Sultan Qaboos University Med J, August 2015, Vol. 15, Iss. 3, pp. e364–369, Epub. 24 Aug 15. doi: 10.18295/squmj.2015.15.03.010.
Submitted 19 Nov 14
Revisions Req. 15 Dec 14 & 24 Mar 15; Revisions Recd. 20 Jan & 31 Mar 15
Accepted 9 Apr 15

Departments of 1Child Health, 2Radiology & Molecular Imaging, 3Pathology and 4Genetics, Sultan Qaboos University Hospital, Muscat, Oman
Corresponding Author e-mails: koul@squ.edu.om and roshankoul@hotmail.com

متالزمة تصلب العمود الفقري لدى األطفال يف سلطنة عمان
رو�سان كول، دليب �سانكالة، �سعاد اجله�سمية، رجنيت ماين، رنا عبد الرحيم، �سيف اليعربي، ح�سني الكندي، خالد الذهلي، اآمنة الفطي�سية

abstract: Objectives: Rigidity of the spine is common in adults but is rarely observed in children. The aim 
of this study was to report on rigid spine syndrome (RSS) among children in Oman. Methods: Data on children 
diagnosed with RSS were collected consecutively at presentation between 1996 and 2014 at the Sultan Qaboos 
University Hospital (SQUH) in Muscat, Oman. A diagnosis of RSS was based on the patient’s history, clinical 
examination, biochemical investigations, electrophysiological findings, neuro-imaging and muscle biopsy. Atrophy 
of the paraspinal muscles, particularly the erector spinae, was the diagnostic feature; this was noted using magnetic 
resonance imaging of the spine. Children with disease onset in the paraspinal muscles were labelled as having 
primary RSS or rigid spinal muscular dystrophy. Secondary RSS was classified as RSS due to the late involvement 
of other muscle diseases. Results: Over the 18-year period, 12 children were included in the study, with a male-
to-female ratio of 9:3. A total of 10 children were found to have primary RSS or rigid spinal muscular dystrophy 
syndrome while two had secondary RSS. Onset of the disease ranged from birth to 18 months of age. A family 
history was noted, with two siblings from one family and three siblings from another (n = 5). On examination, 
children with primary RSS had typical features of severe spine rigidity at onset, with the rest of the neurological 
examination being normal. Conclusion: RSS is a rare disease with only 12 reported cases found at SQUH during 
the study period. Cases of primary RSS should be differentiated from the secondary type.

Keywords: Rigid Spine Syndrome; Rigid Spine Muscular Dystrophy; Selenoprotein; Children; Magnetic Resonance 
Imaging; Oman.

امللخ�ص: الهدف: ت�سلب العمود الفقري مر�س �سائع لدى الكبار و لكنه نادر احلدوث عند الأطفال. الهدف من هذه الدرا�سة هو اكت�ساف 
حالت ت�سلب العمود الفقري لدى الأطفال العمانيني. الطريقة: مت ا�ستخراج املعلومات عن الأطفال الذين مت ت�سخي�سهم مبتالزمة ت�سلب 
ت�سلب  متالزمة  ت�سخي�س  مت  عمان.  �سلطنة  مب�سقط،  قابو�س  ال�سلطان  جامعة  م�ست�سفى  يف   2014 و   1996 بني  الفرتة  يف  الفقري  العمود 
العمود الفقري اعتمادا على التاريخ املر�سي، و الفح�س ال�رسيري، و الفحو�سات الألكرتوف�سيولوجية، و �سور الأ�سعة و حتليل عينة من 
الع�سلة. ما مييز هذه املتالزمة هو وجود �سمور يف الع�سلة املحيطة بالنخاع بالتحديد وهو ما ميكن ت�سخي�سه عن طريق اأ�سعة الرنني 
املغناطي�سي للعمود الفقري. و�سفت اإ�سابات الأطفال باأولية او ثانوية بناءا على الع�سلة امل�سابة اأول. النتائج: خالل فرتة 18 �سنة، مت 
ت�سخي�س 12 طفال مبتالزمة ت�سلب العمود الفقري، بن�سبة الذكور اإىل الإناث 9 اإىل 3. مت ت�سخي�س متالزمة ت�سلب العمود الفقري الأويل يف 
10 من الأطفال اأما الثنان املتبقيان فتم ت�سخي�سهم مبتالزمة ت�سلب العمود الفقري الثانوي. مت مالحظة اأن اأعرا�س املر�س تبداأ عادة يف 
الفرتة ما بني الولدة و حتى عمر 18 �سهرا. كان هناك تاريخ عائلي للمر�س يف حالتني من الأطفال امل�سابني. الفح�س ال�رسيري اأو�سح 
اأن الأطفال امل�سابني مبتالزمة ت�سلب العمود الفقري الأويل لديهم ت�سلب �سديد يف ع�سالت العمود الفقري. اأما بقية فحو�سات الأع�ساب 
ال�رسيرية فكانت �سليمة. اخلال�صة: متالزمة ت�سلب العمود الفقري مر�س نادر احلدوث، و قد مت ت�سجيل 12 حالة فقط يف م�ست�سفى جامعة 

