Hypophosphataemic Rickets Secondary to Raine Syndrome: A Review of the Literature and Case Reports of Three Paediatric Patients’ Dental Management

Hirst, Lorna; Abou-Ameira, Gehan; Critchlow, Simon

doi:https://doi.org/10.1155/2021/6637180

Case Reports in Pediatrics

On this page

Abstract Introduction Discussion Data Availability Consent Conflicts of Interest Authors’ Contributions Supplementary Materials References Copyright Related Articles

Case Report | Open Access

Volume 2021 | Article ID 6637180 | https://doi.org/10.1155/2021/6637180

Hypophosphataemic Rickets Secondary to Raine Syndrome: A Review of the Literature and Case Reports of Three Paediatric Patients’ Dental Management

Lorna Hirst,¹Gehan Abou-Ameira,¹and Simon Critchlow¹

Academic Editor: Junji Takaya

Received27 Oct 2020

Revised20 Dec 2020

Accepted23 Dec 2020

Published07 Jan 2021

Abstract

Raine Syndrome (RS) also referred to as lethal osteosclerotic bone dysplasia describes an exceptionally rare autosomal recessive disorder with an estimated prevalence of <1 in 1,000,000. Endocrinological manifestations such as hypophosphataemic rickets depict a recent finding within the phenotypic spectrum of nonlethal RS. The dental sequelae of hypophosphataemic rickets are significant. Spontaneous recurrent abscesses on noncarious teeth result in significant odontogenic pain and multiple dental interventions. The dental presentations of nonlethal RS are less widely described within the literature. Amelogenesis Imperfecta (AI), however, was recently postulated as a key characteristic. This article presents the dental manifestations and extensive restorative and oral surgical intervention of three siblings with hypophosphataemic rickets secondary to Raine Syndrome treated at Great Ormond Street Hospital for Children, a tertiary referral hospital.

1. Introduction

Raine syndrome (RS) (OMIM # 259775) is an especially rare autosomal recessive disorder with an estimated prevalence of <1 in 1,000,000 [1, 2]. Endocrinological manifestations such as hypophosphataemic rickets are a newly described feature within the phenotypical plethora of RS [3]. Dental sequelae of hypophosphataemic rickets are significant, broadly encompassing multiple spontaneous dental abscesses in noncarious teeth, dentine and enamel defects, and dental anomalies [4–7]. The dental presentation in RS is less frequently described in the literature.

RS is commonly referred to as lethal osteosclerotic bone dysplasia due to high mortality in the neonatal period [8]. More recently, a milder phenotype has been described that is compatible with life [1–3]. RS characteristically presents with exophthalmos, cerebral calcifications, choanal atresia, and osteosclerosis [2, 8]. Exorbitism and midfacial hypoplasia often present as a Crouzon-like facial appearance. Heterogeneity is considerable amongst the nonlethal type, and a paucity of data results in the possibility of the complete phenotypic spectrum not being delineated [1–3]. Genetically, mutations in the FAM20C gene on chromosome 7, which encodes a Golgi Casein Kinase that phosphorylates fibroblast growth factor 23 (FGF23), account for RS, with a high frequency of consanguineous parents in affected patients [2, 3, 9, 10].

Hypophosphataemic rickets is a disorder of the growing skeleton, characterised by hypophosphatemia, impaired intestinal absorption of calcium, and rickets that is resistant to vitamin D [11, 12]. Phosphate is the main component of hydroxyapatite (Ca₁₀(PO₄)₆(OH)₂) and essential in cell metabolism (adenosine triphosphate (ATP)) [11]. Homeostasis of serum phosphate levels are controlled by renal absorption, bone resorption, and hormonal (calcitriol, parathyroid hormone (PTH), and fibroblast growth factor 23 (FGF23)) regulation of intestinal absorption [5, 11]. Subsequent hypophosphatemia, thus, impairs mineralisation of the teeth, bones, and cartilage [5, 13].

Clinical features include bowing of lower extremities, disproportionately short stature, cranial osseous deformities, and dental manifestations [5, 12, 14]. The dental presentation is significant and associated with a lifelong burden of restorative and oral surgical intervention. The most common clinical presentation is multiple recurrent dental abscesses in noncarious teeth, and in some patients, this may be the first clinical manifestation of their disease [4, 5]. Defects in dentine mineralisation, thin, hypoplastic enamel, enlarged pulp chambers extending to the enamel–dentine junction (EDJ), and root resorption are commonly cited [4–6, 11, 14, 15].

2. Case Descriptions

This paper describes three siblings, 14- and 13-year-old males and an 11-year-old female, of Somalian descent. Their parents are second cousins. The siblings had a diagnosis of hypophosphataemic rickets secondary to Raine Syndrome caused by homozygous mutation in FAM20C gene [FAM20C. C (1094G > T); C (1094G > T). P. (Gly365Val); and (P. (Gly365Val)]. A summary of their medical and dental management can be seen in Table 1.

