Next Article in Journal
Lactate-Mediated Signaling in the Brain—An Update
Next Article in Special Issue
The Impact of Single-Level ACDF on Neural Foramen and Disc Height of Surgical and Adjacent Cervical Segments: A Case-Series Radiological Analysis
Previous Article in Journal
2D Measurements of the Angle of the Vestibular Aqueduct Using CT Imaging
Previous Article in Special Issue
Is the Zero-P Spacer Suitable for 3-Level Anterior Cervical Discectomy and Fusion Surgery in Terms of Sagittal Alignment Reconstruction: A Comparison Study with Traditional Plate and Cage System
 
 
Search for Articles:
Title / Keyword
Author / Affiliation / Email
Journal
Article Type
 
 
Advanced Search
 
Section
Special Issue
Volume
Issue
Number
Page
 
Journals
Brain Sciences
Volume 13
Issue 1
10.3390/brainsci13010048
brainsci-logo
Submit to this Journal Review for this Journal Propose a Special Issue
Article Menu

Article Menu

share Share announcement Help format_quote Cite question_answer Discuss in SciProfiles thumb_up
...
Endorse textsms
...
Comment
first_page
settings
Order Article Reprints
Font Type:
Arial Georgia Verdana
Font Size:
Aa Aa Aa
Line Spacing:
Column Width:
Background:
Systematic Review

Burden of Surgical Treatment for the Management of Cervical Myelopathy in Mucopolysaccharidoses: A Systematic Review

by
Roberta Costanzo
1,*,
Lapo Bonosi
1,
Massimiliano Porzio
1,
Federica Paolini
1,
Lara Brunasso
1,
Andrea Evier Giovannini
1,
Manikon Poullay Silven
1,
Giuseppe Roberto Giammalva
1,
Giuseppe Emmanuele Umana
2,
Gianluca Scalia
3,
Domenico Gerardo Iacopino
1 and
Rosario Maugeri
1
1
Neurosurgical Clinic, AOUP “Paolo Giaccone”, Post Graduate Residency Program in Neurologic Surgery, Department of Biomedicine Neurosciences and Advanced Diagnostics, School of Medicine, University of Palermo, 90127 Palermo, Italy
2
Department of Neurosurgery, Cannizzaro Hospital, Trauma Center, Gamma Knife Center, 95125 Catania, Italy
3
Head and Neck Surgery Department, Neurosurgery Unit, Garibaldi Hospital, 95123 Catania, Italy
*
Author to whom correspondence should be addressed.
Brain Sci. 2023, 13(1), 48; https://doi.org/10.3390/brainsci13010048
Submission received: 22 November 2022 / Revised: 18 December 2022 / Accepted: 23 December 2022 / Published: 26 December 2022
(This article belongs to the Special Issue Cervical Myelopathy: Current Hurdles and Future Perspectives)
Browse Figures
Versions Notes

Abstract

:
Mucopolysaccharidoses (MPSs) are a rare group of heterogeneous genetic and metabolic disorders, caused by loss of functions of several enzymes that are involved in glycosaminoglycan catabolism. Their progressive accumulations in cells, tissues, and consequently, organs lead to several clinical manifestations, such as musculoskeletal involvement. Indeed, the most common manifestation in the central nervous system is represented by cervical spinal stenosis due to bony alterations or dural thickening. Cervical involvement can commonly cause myelopathy and instability exerting severe symptoms. A prompt diagnosis and treatment of the aforementioned conditions is mandatory to ensure a better quality of life in patients with such debilitating disorders. Nevertheless, a clear consensus about their management (i.e., surgical or not) is still lacking, leading to an inevitable delay. This review aims to investigate and discuss the main causes of myelopathy in patients with mucopolysaccharidoses, available therapeutic strategies, and the impact and role of surgery on the neurological outcome.

1. Introduction

Mucopolysaccharidoses (MPSs) are a rare group of heterogeneous genetic disorders involving glycosaminoglycan (GAGs)—or mucopolysaccharides—catabolism, caused by mutations inactivating lysosomal enzymes that are required for GAGs degradation [1].
The incidence rate of MPSs is around 1:22,000–25,000 live births. The overall incidence of specific MPSs disorders varies between ethnic groups [2,3].
GAGs are a heterogeneous family of linear, complex, and highly sulfated polysaccharides which constitute many proteins and proteoglycans, which are functional units of human connective tissue [2,4]. GAGs degradation is performed by specific enzymes, exoglycosidases, and sulfatases, acting in succession; therefore, a lack of their function leads to altered GAGs degradation and overloading in urine, blood, and cerebrospinal fluid (CSF) [1,3,5]. MPSs pathophysiological mechanisms hence regard a block of the lysosomal degradative function, leading to GAGs accumulation and progressive cellular damage. Multiple tissues and organs can be involved [1]. Nowadays, 7 types and 13 subgroups of MPSs syndromes have been identified, which are caused by deficiencies in one or multiple of eleven different enzymes [3].
The symptoms and their severity widely diverge between the wide-ranging set of these syndromes. Musculoskeletal involvement is a common manifestation. In particular, the thoracolumbar spine and the cranio-cervical junction with consequent cervical myelopathy represent the two main locations of spinal cord compression [2]. Early diagnosis and treatment are the only chance to ensure stable clinical status and a better quality of life. In this regard, neurosurgeons play a crucial role in patients’ therapeutic strategy. Hence, in this systematic review the authors searched the literature to investigate and discuss the main causes of myelopathy in patients with mucopolysaccharidoses, available therapeutic strategies, and the impact of surgery on the neurological outcome, considering new enzyme replacement therapies.

2. Materials and Methods

A systematic literature review was conducted following the preferred reporting Items for systematic reviews and meta-analyses guidelines (PRISMA) (Figure 1). The authors performed a broad systematic literature search in the PubMed database for all studies investigating the cervical spine involvement in patients with mucopolysaccharidosis (MPS), both clinically and surgically. The authors made systematic searches for studies that were published up to June 2022, without backward limits, using the following Mesh and free text terms as follows: “Mucopolysaccharidosis”, “Cervical Spine”, “Spinal Cord”, “Cervical”, “Myelopathy”, “Spinal Cord Compression”, “Cervical Stenosis”, Cervical disease”, “Hurler”, “Scheie”, “Maroteaux”, “Morquio”, “Hunter”, “Sly”, and “Sanfilippo” combined using Boolean operators “AND” and “OR”. To avoid the potential omission of relevant studies, the authors also manually screened reference lists of articles that were included and previous systematic reviews and meta-analyses regarding cervical spine involvement in MPS diseases. Duplicate articles were excluded using Microsoft Excel 16.37 (Redmond, WA, USA).

2.1. Study Selection

The research strategy initially relied on title and abstract analysis. The article’s full text was retrieved for further investigation if the title and abstract met the inclusion criteria. Two authors (M.P. and L.B.) independently assessed eligibility based on “a priori” criteria. The data collection process was conducted without using any automated tools. No ethical approval was required for this study.