ال�سلطان قابو�س خالل فرتة الدرا�سة.
الكلمات املفتاحية: متالزمة ت�سلب العمود الفقري؛ ت�سلب العمود الفقري احلثلي؛ �سلينوبروتني؛ الأطفال؛ اأ�سعة الرنني املغناطي�سي؛ عمان.

Rigid Spine Syndrome among Children in Oman
*Roshan Koul,1 Dilip Sankhla,2 Suad Al-Jahdhami,3 Renjith Mani,1 Rana A. Rahim,1 Saif Al-Yaarubi,1 

Hussein Al-Kindy,1 Khalid Al-Thihli,4 Amna Al-Futaisi1

clinical & basic research

Advances in Knowledge
- Rigid spine syndrome (RSS) is common in adults but is infrequently seen among children. This study presents a large series of paediatric 

patients with this rare condition in Oman.

Application to Patient Care
- The results of this study support the implementation of support groups and family counselling services for the parents and guardians of 

children suffering from RSS in Oman. 
- Genetic tests were available for only three patients during the study period. The development of genetic testing facilities in Oman is 

recommended for diagnosing this condition among those with a family history of RSS.
- Paediatricians and physicians should learn to recognise this rare entity, particularly as diagnosed RSS patients will require 

multidisciplinary care.



Roshan Koul, Dilip Sankhla, Suad Al-Jahdhami, Renjith Mani, Rana A. Rahim, Saif Al-Yaarubi, Hussein Al-Kindy, 
Khalid Al-Thihli and Amna Al-Futaisi

Clinical and Basic Research | e365

Rigidity or stiffness of the spine is common in adults and among the elderly but is rarely seen in children.1,2 In adults, 
the disease mainly results in a bent spine (forward 
bending), often with a bent or drooping head. In 
children, while the spine may also be bent, the head 
remains upright and the neck becomes so stiff that 
the child cannot look to the ground. Differences have 
been noted between the underlying aetiopathology of 
a rigid spine in children and adults, although the usual 
causes are bone, neuromuscular and brain disorders.3,4 
Inheritance patterns also differ between adults and 
children as the condition is generally autosomal 
dominant in the former and recessive in the latter.5 
The disease presents between the 4–6th decade of life 
for adults and during the first decade for children.5 
For adults, this condition is known as axial myopathy, 
camptocormia, rigid spine syndrome (RSS) and, more 
recently, paraspinal neuromuscular syndrome.4,6,7 

Rigidity of the spine is noted in the late stages 
of several childhood muscular dystrophies and 
myopathies. In these diseases, the rigid spine is due 
to the spread of the disease to the muscles and the late 
involvement of the paraspinal muscles.5 This is known 
as secondary RSS; a specific muscle disease is usually 
the underlying cause. Rigid spinal muscular dystrophy 
syndrome (primary RSS) develops when the onset of 
the disease occurs in the paraspinal muscles and then 
spreads to the other muscles of the body.5,8 In the 
primary form of RSS, the muscle disease is often of 
non-specific origin or is due to congenital myopathies 
such as multicore disease or desmin-related myopathy 
with Mallory body-like inclusions. In these cases, the 
disease originates outside the dystrophin, glycoprotein 
or extracellular matrix.9 The muscle histopathology is 
therefore non-specific as the myopathy changes with 
fibro-fatty accumulation.10–12 The diagnosis of RSS is 
based on the clinical course of the illness as well as 
biochemical, electrophysiological, histopathological, 
genetic and radiological findings. 

