Hypophosphatemic osteosclerosis, hyperostosis, and enthesopathy associated with novel homozygous mutations of <em>DMP1</em> encoding dentin matrix protein 1 and <em>SPP1</em> encoding osteopontin:​ the first digenic SIBLING protein osteopathy?

Whyte, Michael P.; Amalnath, S. Deepak; McAlister, William H.; McKee, Marc D.; Veis, Deborah J.; Huskey, Margaret; Duan, Shenghui; Bijanki, Vinieth N.; Alur, Suhas; Mumm, Steven

Affiliations

¹Center for Metabolic Bone Disease and Molecular Research, Shriners Hospitals for Children - St. Louis, St. Louis, MO 63110, USA

²Division of Bone and Mineral Diseases, Department of Internal Medicine, Washington University School of Medicine at Barnes-Jewish Hospital, St. Louis, MO 63110, USA

³Department of Medicine, Jawaharlal Institute of Postgraduate Medical Education and Research, Pondicherry 605006, India

⁴Mallinckrodt Institute of Radiology, Washington University School of Medicine at St. Louis Children's Hospital, St. Louis, MO 63110, USA

⁵Faculty of Dentistry and Department of Anatomy and Cell Biology, McGill University, Montreal, Quebec H3A 0C7, Canada

Abstract and keywords

The SIBLINGs are a subfamily of the secreted calcium-binding phosphoproteins and comprise five small integrin-binding ligand N-linked glycoproteins [dentin matrix protein-1 (DMP1), secreted phosphoprotein-1 (SPP1) also called osteopontin (OPN), integrin-binding sialoprotein (IBSP) also called bone sialoprotein (BSP), matrix extracellular phosphoglycoprotein (MEPE), and dentin sialophosphoprotein (DSPP)]. Each SIBLING has at least one “acidic, serine- and aspartic acid-rich motif” (ASARM) and multiple Ser-x-Glu/pSer sequences that when phosphorylated promote binding of the protein to hydroxyapatite for regulation of biomineralization. Mendelian disorders from loss-of-function mutation(s) of the genes that encode the SIBLINGs thus far involve DSPP causing various autosomal dominant dysplasias of dentin but without skeletal disease, and DMP1 causing autosomal recessive hypophosphatemic rickets, type 1 (ARHR1). No diseases have been reported from gain-of-function mutation(s) of DSPP or DMP1 or from alterations of SPP1, IBSP, or MEPE.

Herein, we describe severe hypophosphatemic osteosclerosis and hyperostosis associated with skeletal deformity, short stature, enthesopathy, tooth loss, and high circulating FGF23 levels in a middle-aged man and young woman from an endogamous family living in southern India. Both shared novel homozygous mutations within two genes that encode a SIBLING protein: stop-gain (“nonsense”) DMP1 (c.556G>T,p.Glu186Ter) and missense SPP1 (c.769C>T,p.Leu266Phe). The man alone also carried novel heterozygous missense variants within two additional genes that condition mineral homeostasis and are the basis for autosomal recessive disorders: CYP27B1 underlying vitamin D dependent rickets, type 1, and ABCC6 underlying both generalized arterial calcification of infancy, type 2 and pseudoxanthoma elasticum (PXE). By immunochemistry, his bone contained high amounts of OPN, particularly striking surrounding osteocytes. We review how our patients' disorder may represent the first digenic SIBLING protein osteopathy.

Keywords: ABCC6; Autosomal recessive hypophosphatemic rickets; Burosumab; CYP27B1; Endogamy; FGF23; Heterotopic ossification; Hydroxyapatite; Hypophosphatemia; Inorganic phosphate; Iron deficiency; Mineralization; Osteomalacia; Phosphatonin; Rickets; Scoliosis; Tooth loss

Links

DOI: 10.1016/j.bone.2019.115190

PubMed: 31843680

WoS: 000510529200021

History

Received: 2019-10-16

Revised: 2019-12-10

Accepted: 2019-12-12

Online: 2019-12-13

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Cited By (1)

Year	Entry
2021	Bhadada SK, Rao SD. Role of phosphate in biomineralization. Calcif Tiss Int. January 2021;108(1):32-40.