2.1.1. Eligibility Criteria

The articles were selected according to the following inclusion criteria:
  • Full article in English
  • Clinical studies (case reports, case series, retrospective/prospective studies)
  • Patients that were affected by MPS without regarding the type of disease
  • Studies focusing on patients with cervical spine involvement and consequent cervical myelopathy
The exclusion Criteria were:
  • Articles that were not in English
  • Article that did not focus on surgical treatment
  • Patients that were not affected by MPS
  • Patients with spine involvement other than cervical segment
  • Patients with cervical spine involvement without clinical signs of cervical myelopathy

2.1.2. Data Extraction

According to the aforementioned criteria, all of the articles were identified independently by two reviewers (M.P and L.B). The extracted data included the following: author, publication time, country, study design, patient characteristics (number of patients, age, and gender), MPS typology, cervical spine level, etiology of myelopathy and clinical manifestations, surgical treatment modalities, clinical outcomes, additional treatment, adverse events (AEs), other localizations of MPS disease, and follow-up time.

3. Results

3.1. Data Selection

A total of 1176 articles were identified on the PubMed database. After duplicates removal (1104), based on a screening by title and abstract, we excluded further 519 articles.
There were 25 articles that were not included because they were based on preclinical studies, 32 were excluded because they were not focused on surgical strategies, 27 because they did not mention a cervical spine involvement, and finally, 27 due to incompatibility with our eligibility criteria. A total of 42 articles were included in the present systematic review. The patients’ demographics are shown in Table 1.

Patients’ Demographic and Clinical Evidence

A total of 247 patients were collected, 43.13% females (n =66) and 56.86% males (n = 87). The mean age of the patients at the time of myelopathy diagnosis was about 11.01 ± 8.80 years. The main types of mucopolysaccharidosis that were involved were: 13 patients with Type I (5.26%), 10 patients with Type II (4.04%), 1 patient with Type III (0.40%), 132 patients with Type IV (53.44%), 88 patients with Type VI (35.62%), 2 patients with Type VII (0.80%), 1 patient with the intermediate phenotype V-VI (0.40%); the rates are shown in Figure 2.
For each type of Mucopolysaccharidosis, the main level of cervical compression is shown in Table 2. The main cervical spine tracts that were involved were: 3 patients C0–C1 (1.21%); 112 patients C0–C2 (45.34%); 21 patients C0–C3 (8.50%); 2 patients C0–C4 (0.80%); 7 patients C1 (2.83%); 73 patients C1–C2 (29.55%); 4 patients C1–C3 (1.61%); 1 patient C1–C4 (0.40%); 1 patient C1–C6 (0.40%); 1 patient C1–C7 (0.40%); 2 patients C2 (0.80%); 6 patients C2-C3 (2.42%); 2 patients C2–C4 (0.80%); 1 patient C2–C5 (0.40%); 1 patient C3–C4 (0.40%); 2 patients C3–C5 (0.80%); 3 patients C7–T1 (1.21%); 2 patients C7–T2 (0.80%); and 3 N/A (1.21%) (Figure 3).
In Figure 3, we show the main cervical spine level that is involved with a clear prevalence of the cranio-vertebral junction (C0–C2), including a total of 197 patients (79.73%).
The different etiologies of MPS cervical compression were investigated and 15.38% (n = 38) of the cases were related to flavum ligamentum hypertrophy and dura mater thickening, 14.57% (n = 36) cases were due to atlanto-axial instability, and 65.58% (n = 162) of cases were due to the association of both conditions. Moreover, 39.67% of patients that were included in this review that were affected by MPS Type IV cervical myelopathy were related to atlanto-axial instability, while in 23.88% of patients with MPS Type VI were due to cervical stenosis. Patients that were included in this review presented clinical symptoms of motor disturbances, ranging from 78.07% of myelopathy symptoms, to 70.17% of paresis, 1.31% of plegia, and 47.80% alteration or/and inability to walk. Surgical treatment of choice was osteo-ligamentous decompression in 92.30% of patients (n = 228), and was associated to fusion in 45.17% of cases (n = 103). The median follow-up was about 61.31 ± 65.07 months, with a comprehensive evaluation of patients’ postoperative neurological status. The clinical outcome improved in 90.04% (n = 199), deteriorated in 4.07% (n = 9), while was stable in 5.42% of cases (n = 12). Furthermore, according to our literature review, among 10 studies (27.02%) surgery was delayed, with a mean time of 2.9 years after diagnosis of cervical myelopathy. In the other 27 studies (72.97%), surgery was planned immediately after the diagnosis of cervical myelopathy.