2.1. Case One

Case one describes a 14-year-old male who initially presented to Great Ormond Street Hospital with nystagmus and raised intracranial pressure associated with a sagittal synostosis. This was treated with a posterior vault expansion at the age of 2. On clinical examination, he had a convexity over the closed anterior fontanelle, a high anterior hairline, mild exorbitism, midfacial hypoplasia, narrow nose, and high narrow palate. He also had generalised osteosclerosis. His body proportions and limbs were only mildly affected.

Dentally, he was first treated at the age of seven, when he presented with spontaneous abscesses of the maxillary central incisors, left lateral incisor, and left first permanent molars requiring extraction under general anaesthetic (GA). At the age of eight, further abscesses of the mandibular incisors and maxillary left first premolar occurred, which were also extracted under GA. He later presented with additional abscesses on the maxillary right first premolar at the age of nine, which was extracted under local anaesthetic (LA). Later that year, abscesses also presented on all mandibular premolars. These teeth were surgically extracted under GA along with the mandibular left canine. At the age of ten, further abscesses presented and the decision to complete a full clearance under GA was made. Prosthetic intervention included provision of sequential complete dentures (C/C) to account for the growth. In the future, dental implants may be considered to enhance the stability and retention of the prostheses.

2.2. Case Two

Case two depicts a 13-year-old male. He presented with sagittal and lambdoid craniosynostosis with raised intracranial pressure at the age of 15 months, which was treated with biparietal vault expansion. Bilateral intracranial calcification was also diagnosed of the globi pallidi, right corona radiata, and left parietal lobes. On clinical examination, he had a turricephalic head shape with a tall, bossed forehead, high anterior hairline, and convexity over the closed anterior fontanelle. Hypotelorism, down-slanting palpebral fissures and midfacial hypoplasia with a high narrow palate, midline raphe, and wide uvula were also present. Additionally, he had generalised osteosclerosis, a barrel-shaped chest, spinal hyperlordosis, and scoliosis, and leg bowing was apparent with joint laxity. Furthermore, he had obstructive sleep apnoea (OPA), which was treated with Bilevel Positive Airway Pressure (BiPAP); in addition, he received an adenoidectomy at the age of 6.

Dentally, at the age of three, he presented with multiple spontaneous abscesses in the primary dentition. He required a GA for extraction of all primary first and second molars and primary maxillary canines. The first permanent molars were spontaneously abscessed at the age of six and were also extracted under GA. At the age of nine, he presented with significant odontogenic pain and further abscesses. Radiographically, bilateral cysts were noted in the mandible. Treatment options for multiple root canal treatments (RCTs) or extractions were discussed with the family, who opted for a full clearance at this time. This was completed under GA along with enucleation of the mandibular cysts. Removable prosthesis was subsequently constructed.

2.3. Case Three

Case three presents the youngest sibling, an 11-year-old female. Craniofacially, she presented with sagittal craniosynostosis and metopic ridging. Additionally, bilateral intracranial calcification was evident of the globus pallidi and scattered throughout both cerebral hemispheres. There were no concerns about raised intracranial pressure. Clinically, she also had a convexity over the closed anterior fontanelle, a high anterior hairline, mild exorbitism, midfacial hypoplasia, narrow nose, and high narrow palate. She also had generalised osteosclerosis, short stature, and leg bowing. Additionally, she had hypertension with mild renal impairment.

Dentally, she initially presented with multiple recurrent abscesses requiring repeat courses of amoxicillin. She received a general anaesthetic (GA) at the age of seven, for extraction of all primary first and second molars and primary maxillary canines. At the age of eight, she presented with a spontaneous abscess of mandibular right central incisor and had first-stage root canal therapy under local anaesthetic. At the age of nine, she presented with a retained root of the maxillary right primary second molar, which was extracted under local anaesthetic (LA). At the age of ten, she presented with draining sinuses and pulp exposure of the maxillary left central incisor. Treatment options were attempt root canal treatment (RCT) of mandibular central incisors, left lateral incisor, and maxillary left central incisor and extractions of maxillary left second premolar and first permanent molar or full clearance and provision of a prosthesis.

3. Discussion

Metabolic bone disorders, such as hypophosphataemic rickets, pose a relatively new characteristic of Raine Syndrome (RS) [1, 3]. Biallelic variations in the FAM20C gene provide the genetical basis of RS [1, 2]. FAM20C is essential for biomineralization and encodes the human homolog of dentine matrix protein 4 (DMP4), which is highly expressed in odontoblasts and somewhat in bone, where it is postulated to have a role in mineralisation [1, 3]. Mutations in dentine matrix protein 1 (DMP1) have been established in the aetiology of inherited forms of hypophosphataemic rickets (HHR) [1]. Further research is warranted, although it is anticipated that the roles of DMP4 and DMP1 are comparable, thus hypothesising a link between Raine Syndrome and hypophosphataemic rickets [1, 3]. A comparison of the clinical, radiographic, and histological features of RS and HHR are depicted in Table 2.

