3 missense mutations resulting in seven different amino acid substitutions are described: one in exon 9 (N328I), four in exon 13 (N540K, N540T, N540S, and I538V) and two in exon 15 (K650N and K650Q). The most frequent, N540K, accounts for more than 50% of all FGFR3 mutations in hypochondroplasia [Bellus et al, 1995; Prinos et al, 1995; Bonaventure et al, 1996; Deutz‐Terlouw et al, 1998; Grigelioniene et al, 1998; Matsui et al, 1998; Bellus et al, 2000; Mortier et al, 2000; Winterpacht et al, 2000]. Patients with N540K mutation tend to have more severe short stature and more disproportion than patients with other mutations.…”

Section: To the Editormentioning

confidence: 99%

“…Patients with N540K mutation tend to have more severe short stature and more disproportion than patients with other mutations. However, macrocephaly appears to be more severe in patients with the K650N and K650Q mutations than in patients with the other mutations (Table I) [Grigelioniene et al, 1998; Bellus et al, 2000; Winterpacht et al, 2000].…”

Section: To the Editormentioning

confidence: 99%

Hypochondroplasia and stature within normal limits: Another family with an Asn540Ser mutation in the fibroblast growth factor receptor 3 gene

Thauvin‐Robinet

Faivre

Lewin³

et al. 2003

American J of Med Genetics Pt A

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A novel missense mutation Ile538Val in the fibroblast growth factor receptor 3 in hypochondroplasia

Cited by 11 publications

References 0 publications

Monoallelic FGFR3 and Biallelic ALPL mutations in a Thai girl with hypochondroplasia and hypophosphatasia

Monoallelic FGFR3 and Biallelic ALPL mutations in a Thai girl with hypochondroplasia and hypophosphatasia

The new bone biology: Pathologic, molecular, and clinical correlates

Hypochondroplasia and stature within normal limits: Another family with an Asn540Ser mutation in the fibroblast growth factor receptor 3 gene

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