4. Discussion

Mucopolysaccharidoses are a heterogeneous and wide-ranging set of genetic syndromes that are characterized by progressive and debilitating diffuse manifestations, with a high rate of morbidity and mortality for affected patients. Even so, some key manifestations, such as musculo-skeletal spinal features, are commonly shared among some types of MPSs.
Once a clinical diagnosis is made, typically within the first years of life, based on the phenotype of these patients, neurologic assessment, and neuroimaging features, a following biochemical diagnosis is conducted. Moreover, genetic examinations of the patients and their relatives can be performed before birth as well [25,47].
The cervical spine is often affected by radiological abnormalities, resulting in spinal cord compression, secondary to malformations of the spine and the CVJ, and/or deposit of GAGs in the soft tissues adjacent the spinal cord. The natural history of spinal cord compression sequentially encompasses local ischemia, edema, neuronal cell death, with subsequent myelomalacia.
Notably, CVJ instability is a hallmark feature in many different diseases and is mostly recognized in MPS Type I, IV, and VI, while cervical canal stenosis can be often found in the majority of MPSs, mainly in Type I, II, VI, and VII [45,48].
In addition, patients with classical MPS Type IV A may present severe skeletal dysplasia and growth disturbances that affect the respiratory function [44].
Clinical findings are often represented by cervical myelopathy symptoms, arising from long tracts compression, including bilateral motor deficits, painful paresthesia, sphincter disturbances, and hyperreflexia. Thus, in this systematic review, all of the studies that were selected and evaluated involved patients with cervical myelopathy, enlightening how this condition is a common and recurring characteristic of these genetic disorders. Indeed, from a neurosurgical point of view, plain and dynamic radiographs, CT, and MR scans play an important role in MPSs management.
Typical radiological musculoskeletal features that are observed in MPSs cervical spine are:
  • Odontoid hypoplasia and peri-odontoid soft tissue masses arising from GAGs deposits posterior to the odontoid process. Atlantoaxial subluxation and occipito-atlantoaxial instability, sustained by odontoid hypoplasia and laxity of the transverse and alar ligaments is less commonly observed in MPSs [47].
  • Reactive hypertrophy of the ligamentum flavum
  • Dural thickening
  • Protrusion and/or intervertebral disc herniations [2,44].
  • Basilar invagination or enlarged morphology of the mastoid processes [44].
All these abnormalities can lead to severe spinal canal stenosis and related alterations, with or without abnormally high signal intensity zone in T2-weighted MRI sequences, otherwise the typical radiological signs that are associated with cervical myelopathy [49,50].
It has been observed that patients with MPS Type VI tend to develop posterior longitudinal ligament hypertrophy, with a consequent cervical spinal stenosis. On the other hand, MPS Type IV is characterized by early development of cervical instability, due to the accumulation of keratan sulfate (KS) and chondroitin-6-sulfate, that alter cartilage and bone development, as reported in Table 1 [25,44].
According to Horovitz et al., MRI studies have documented that a sagittal diameter of 13 mm may be associated with neurological symptoms or signs. Indeed, there may be dynamic spinal canal stenosis during flexion-extension excursions—without compression of the spinal cord in a neutral cervical position—since the antero-posterior diameter of the spinal cord is a few millimeters narrower than the canal itself [25].
With regards to the radiological study of MPSs, a plain radiograph in two projections is generally first accomplished to evaluate spinal involvement, followed by flexion-extension lateral radiographs. CT scans allow a more accurate characterization of bony changes and abnormality; it is nowadays considered as the gold standard to achieve a better characterization of the odontoid process and atlanto-axial articulation. Furthermore, MRI can be used to adequately assess the spinal cord’s involvement signs. Routine MRI assessment instead, and even flexion-extension dynamic MRI, can be used in the monitoring of spinal cord compression, spinal canal stenosis, and cervical myelopathy [2,34].
Somatosensory evoked potentials (SSEP) and motor evoked potentials (MEP) analysis seems helpful in patients’ follow-up to monitor the peri-operative neurological status in MPSs with signs of spinal cord compression [25].
Among all the available tools to detect spinal cord alterations, transcranial magnetic stimulation has proven to be useful in the evaluation of spinal cord disease, especially at the first stages of neural compression, as it may be deemed as a functional counterpart of neuroimaging, and an extension of clinical assessment [51,52].
To gain a better understanding of the main features of MPSs, here we focus on a study by Montaño et al., including 143 patients with MPS VII, that were diagnosed in 30 countries. Patients with more severe phenotypes had short stature and increased features of skeletal dysplasia. A total of 90% of patients with MPS VII presented with skeletal dysplasia such as vertebral breaking and hypoplastic odontoid process, with atlantoaxial instability. These patients have an increased risk of cervical dislocation, even from minor trauma or intubation maneuvers [53].
Another interesting case that was reported by Utsunomiya et al., has shown a child with MPS Type IVA that during the second year of enzyme replacement therapy (ERT) developed a compression of the spinal cord at the C1 level with a consequent instability of the atlantoaxial joint. Although fusion of the occipito-cervical spine with C1 posterior decompression is generally performed for patients with MPS Type IV A, decompression surgery was performed at first, and only later, fusion with instrumentation was performed because the bone structures were initially too small due to the young age of the patient [44]. This case has opened the demanding role of timing in the surgical treatment of these disorders, especially during ERT therapy. Indeed, after the first year of treatment, an improvement of posture has been evaluated leading to a late development of spinal stenosis that is probably related to a difficult capacity to reach bone tissues by the ERT agent.
The main role of surgery in these patients is to determine a neurological improvement, whenever feasible, and/or prevent further neurological impairment, ultimately allowing for a better quality of life. However, given the heterogeneity of the syndromic manifestations that are linked to different types of MPSs, a clear consensus regarding surgical indications is lacking.
As previously explained, one of the main causes of cervical myelopathy can be related to a narrow osseous neural canal due to dural thickening [9,54].
Indeed, the study by Ballenger et al. was the first study of Hunter syndrome complicated by cervical myelopathy due to thickened meninges which is also implicated in intracranial subarachnoid blockade of CSF, thus promoting communicating hydrocephalus. In this case, early cervical decompression was found to be promising for stabilization and improvement of myelopathic symptoms [9].
Nevertheless, preventive treatment in asymptomatic patients with neither clinical or radiologic evidence of myelopathy is still a matter of debate.
On considering the natural course of MPSs, prophylactic fusion of the cervical spine has been recommended to prevent cervical myelopathy. Early surgery is proven to obtain better neurological outcomes, preventing otherwise progressive neurological impairment [29]. As shown in Table 1, 90.04% of the patients reported a significant clinical improvement after surgery.
Upper cervical fusion is recommended when radiographic signs of progressive spinal instability and/or compression are present, even without neurologic impairment, to prevent spinal cord compression and improve neurologic outcome [29].
Dede et al. observed that plain radiographs in children that were affected by Morquio syndrome underestimated the real diameter of the spinal canal. In fact, due to the presence of an unossified odontoid tip and soft tissue GAGs deposition posterior to the odontoid, an MRI study of the cervical spine is essential in children with Morquio syndrome with neural changes and instability, highly suggestive of subsequent spinal cord compression. [29].
According to some authors, surgical preventive treatment should be recommended in all MPS IV (Morquio syndrome) patients with MRI evidence of CVJ stenosis and instability, with canal narrowing of >50% [38]. Moreover, clinical evidence of acute or progressive myelopathy due to spinal cord compression at the CVJ represents a clear surgical indication. First, surgical decompression could, therefore, lead to a neurological function improvement even in long-term follow-up [29,38].
Otherwise, patients with severe compression at CVJ may benefit from anterior transoral decompression and posterior fusion, as it could possibly give a better and prompter neurological recovery [11,55].
Laminoplasty can also be considered a safe and effective surgical procedure allowing for a better preservation of the cervical range of motion, thus preventing kyphotic transformation after surgery. Nevertheless, it cannot be performed in most pediatric patients due to the small dimension of the laminae, and when odontoid hypoplasia is highlighted [45].
Early decompression surgery for CVJ disease is often required in most young patients with MPS IV A Type (Morquio syndrome), when considering the aggressive natural history of the disease and high risk of acute neurologic deterioration [39].
In the literature, an interesting case of a child with MPS type IV A, affected by C3–C5 kyphotic deformity myelopathy has been documented. At first, the patient underwent conservative treatment with halo ring placement. Then, C3–C5 corpectomy was performed using a cranial bone graft between the bodies of C2 and C6, to gain anterior decompression. Finally, a halo-vest was applied.
Even the use of occipital bone grafts is reported in patients thata re affected by atlantoaxial instability to obtain further stabilization of the midcervical region [14].

5. Conclusions

The results of our systematic review confirm prior investigations, assessing that surgical decompression, performed with or without fusion, can be considered the most efficacious and safe surgical treatment. Above all, surgery should be considered in MPSs with neural compression from either atlanto-axial instability and soft tissue thickening in patients with clinical evidence of myelopathy and/or spinal cord compression.
The main limitation of this study concerns a selection bias since several studies regarding surgical strategies for MPSs have been excluded due to the lack of clinical data. Therefore, uniform data for pre- and post-operative clinical evaluation could not be fully extracted from all the selected studies.
Nevertheless, MPSs are rare genetic disorders that, due to the lack of clear guidelines and uniform data, require future studies and longitudinal pre- and post-operative exams for early diagnosis, accurate prognosis, and adequate surgical treatment.

