Phenotypic spectrum in osteogenesis imperfecta due to mutations in TMEM38B: unravelling a complex cellular defect.

Alsaedi, A.; Balasubramanian, M.; Cabral, W.A.; Cole, T.; Crabtree, N.J.; Fratzl-Zelman, N.; Gamsjaeger, S.; Högler, W.; Klaushofer, K.; Marini, J.C.; Paschalis, E.P.; Roschger, P.; Saraff, V.; Sargent, B.M.; Shaw, N.J.; Stewart, S.; Titheradge, H.; Vogt, J.; Webb, E.A.

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Phenotypic spectrum in osteogenesis imperfecta due to mutations in TMEM38B: unravelling a complex cellular defect.

Authors: A. Alsaedi
M. Balasubramanian
W.A. Cabral
T. Cole
N.J. Crabtree
N. Fratzl-Zelman
S. Gamsjaeger
W. Högler
K. Klaushofer
J.C. Marini
E.P. Paschalis
P. Roschger
V. Saraff
B.M. Sargent
N.J. Shaw
S. Stewart
H. Titheradge
J. Vogt
E.A. Webb
Publication date: 16 March 2017
Publisher: 'The Endocrine Society'
Doi

Abstract

Context: Recessive mutations in TMEM38B cause type XIV osteogenesis imperfecta (OI) by dysregulating intracellular calcium flux. Objectives: Clinical and bone material phenotype description and osteoblast differentiation studies. Design and Setting: Natural history study in paediatric research centres. Patients: Eight patients with type XIV OI. Main Outcome Measures: Clinical examinations included: bone mineral density, radiographs, echocardiography and muscle biopsy. Bone biopsy samples (n=3) were analysed using histomorphometry, quantitative backscattered electron microscopy and Raman microspectroscopy. Cellular differentiation studies were performed on proband and control osteoblasts and normal murine osteoclasts. Results: The clinical phenotype of type XIV OI ranges from asymptomatic to severe. Previously unreported features include vertebral fractures, periosteal cloaking, coxa vara and extraskeletal features (muscular hypotonia, cardiac abnormalities). Proband L1-L4 bone density Z-score was reduced (median -3.3 [range -4.77 to +0.1; n=7]), and increased by +1.7 (1.17 to 3.0; n=3) following bisphosphonate therapy. TMEM38B mutant bone has reduced trabecular bone volume, osteoblast and particularly osteoclast numbers, with >80% reduction in bone resorption. Bone matrix mineralization is normal and nanoporosity low. We demonstrate a complex osteoblast differentiation defect with decreased expression of early markers and increased late and mineralization-related markers. Predominance of TRIC-B over TRIC-A expression in murine osteoclasts supports an intrinsic osteoclast defect underlying low bone turnover. Conclusions: OI type XIV has a bone histology, matrix mineralization and osteoblast differentiation pattern that is distinct from OI with collagen defects. Probands are responsive to bisphosphonates and some show muscular and cardiovascular features possibly related to intracellular calcium flux abnormalities