The dental presentations of the three siblings are complex and significant, overlapping the phenotypic spectra of both HHR and RS described within the literature. Notably, features specific to RS were evident, such as high-vaulted palate and radiographic lack of distinction between enamel and dentine. Characteristics implying HHR were also present, such as recurrent spontaneous dental abscesses, sinus tracts, spontaneous loss of vitality, enlarged pulp horns, and taurodontism. Overarching and interrelated features across both RS and HHR included generalised hypoplastic, yellow-brown enamel, malocclusion, and root hypoplasia. The paucity of data regarding the complete dental phenotypical spectra of nonlethal RS, combined with the superimposed infrequent finding of hypophosphataemic rickets, makes it challenging to ascertain with a great degree of confidence the precise aetiology of the dental anomalies within the three siblings.

A presenting complaint of multiple recurrent abscesses associated with noncarious teeth is frequent in certain patients with hereditary hypophosphataemic rickets and was the underlying presentation in our cases. Provision of root canal treatment (RCT) in such patients can be complicated by atypical pulpal morphology and root hypoplasia [4, 6, 14]. The propensity towards endodontic failure and recurrent abscess formation may be attributed to reinfection of the root canal system due to dentinal defects [4]. Preventative measures such as oral hygiene instruction, dietary advice, and fluoride varnish application (22,600 ppm) are indispensable in reducing the burden of dental disease.

Whether medical treatment of hereditary hypophosphataemic rickets can prevent or expressively reduce the characteristic dental phenotype is a contentious issue in the medical literature. Prevention of dentinal effects in the primary dentition is evidently largely unfeasible since dentinogenesis of the primary dentition occurs in utero. The provision of medication postnatally, however, theoretically has the potential to beneficially affect the formation of permanent dentinal hard tissues. Conventional treatment regimens for HHR may include oral phosphate supplementation and activated vitamin D, such as calcitriol. Since inorganic phosphate and calcium are fundamental for dental mineralisation in a similar way to bone mineralisation, a link between hypophosphatemia and aberrations in dental structure is clearly discernible [6]. Several studies have demonstrated phosphate supplements reducing irregularities in mineralisation or even curing dental anomalies [6]. Contrarily, other studies debate the role of medical therapy in the correction of dental calcification [4, 6, 16], whilst others suggest that conventional therapy may be preferable to newer therapies, such as Burosumab, in reducing dental effects in HRR [4, 6, 16].

The paucity of cases of Raine Syndrome, particularly the nonlethal phenotype and challenges in management, precludes the ability to definitively determine the relationship between disease progression and dental manifestations. To further complicate matters, the complete dental phenotype of Raine Syndrome is unlikely fully delineated. Additionally, certain dental manifestations, notably, amelogenesis imperfecta and cleft lip and palate, have the potential to be superimposed dental features in some patients, rather than related to the underlying Raine Syndrome diagnosis.

Raine Syndrome is an extremely rare inherited disorder with amelogenesis imperfecta and ectopic tissue calcifications being common dental manifestations. The dental phenotype of hereditary hypophosphataemic rickets is, however, more widely described within the literature. The precise aetiology of the dental anomalies in our patients may be attributable to hypophosphatemia during dentinogenesis or primarily due to mutations in the FAM20C gene itself. The paucity of cases of nonlethal Raine Syndrome means that dental phenotypical spectrum may not be fully known. Independent of the exact aetiology of the enamel–dentine defects present in these three patients, the dental management follows the overarching principles of comprehensive prevention, early control of infection, pulpal protection, and long-term restorative stability.

Data Availability

Data sharing was not applicable to this article as no datasets were generated or analysed in the production of the manuscript.

Informed written consent was obtained from the parents/legal guardians of all cases in this case report prior to submission regarding the publication of images and data. The purpose of the case report was explained to all participants including what information would be published. All participants were advised that declining consent would not impact their clinical care and that they have the right to withdraw their consent at any point prior to publication.

Conflicts of Interest

The authors declare that they have no conflicts of interest regarding the publication of this paper.

Authors’ Contributions

LH was responsible for writing the first draft and modifying subsequent drafts as the first author and also responsible for obtaining consent. GAA and SC were responsible for verifying dental content and acted as treating clinicians. All authors have made substantive contribution to this manuscript, and all have reviewed the final paper prior to submission.