Author Contributions

Conceptualization, R.C. and L.B. (Lapo Bonosi); methodology, L.B. (Lapo Bonosi) and M.P.; validation, R.C., L.B. (Lapo Bonosi), and F.P.; formal analysis, L.B. (Lara Brunasso); investigation, A.E.G. and M.P.S.; resources, G.S.; data curation, M.P. and F.P.; writing—original draft preparation, R.C.; writing—review and editing, R.C.; visualization, G.E.U.; supervision, G.E.U., G.R.G. and D.G.I.; project administration, D.G.I., R.M., and R.C. All authors have read and agreed to the published version of the manuscript.

Funding

This research received no external funding.

Institutional Review Board Statement

Not applicable.

Informed Consent Statement

Not applicable.

Data Availability Statement

Not applicable.

Conflicts of Interest

The authors declare no conflict of interest.

References

  1. Cimaz, R.; la Torre, F. Mucopolysaccharidoses. Curr. Rheumatol. Rep. 2014, 16, 1–9. [Google Scholar] [CrossRef] [PubMed]
  2. Crostelli, M.; Mazza, O.; Mariani, M.; Mascello, D.; Iorio, C. Spine challenges in mucopolysaccharidosis. Int. Orthop. 2019, 43, 159–167. [Google Scholar] [CrossRef] [PubMed]
  3. Kobayashi, H. Recent trends in mucopolysaccharidosis research. J. Hum. Genet. 2019, 64, 127–137. [Google Scholar] [CrossRef] [PubMed]
  4. Fecarotta, S.; Tarallo, A.; Damiano, C.; Minopoli, N.; Parenti, G. Pathogenesis of Mucopolysaccharidoses, an Update. Int. J. Mol. Sci. 2020, 21, 2515. [Google Scholar] [CrossRef] [Green Version]
  5. Sharma, N.; Nagpal, R.; Goyal, R.; Priyadarshini, K.; Kashyap, S.; Sharma, M.; Sinha, R. Mucopolysaccharidosis: A broad review. Indian J. Ophthalmol. 2022, 70, 2249–2261. [Google Scholar] [CrossRef]
  6. Kennedy, P.; Swash, M.; Dean, M.F. Cervical Cord Compression in Mucopolysaccharidosis. Dev. Med. Child. Neurol. 1973, 15, 194–199. [Google Scholar] [CrossRef]
  7. Paulson, G.W.; Meagher, J.N.; Burkhart, J. Spinal Pachymeningitis Secondary to Mucopolysaccharidosis Case Report. J. Neurosurg. 1974, 41, 68–621. [Google Scholar] [CrossRef]
  8. Peterson, D.I.; Bacchus, H.; Seaich, L.; Kelly, T.E. Myelopathy associated with Maroteaux-Lamy syndrome. Arch Neurol. 1975, 32, 127–129. [Google Scholar] [CrossRef]
  9. Ballenger, C.E.; Swift, T.R.; Leshner, R.T.; el Gammal, T.A.; Mcdonald, T.F. Mucopoly Saccharidosis Type II (Hunter Syndrome). Ann. Neurol. 1980, 7, 382–385. [Google Scholar] [CrossRef]
  10. Sanna, M.; Hollenberg, R. Compressive Meningeal Hypertrophy in Mucopolysaccharidosis. Am. J. Neuroradiol. 1987, 8, 385–386. [Google Scholar]
  11. Ashraf, J.; Alan Crockard, H.; Stevens, J.M. Transoral Decompression and Posterior Stabilisation in Morquio’s Disease. Arch. Dis. Child. 1991, 66, 1318–1321. [Google Scholar] [CrossRef] [PubMed]
  12. Stevens, J.M.; Kendall, B.E.; Crockard, H.A.; Ransford, A. The Odontoid Process in Morquio-Brailsford’s Disease the Effects of Occipitocervical Fusion. J. Bone Joint Surg. Br. 1991, 73, 851–858. [Google Scholar] [CrossRef] [PubMed]
  13. Northover, H.; Cowie, R.A.; Wraith, J.E. Mucopolysaccharidosis Type IVA (Morquio Syndrome): A Clinical Review. J. Inherit. Metab. Dis. 1996, 19, 357–365. [Google Scholar] [CrossRef]
  14. Piccirilli, C.B.; Chadduck, W.M.; Piccirilli, C.B.; Chadduck, W.M. Cervical Kyphotic Myelopathy in a Child with Morquio Syndrome. Childs Nerv. Syst. 1996, 12, 114–116. [Google Scholar] [CrossRef] [PubMed]
  15. O’Brien, D.P.; Cowie, R.A.; Wraith, J.E. Cervical decompression in Mild Mucopolysaccharidosis Type II (Hunter Syndrome). Childs Nerv. Syst. 1997, 13, 87–90. [Google Scholar] [CrossRef] [PubMed]
  16. Kachur, E.; del Maestro, R. Mucopolysaccharidoses and Spinal Cord Compression: Case Report and Review of the Literature with Implications of Bone Marrow Transplantation. Neurosurgery 2000, 47, 223–229. [Google Scholar] [CrossRef]
  17. Thorne, J.A.; Sn, F.R.C.S.; Javadpour, M.; Hughes, D.G.; Wraith, E.; Cowie, R.A. Craniovertebral Abnormalities in Type VI Mucopolysaccharidosis (Maroteaux-Lamy Syndrome). Neurosurgery 2001, 48, 849–853. [Google Scholar]
  18. Alam Khan, S.; Ortho, M.; Ortho Surg, D.; Sehat, K.; Eng, M.; Calthorpe, D.; Ortho, F.; Ch Orth, M. Cervical Cord Compression in an Elderly Patient with Hurler’s Syndrome: A Case Report. Spine 2003, 28, E313–E315. [Google Scholar] [CrossRef]
  19. Dickerman, R.D.; Colle, K.O.; Bruno, C.A.; Schneider, S.J. Craniovertebral Instability with Spinal Cord Compression in a 17-Month-Old Boy With Sly Syndrome (Mucopolysaccharidosis Type VII) A Surgical Dilemma. Spine 1976, 29, E92–E94. [Google Scholar] [CrossRef]
  20. Mut, M.; Cila, A.; Varli, K.; Akalan, N. Multilevel Myelopathy in Maroteaux-Lamy Syndrome and Review of the Literature. Clin. Neurol. Neurosurg. 2005, 107, 230–235. [Google Scholar] [CrossRef]
  21. Illsinger, S.; Lücke, T.; Hartmann, H.; Mengel, E.; Müller-Forell, W.; Donnerstag, F.; Das, A.M. Scheie Syndrome: Enzyme Replacement Therapy Does Not Prevent Progression of Cervical Myelopathy Due to Spinal Cord Compression. J. Inherit. Metab. Dis. 2009, 32, 321–325. [Google Scholar] [CrossRef] [PubMed]
  22. White, K.K.; Steinman, S.; Mubarak, S.J. Cervical Stenosis and Spastic Quadriparesis in Morquio Disease (MPS IV): A Case Report with Twenty-Six-Year Follow-Up. J. Bone Jt. Surg. 2009, 91, 438–442. [Google Scholar] [CrossRef] [PubMed]
  23. Giussani, C.; Roux, F.E.; Guerra, P.; Pirillo, D.; Grimaldi, M.; Citerio, G.; Sganzerla, E.P. Severely Symptomatic Craniovertebral Junction Abnormalities in Children: Long-Term Reliability of Aggressive Management. Pediatr. Neurosurg. 2009, 45, 29–36. [Google Scholar] [CrossRef] [PubMed]
  24. Houten, J.K.; Kinon, M.D.; Goodrich, J.T. Morquio’s Syndrome and Craniocervical Instability. Pediatr. Neurosurg. 2012, 47, 238–240. [Google Scholar] [CrossRef] [PubMed]
  25. Horovitz, D.D.G.; Magalhães, T.d.S.P.C.; Costa, A.P.; Carelli, L.E.; Silva, D.S.; de Linhares e Riello, A.P.F.; Llerena, J.C. Spinal Cord Compression in Young Children with Type VI Mucopolysaccharidosis. Mol. Genet. Metab. 2011, 104, 295–300. [Google Scholar] [CrossRef]
  26. Tchan, M.C.; Devine, K.T.; Sillence, D.O. Three Adult Siblings with Mucopolysaccharidosis Type II (Hunter Syndrome): A Report on Clinical Heterogeneity and 12 Months of Therapy with Idursulfase. J. Inherit. Metab. Dis. 2011, 1, 57–64. [Google Scholar] [CrossRef] [Green Version]
  27. Shukla, D.; Arvind, S.; Devi, B.I. Myelopathy in a Dwarf: A Case of Morquio’s Syndrome without Odontoid Hypoplasia. Neurol. India 2011, 59, 126–127. [Google Scholar] [CrossRef]
  28. Tong, C.K.W.; Chen, J.C.H.; Cochrane, D.D. Spinal Cord Infarction Remote from Maximal Compression in a Patient with Morquio Syndrome. J. Neurosurg. Pediatr. 2012, 9, 608–612. [Google Scholar] [CrossRef]
  29. Dede, O.; Thacker, M.M.; Rogers, K.J.; Oto, M.; Belthur, M.v.; Barátela, W.; Mackenzie, W.G. Upper Cervical Fusion in Children with Morquio Syndrome Intermediate to Long-Term Results. J. Bone Jt. Surg. 2013, 95, 1228–1234. [Google Scholar] [CrossRef]
  30. Möllmann, C.; Lampe, C.G.; Müller-Forell, W.; Scarpa, M.; Harmatz, P.; Schwarz, M.; Beck, M.; Lampe, C. Development of a scoring system to evaluate the severity of craniocervical spinal cord compression in patients with mucopolysaccharidosis iva (morquio a syndrome). In JIMD Reports; Springer: Berlin/Heidelberg, Germany, 2013; Volume 11, pp. 65–72. [Google Scholar]
  31. Lampe, C.; Lampe, C.; Schwarz, M.; Müller-Forell, W.; Harmatz, P.; Mengel, E. Craniocervical Decompression in Patients with Mucopolysaccharidosis VI: Development of a Scoring System to Determine Indication and Outcome of Surgery. J. Inherit. Metab. Dis. 2013, 36, 1005–1013. [Google Scholar] [CrossRef]
  32. Baratela, W.A.R.; Bober, M.B.; Thacker, M.M.; Belthur, M.v.; Oto, M.; Rogers, K.J.; Mackenzie, W.G. Cervicothoracic Myelopathy in Children with Morquio Syndrome A: A Report of 4 Cases. J. Pediatr. Orthop. 2013, 34, 223–228. [Google Scholar] [CrossRef] [PubMed]
  33. Vanek, P.; Homolkova, H.; Benes, V.; Zeman, J. Occipitocervical Stabilization Using Bilateral Laminar C2 Screws in Children with Mucopolysaccharidosis IVA. Eur. Spine J. 2015, 24, 2756–2762. [Google Scholar] [CrossRef] [PubMed]
  34. Solanki, G.A.; Sun, P.P.; Martin, K.W.; Hendriksz, C.J.; Lampe, C.; Guffon, N.; Hung, A.; Sisic, Z.; Shediac, R.; Harmatz, P.R. Cervical Cord Compression in Mucopolysaccharidosis VI (MPS VI): Findings from the MPS VI Clinical Surveillance Program (CSP). Mol. Genet. Metab. 2016, 118, 310–318. [Google Scholar] [CrossRef] [PubMed]
  35. Eisengart, J.B.; Jarnes, J.; Ahmed, A.; Nestrasil, I.; Ziegler, R.; Delaney, K.; Shapiro, E.; Whitley, C. Long-Term Cognitive and Somatic Outcomes of Enzyme Replacement Therapy in Untransplanted Hurler Syndrome. Mol. Genet. Metab. Rep. 2017, 13, 64–68. [Google Scholar] [CrossRef] [PubMed]
  36. Vazifehdan, F.; Karantzoulis, V.G.; Ebner, R.; Igoumenou, V.G. A Unique Case of Cervical Myelopathy in an Adult Patient with Scheie Syndrome. J. Orthop. Case Rep. 2017, 7, 27–30. [Google Scholar] [CrossRef] [PubMed]
  37. Broomfield, A.; Zuberi, K.; Mercer, J.; Moss, G.; Finnegan, N.; Hensman, P.; Walker, R.; Bukhari, S.; Wright, N.B.; Stewart, F.; et al. Outcomes from 18 Years of Cervical Spine Surgery in MPS IVA: A Single Centre’s Experience. Child’s Nerv. Syst. 2018, 34, 1705–1716. [Google Scholar] [CrossRef]
  38. Giussani, C.; Guida, L.; Canonico, F.; Sganzerla, E.P. Cerebral and Occipito-Atlanto-Axial Involvement in Mucopolysaccharidosis Patients: Clinical, Radiological, and Neurosurgical Features 11 Medical and Health Sciences 1103 Clinical Sciences 11 Medical and Health Sciences 1109 Neurosciences. Ital. J. Pediatr. 2018, 44, 119. [Google Scholar] [CrossRef] [Green Version]
  39. Williams, N.; Narducci, A.; Eastwood, D.M.; Cleary, M.; Thompson, D. An Evidence-Based Approach to the Management of Children with Morquio a Syndrome Presenting with Craniocervical Pathology. Spine 2018, 43, E1443–E1453. [Google Scholar] [CrossRef]
  40. Krenzlin, H.; Ta-Chih, T.; Lampe, C.; Lampe, C.; Knuf, M.; Horn, P.; Schwarz, M. Stand-Alone Craniocervical Decompression Is Feasible in Children with Mucopolysaccharidosis Type I, IVA, and VI. Spine J. 2018, 18, 1455–1459. [Google Scholar] [CrossRef]
  41. Okumura, R.; Hasegawa, K.; Tsuge, S.; Fukutake, K.; Nakamura, K.; Takahashi, H.; Wada, A. Adult Morquio Syndrome Requiring Occipito-Thoracic Fusion. J. Orthop. Surg. 2020, 28, 2309499020918424. [Google Scholar] [CrossRef]
  42. Kiessling, P.; Stans, A.A.; Dearani, J.A.; Boesch, R.P.; Fogelson, J.L.; Matsumoto, J.M.; Haile, D.T.; Balakrishnan, K. Coordinated Approach to Spinal and Tracheal Reconstruction in a Patient with Morquio Syndrome. Int. J. Pediatr. Otorhinolaryngol. 2020, 128, 109721. [Google Scholar] [CrossRef] [PubMed]
  43. Moon, E.J.; Lee, S.; Chong, S.; Park, J.H. Atlantoaxial Instability Treated with Free-Hand C1–C2 Fusion in a Child with Morquio Syndrome. Child’s Nerv. Syst. 2020, 36, 1785–1789. [Google Scholar] [CrossRef] [PubMed]
  44. Nakamura-Utsunomiya, A.; Nakamae, T.; Kagawa, R.; Karakawa, S.; Sakata, S.; Sakura, F.; Tani, C.; Matsubara, Y.; Ishino, T.; Tajima, G.; et al. A Case Report of a Japanese Boy with Morquio a Syndrome: Effects of Enzyme Replacement Therapy Initiated at the Age of 24 Months. Int. J. Mol. Sci. 2020, 21, 989. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  45. Terai, H.; Tamai, K.; Hoshino, M.; Toyoda, H.; Suzuki, A.; Takahashi, S.; Hori, Y.; Yabu, A.; Nakamura, H. Clinical Outcomes of Laminoplasty for Patients with Lysosomal Storage Disease Including Mucopolysaccharidosis and Mucolipidoses: A Retrospective Cohort Study. Orphanet. J. Rare Dis. 2021, 16, 1–10. [Google Scholar] [CrossRef]
  46. Demartini, Z.; Munhoz da Rocha Guimaraes, R.; Cardoso-Demartini, A.A. Cervical Disorders in Mucopolysaccharidosis IVA—Morquio Disease. World Neurosurg. 2021, 153, 41–43. [Google Scholar] [CrossRef]
  47. Stapleton, M.; Arunkumar, N.; Kubaski, F.; Mason, R.W.; Tadao, O.; Tomatsu, S. Clinical presentation and diagnosis of mucopolysaccharidoses. Mol. Genet. Metab. 2018, 125, 4–17. [Google Scholar] [CrossRef]
  48. Ferrante, A.; Ciccia, F.; Giammalva, G.R.; Iacopino, D.G.; Visocchi, M.; Macaluso, F.; Maugeri, R. The Craniovertebral Junction in Rheumatoid Arthritis: State of the Art. Acta Neurochir. Suppl. 2019, 125, 79–86. [Google Scholar] [CrossRef]
  49. Gerardi, R.M.; Giammalva, G.R.; Basile, L.; Gulì, C.; Pino, M.A.; Messina, D.; Umana, G.E.; Graziano, F.; di Bonaventura, R.; Sturiale, C.L.; et al. White Cord Syndrome After Cervical or Thoracic Spinal Cord Decompression. Hemodynamic Complication or Mechanical Damage? An Underestimated Nosographic Entity. World Neurosurg. 2022, 164, 243–250. [Google Scholar] [CrossRef]
  50. Giammalva, G.R.; Maugeri, R.; Graziano, F.; Gulì, C.; Giugno, A.; Basile, L.; Iacopino, D.G. White Cord Syndrome after Non-Contiguous Double-Level Anterior Cervical Decompression and Fusion (ACDF): A “No Reflow Phenomenon”? Interdiscip. Neurosurg. 2017, 7, 47–49. [Google Scholar] [CrossRef]