Supplementary Materials

Case 1. Complete prosthesis at the age of 14. Case 2. Dentition at the age of 5. Case 2. Extra-oral midface hypoplasia at the age of 5. Case 3. Abnormal pulpal pathology, root hypoplasia, and poor discrimination between enamel and dentine radiographically. Case 3. Dentition at the age of 11. (Supplementary Materials)

References

C. Mameli, G. Zichichi, N. Mahmood et al., “Natural history of non-lethal Raine syndrome during childhood,” Orphanet Journal of Rare Diseases, vol. 15, no. 1, 2020.
View at: Publisher Site | Google Scholar
S. C. Elalaoui, N. Al-Sheqaih, I. Ratbi et al., “Non lethal Raine syndrome and differential diagnosis,” European Journal of Medical Genetics, vol. 59, no. 11, pp. 577–583, 2016.
View at: Publisher Site | Google Scholar
N. Mahmood, A. Donne, A. Weber, and P. Dharmraj, “Raine syndrome: a review and a report of metabolic bone disease as a new link,” Research, vol. 1, p. 1, 2014.
View at: Publisher Site | Google Scholar
S. Alexander, L. Moloney, and N. Kilpatrick, “Endodontic management of A patient with X-linked hypophosphataemic rickets,” Australian Endodontic Journal, vol. 27, no. 2, pp. 57–61, 2001.
View at: Publisher Site | Google Scholar
A. Coelho, P. Marques, and J. P. Canta, “Case report: dental treatment of a child with hypophosphataemic rickets,” European Archives of Paediatric Dentistry, vol. 8, no. S1, pp. 35–38, 2007.
View at: Publisher Site | Google Scholar
M. M. I. Sabandal, P. Robotta, S. Bürklein, and E. Schäfer, “Review of the dental implications of X-linked hypophosphataemic rickets (XLHR),” Clinical Oral Investigations, vol. 19, no. 4, pp. 759–768, 2015.
View at: Publisher Site | Google Scholar
C. Chaussain-Miller, C. Sinding, D. Septier, M. Wolikow, M. Goldberg, and M. Garabedian, “Dentin structure in familial hypophosphatemic rickets: benefits of vitamin D and phosphate treatment,” Oral Diseases, vol. 13, no. 5, pp. 482–489, 2007.
View at: Publisher Site | Google Scholar
B. Vishwanath, K. Srinivasa, and M. V. Shankar, “Raine syndrome,” Indian Journal of Human Genetics, vol. 20, no. 1, p. 72, 2014.
View at: Publisher Site | Google Scholar
M. Koob, B. Doray, M. Fradin, D. Astruc, and J.-L. Dietemann, “Raine syndrome: expanding the radiological spectrum,” Pediatric Radiology, vol. 41, no. 3, pp. 389–393, 2010.
View at: Publisher Site | Google Scholar
K. Michael, D. M. Nelson, and A. Ortmeier, “Raine syndrome,” Journal of Diagnostic Medical Sonography, vol. 27, no. 4, pp. 167–170, 2011.
View at: Publisher Site | Google Scholar
V. Saraff, R. Nadar, and W. Högler, “New developments in the treatment of X-linked hypophosphataemia: implications for clinical management,” Pediatric Drugs, vol. 22, no. 2, pp. 113–121, 2020.
View at: Publisher Site | Google Scholar
A. McBride, M. Edwards, F. Monsell, and M. Gargan, “Vitamin D-resistant rickets (X-linked hypophosphataemic rickets),” Current Orthopaedics, vol. 21, no. 5, pp. 396–399, 2007.
View at: Publisher Site | Google Scholar
B. Godden, C. Hilditch, and R. Agrawal, “Unexplained case of hypophosphataemic rickets,” Journal of Paediatrics and Child Health, vol. 55, no. 7, pp. 851–853, 2019.
View at: Publisher Site | Google Scholar
S. L. Hughes and E. J. Hingston, “Spontaneous dental abscesses in hereditary hypophosphataemic rickets: a preventive restorative approach in the primary dentition,” Dental Update, vol. 46, no. 11, pp. 1067–1072, 2019.
View at: Publisher Site | Google Scholar
M. Zambrano, N. G. Nikitakis, M. C. Sanchez-Quevedo, J. J. Sauk, H. Sedano, and H. Rivera, “Oral and dental manifestations of vitamin D-dependent rickets type I: report of a pediatric case,” Oral Surgery, Oral Medicine, Oral Pathology, Oral Radiology, and Endodontology, vol. 95, no. 6, pp. 705–709, 2003.
View at: Publisher Site | Google Scholar
R. J. Gordon and M. A. Levine, “Burosumab treatment of children with X-linked hypophosphataemic rickets,” The Lancet, vol. 393, no. 10189, pp. 2364–2366, 2019.
View at: Publisher Site | Google Scholar

Copyright

Copyright © 2021 Lorna Hirst et al. This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

PDF Download Citation

Download other formats

Order printed copies

Views

564

Downloads

815

Citations