  51. Cantone, M.; Lanza, G.; Le Pira, A.; Barone, R.; Pennisi, G.; Bella, R.; Pennisi, M.; Fiumara, A. Adjunct diagnostic value of transcranial magnetic stimulation in mucopolysaccharidosis-related cervical myelopathy: A pilot study. Brain Sci. 2019, 9, 200. [Google Scholar] [CrossRef] [Green Version]
  52. Costanzo, R.; Brunasso, L.; Paolini, F.; Benigno, U.E.; Porzio, M.; Giammalva, G.R.; Gerardi, R.M.; Umana, G.E.; di Bonaventura, R.; Sturiale, C.L.; et al. Spinal Tractography as a Potential Prognostic Tool in Spinal Cord Injury: A Systematic Review. World Neurosurg. 2022, 164, 25–32. [Google Scholar] [CrossRef] [PubMed]
  53. Montaño, A.M.; Lock-Hock, N.; Steiner, R.D.; Graham, B.H.; Szlago, M.; Greenstein, R.; Pineda, M.; Gonzalez-Meneses, A.; Çoker, M.; Bartholomew, D.; et al. Clinical course of sly syndrome (mucopolysaccharidosis type VII). J. Med. Genet. 2016, 53, 403–418. [Google Scholar] [CrossRef] [PubMed]
  54. Vinchon, M.; Cotten, A.; Clarisse, J.; Chiki, R.; Christiaens, J.L. Cervical Myelopathy Secondary to Hunter Syndrome in an Adult. Am. J. Neuroradiol. 1995, 16, 1402–1403. [Google Scholar]
  55. Giammalva, G.R.; Iacopino, D.G.; Graziano, F.; Giugno, A.; Gulì, C.; Basile, L.; Visocchi, M.; Maugeri, R. Surgical highways to the craniovertebral junction: Is it time for a reappraisal? In New Trends in Craniovertebral Junction Surgery; Acta Neurochirurgica Supplement; Visocchi, M., Ed.; Springer: Berlin/Heidelberg, Germany, 2019; Volume 125. [Google Scholar] [CrossRef]
Brainsci 13 00048 g001 550
Figure 1. PRISMA flow diagram.
Figure 1. PRISMA flow diagram.
Brainsci 13 00048 g001
Brainsci 13 00048 g002 550
Figure 2. Rate of MPS type that is associated to cervical myelopathy (Other: one patient has an intermediate phenotype V/VI).
Figure 2. Rate of MPS type that is associated to cervical myelopathy (Other: one patient has an intermediate phenotype V/VI).
Brainsci 13 00048 g002
Brainsci 13 00048 g003 550
Figure 3. The purple line (*) shows the rate of patients that were affected by spinal cord compression related to the cervical levels, with a clear prevalence of the cranio-vertebral junction (C0–C2).
Figure 3. The purple line (*) shows the rate of patients that were affected by spinal cord compression related to the cervical levels, with a clear prevalence of the cranio-vertebral junction (C0–C2).
Brainsci 13 00048 g003
Table
Table 1. Demographic and clinical data from our studies’ selection.
Table 1. Demographic and clinical data from our studies’ selection.
1AuthorCountryStudy DesignN of PatientsMFMean AgeMPS TypeLevel of Spine PathologyAethiology of MyelopathySurgical TreatmentAEsAdditional TreatmentClinical OutcomesFollow Up Time after Surgery (Months)
1973P Kennedy [6]EnglandCase Report10116V/VIC1–C2Ligamentum flavum hypertrophy & dura mater thickeningC1–C5 laminectomyCSF leak; pseudo-myelomeningocele; then AVD-neurological improvement, regain walking(seems long-term)
1974W.G. Paulson [7]USACase Report10155I SC1–C6Ligamentum flavum hypertrophy & dura mater thickening & severe stenosisC1–C6 laminectomyTransient CSF leakage-neurological improvement/
1975D I Peterson [8]California USACase Report10123VIC1–C3Ligamentum flavum hypertrophy & dura mater thickeningC1–C5 laminectomy--neurological improvement, regain walking, and regain continence(seems long-term)
1980C E Ballenger [9]Georgia USACase Report11024II BC2ligamentum flavum hypertrophy & dura mater thickeningC1–C7 laminectomy--neurological improvement, re-gain walking and strengthN/A
1987M Sanna [10]Saudi Arabia/CanadaCase Report10116VIC1–C3Ligamentum flavum hypertrophy & dura mater thickeningC1–C3 laminectomy--neurological improvement/
1991J Ashraf [11]EnglandCase Report1103.5IVC1–C2Atlanto-axial instability, dura mater thickeningtransoral odontoidectomy; posterior decompression and fixation C0–C2-Preop halo traction neurological improvement, re-gain walking and strength/
1991J M Stevens [12]EnglandCase Series8539.7IVC1–C2Odontoid dysplasia, atlanto-axial instabilityCCJ decompression-2 pt: redolimited neurological improvementup to 120 m
1996H Northover [13]NetherlandsClinical Review22N/AN/A1.5IVC1–C2Odontoid dysplasia, ligamentum flavum hypertrophy & dura mater thickeningCCJ decompression and fusion-2 pt: fixation redo-(seems long-term)
1996C B Piccirilli [14]Michigan USACase Report1104.5IVC3–C5Cervical kyphosis with stenosisanterior corpectomy C3–C5, PLL removal, fixation with autologue graft-Preop halo traction neurological improvement-
1997D P O’Brien [15]EnglandCase Report33016.33IIC0–C2Odontoid dysplasia, ligamentum flavum hypertrophy & dura mater thickeningforamen magnum decompression, C1–C6 laminectomy1 pt: wound infection
1 pt: CSF leakage		-neurological improvement-
2000E Kachur [16]CanadaCase Report1018I HC1–C4Ligamentum flavum hypertrophy & dura mater thickeningC1–C5 laminectomy, foramen magnum decompression--neurological improvement24 m
2001J A Thorne [17] EnglandCase Series42212VI1 pt: C1–C3
1 pt: C0–C3
1 pt: C1–C3
1 pt: C0–C4		Ligamentum flavum hypertrophy & dura mater thickeningUpper cercival decompression and fusion1 pt: CSF and wound infection3 pt: Preop halo tractionneurological improvement36 m
2003S A Khan [18]EnglandCase Report10159I HC3–C5Ligamentum flavum hypertrophy & dura mater thickeningC2–C4 laminectomy and fixation--neurological improvement, pain reduction96 m
2004R D Dickerman [19] New York USACase Report1101.41VIIC0–C2Atlanto-axial instability, ligamentum flavum hypertrophy & dura mater thickeningC1–C3 laminectomy, foramen magnum decompression and fusion with autologue graft-Post-op halo vestneurological improvement-
2005M Mut [20]TurkeyCase Report1102VIC0–C4Ligamentum flavum hypertrophy & dura mater thickeningForamen magnum decompression and C1 laminectomy After years, restenosis: C2–C4 laminectomyneurological improvement-
2009S Illsinger [21]GermanyCase Report10126I SC2Ligamentum flavum hypertrophy & dura mater thickeningC2 laminectomy -ERT therapyneurological improvement-
2009K K White [22]California USACase Report11010IVC1–C2Odontoid dysplasia, atlanto-axial instabilityC1 laminectomy and fusion with autologue graft-Post-op halo vestneurological improvement312 m
2009C Giussani [23]ItalyCase Report1016IVC0–C2Odontoid dysplasia, atlantoaxial instabilityC1–C2 decompression, C0–C2 fixation--neurological improvement36 m
2011J K Houten [24]N.Y. USACase Report10117IVC1–C2Atlanto-axial instability, dura mater thickeningC1–C4 laminectomy, foramen magnum decompression and fusion--neurological improvement10 m
2011D D G Horovitz [25]BrazilCase Report3125.26 VIC0–C2Atlanto-axial instability, OPLLCervical decompression and fixation-3 pt: ERT2 pt: neurological improvement
1 pt: neurological improvement and continence improvement 		24 m
2011M C Tchan [26]AustraliaCase Report33043.33II1 pt: C2–C3
1 pt: C2–C4
1 pt: C2–C4		Ligamentum flavum hypertrophy & dura mater thickeningCervical decompression -idursulfase therapy 1,2: neurological improvement; 3: clinically stable64 m
2011D Shukla [27]IndiaCase Report10120IVC0–C2Ligamentum flavum hypertrophy & dura mater thickeningForamen magnum decompression, C1–C2 decompression--neurological improvement10 m
2012CKV Tong [28]CanadaCase Report10116IVC0–C3Odontoid dysplasia, atlantoaxial instability, severe stenosis C1 decompression--neurological deterioration12 m
2013O Dede [29]Delaware USACase serie20N/AN/A5.25IV5 pt: C1–C2
1 pt: C0–C3
14 pt: C0–C2		Atlanto-axial instabilityCCJ decompression +
5 pt: C1–C2 fusion;
1 pt: occipito-C3 fusion;
14 pt: occipito-C2 fusion		 Postop halo vest.
1 pt fixation exstention to c1;
3 pt fixation exstention to c4;
2 fixation exstention to c5		neurological improvement106 m
2013C Möllmann [30]GermanyRetrospective 12N/AN/A7.9IVC0–C2Atlanto-axial instability, ligamentum flavum hypertrophy & dura mater thickening3 pt: foramen magnum and C1–C3
decompression and fixation;
9 pt: foramen magnum and C1–C3 decompression		--neurological improvement/
2013C Lampe [31]GermanyRetrospective 14N/AN/A15VIC0–C2Atlanto-axial instability, ligamentum flavum hypertrophy & dura mater thickeningForamen magnum and C1–C5 decompression--neurological improvement in 46%; no neurological changes in 54%10 m
2014W. A.R. Baratela [32]Delaware USACase report3126.83IV1 pt: C7–T1,
1 pt: C7–T1,
1 pt: C7–T2		Cervical kyphosis with stenosis1 pt: C7–T1 laminectomy and C5–T2 fusion;
1 pt: T1–T2 laminectomy, C7–T4 fixation;
1 pt: C7–T2 laminectomy, C6–T2 fusion.		 Postop halo vest;
1 pt: after 12 years, decompression and fusion T2–T7;
1 pt: redo with C2–C4 laminectomy and posterior C2–C5 fusion		neurological improvement144 m
2015P Vanek [33]Czech RepublicCase report43112IVC0–C2Atlanto-axial instability, ligamentum flavum hypertrophy & dura mater thickeningC0–C2 decompression1 pt: deiscence-neurological improvement36 m
2016G A Solanki [34]California USARetrospective 58273113.05VIC0–C2Odontoid dysplasia, ligamentum flavum hypertrophy & dura mater thickening;
7 pt also atlo-axial instability		51 pt: CCJ decompression;
7 pt: CCJ decompression and fusion		1 pt: meningitis;
2 pt: deaths anesthaesia related		8 pt: redo due to restenosisneurological improvement55.6 m
2017J B Eisengart [35]Minnesota USACase report1018I HC1–C7Ligamentum flavum hypertrophy & dura mater thickeningC1 laminectomy and C2–C7 laminoplasty-after 4 y: (progression with C1–C2 stenosis) CCJ decompression1 pt: neurological improvement, re-gain walking and coordination
1 pt: neurological improvement, pain reduction		72 m
2017F Vazifehdan [36]GreeceCase report11033I SC2–C5Ligamentum flavum hypertrophy & dura mater thickeningLaminectomy C2–C6 and fixation C1–C2–C7-After 6 months and return to sports and failure C7 screws: redo with C1–C2–C5–T1–T2 fixationneurological improvement24 m
2018A. Broomfield [37]GermanyRetrospective 26N/AN/A6.48IV18 pt: C1–C2;
3 pt: N/A;
1 pt: C1;
5 pt: C2–C3		Atlanto-axial instability, ligamentum flavum hypertrophy & dura mater thickening19 pt: fusion;
7 pt: decompression and bone graft		2 pt: bone graft failure;
1 pt:CSF leakage		8 pt: ERT;
each patient had halo vest post-op		5 pt: worsening;
the others: neurological improvement		84 m
2018M Crostelli [2]ItalyReview1014.6I HC0–C2Ligamentum flavum hypertrophy & dura mater thickeningOccipital-C2 decompression and fixation--neurological improvement132 m
2018C Giussani [38]ItalyReview3214.66IVA, VI, IVC0–C1Ligamentum flavum hypertrophy & dura mater thickeningOccipito-C2 decompression and fusion-1 pt: Preop halo vest1 pt: neurological improvement
1 pt: neurological improvement and bladder continence improvement		24 m
2018N Williams [39]EnglandReview181625.8IVC0–C3Odontoid dysplasia, atlanto-axial instability, ligamentum flavum hypertrophy & dura mater thickeningCCJ decompression and fusion-6 ERT7 neurological improvementi; 4 complete neurological restoration; 3 clinically stable; 3 worsened; 1 not identified102 m
2018H Krenzlin [40]GermanyReview157810.85 IH, 5 IVA, 5 VIC1–C2Ligamentum flavum hypertrophy & dura mater thickeningC1–C2 laminectomy2 tracheostomies9 pt: reoperation due to restenosisneurological improvement/
2020R Okumura [41]JapanCase Report11054IVC1–C2C1 hypoplasy, atlanto-axial instabilityCCJ decompression, occipito-C2–C4–C5–T1–T2–T3 fixation--neurological improvement24 m
2020P Kiessling [42]Minnesota USACase Report11017IVC7–T2Cervical kyphosis with stenosisPCF decompression, C6–T2 laminectomy, occipito-T7 fixation-Preop and postop halo vestneurological improvement17 m
2020E Moon [43]GermanyCase Report1103IVC1–C2Atlanto-axial instability, dura mater thickening C1–C2 laminectomy and fixation--neurological improvement, re-gain walking and strength8 m
2020A Nakamura-Utsunomiya [44]JapanCase Report1103IVC1Atlanto-axial instability, ligamentum flavum hypertrophy & dura mater thickeningCCJ decompression-ERTneurological improvement, re-gain walking and strength12 m
2021H Terai [45]JapanCase Report65127.51 pt: I
3 pt: II
1 pt: III
1 pt:VI		1 pt: C3–C4;
5 pt: C1		OPLLC1 laminectomy and cervical laminoplasty-4 ERTneurological improvement, re-gain walking and strength61 m
2021Z Demartini Jr. [46]BrazilCase Report11027IVC7–T1Odontoid dysplasia, atlanto-axial instability, kyphosis with severe stenosisCCJ decompression and fixationdied for tracheal stenosis-neurological improvement, re-gain walking and strength-
M-male, F-female. MPS type: Mucopolysaccharidosis type, AEs: adverse events; CSF leak: cerebrospinal fluid leak; AVD should become VAS: ventriculoatrial shunt; N/A not available; CCJ cranio-cervical junction; PLL posterior longitudinal ligament; ERT: enzyme replacement therapy; PCF posterior cervical decompression and fusion.
Table
Table 2. Main cervical level that was involved for each type of mucopolysaccharidosis.
Table 2. Main cervical level that was involved for each type of mucopolysaccharidosis.
N TotMain Level Involved%n
I13C284.6111
II10C270.007
III1C3–C4100.00119
IV132C290.15119
VI88C1100.0088
VII2C1100.002
Disclaimer/Publisher’s Note: The statements, opinions and data contained in all publications are solely those of the individual author(s) and contributor(s) and not of MDPI and/or the editor(s). MDPI and/or the editor(s) disclaim responsibility for any injury to people or property resulting from any ideas, methods, instructions or products referred to in the content.

Share and Cite

MDPI and ACS Style

Costanzo, R.; Bonosi, L.; Porzio, M.; Paolini, F.; Brunasso, L.; Giovannini, A.E.; Silven, M.P.; Giammalva, G.R.; Umana, G.E.; Scalia, G.; et al. Burden of Surgical Treatment for the Management of Cervical Myelopathy in Mucopolysaccharidoses: A Systematic Review. Brain Sci. 2023, 13, 48. https://doi.org/10.3390/brainsci13010048

AMA Style

Costanzo R, Bonosi L, Porzio M, Paolini F, Brunasso L, Giovannini AE, Silven MP, Giammalva GR, Umana GE, Scalia G, et al. Burden of Surgical Treatment for the Management of Cervical Myelopathy in Mucopolysaccharidoses: A Systematic Review. Brain Sciences. 2023; 13(1):48. https://doi.org/10.3390/brainsci13010048

Chicago/Turabian Style

Costanzo, Roberta, Lapo Bonosi, Massimiliano Porzio, Federica Paolini, Lara Brunasso, Andrea Evier Giovannini, Manikon Poullay Silven, Giuseppe Roberto Giammalva, Giuseppe Emmanuele Umana, Gianluca Scalia, and et al. 2023. "Burden of Surgical Treatment for the Management of Cervical Myelopathy in Mucopolysaccharidoses: A Systematic Review" Brain Sciences 13, no. 1: 48. https://doi.org/10.3390/brainsci13010048

Note that from the first issue of 2016, this journal uses article numbers instead of page numbers. See further details here.

Article Metrics

Back to TopTop