In cases of primary RSS, a magnetic resonance 
imaging (MRI) scan of the spine will reveal atrophy 
of the paraspinal muscles, particularly the erector 
spinae.13 Selenoprotein dysfunction has been 
recognised as the main defect in the muscles 
of children with primary RSS; mutations in the 
selenoprotein N1 (SEPN1) gene-related myopathy were 
found to be associated with this disease and primary 
RSS was mapped to the 1p35–36 chromosome in 
four siblings.9,13 This study aimed to report on the 
characteristics of RSS among children in Oman.

Methods

Children diagnosed with RSS were enrolled in the 
study consecutively at presentation between 1996 
and 2014 at the Sultan Qaboos University Hospital 
(SQUH) in Muscat, Oman. After their initial 
presentation, the children were followed over the 
study period. Children were suspected of having RSS 
if there was restricted neck movement and bending of 
the spine.

A diagnosis of RSS was based on the following 
clinical features: an inability to look down due to 
limited neck movement; restriction of overall spine 
mobility and normal limb strength which did not 
affect day-to-day activities; no difficulty in swallowing, 
breathing or speaking; and no bone or joint 
involvement. Results from biochemical tests, imaging 
and muscle biopsies, as well as electrophysiological 
findings, were also used to make a diagnosis. Genetic 
tests were available for only three patients during the 
study period. These children did not have features 
of other dystrophinopathies so associated tests were  
not performed.

Formal consent for inclusion in this study was 
obtained from the parents or guardians of the children. 
This study was approved by the Medical Research & 
Ethics Committee at the College of Medicine & Health 
Sciences of Sultan Qaboos University (MREC#675).

Results

A total of 12 children with RSS presented to SQUH 
over the 18-year study period. Seven of these children 
had been previously reported in a case series.5 The 
estimated prevalence of RSS in Oman was therefore 
one per 170,000 of the general population or six 
per one million, based on a national population of 
approximately two million.14 There were nine male 
and three female patients. Onset of the disease ranged 
from birth to 18 months old (mean age: eight months 
and five days), although the parents of one child could 
not remember the exact time of disease onset. Seven 
of the children (58.3%) had delayed gross motor skill 
development; the remaining five patients (41.7%) had 
normal milestones. A family history was noted, with 
two siblings from one family and three siblings from 
another (n = 5). The remainder of the patient group 
were single cases (n = 7). 

A total of 10 children were found to have 
primary RSS (83.3%) while the remaining two had 
the secondary form of the disease (16.7%). Muscle 
biopsies were performed in 41.7% of the children 



Rigid Spine Syndrome among Children in Oman

e366 | SQU Medical Journal, August 2015, Volume 15, Issue 3

(three patients with primary RSS and two with 
secondary RSS). Histopathological findings were 
available for five patients (three with primary RSS 
and two with secondary RSS) and genetic information 
was available for two children with primary RSS and 
one with secondary RSS. One child with primary RSS 

was previously diagnosed with stiff person syndrome. 
A summary of the clinical and imaging features of all 
patients is available in Table 1.

On examination, the children with primary RSS 
had typical features of severe spine rigidity although 
their other neurological findings were normal. Gowers’ 

Table 1: Clinical, laboratory and imaging features of children diagnosed with rigid spine syndrome (N = 12)

Disease 
type

Age at 
onset in 
months

Development Age at 
presentation 

in years

Creatine 
kinase 

level* in 
IU/L

EMG ECG Muscle 
biopsy 

findings

Spine MRI 
findings

Primary 6 N 12 94 Myo Normal Myo, fat and 
collagen

Muscle 
wasting, 

hypointensity 
and fibro-fatty 

infiltration

Primary 6 N Not seen Not 
performed

Not 
performed

Not 
performed

Not 
performed

Not performed

Primary Unknown N 7 150 Myo Normal None Muscle 
wasting, 

hypointensity 
and fibro-fatty 

infiltration

Primary 18 N 5 145 Myo Normal None Muscle 
wasting, 

hypointensity 
and fibro-fatty 

infiltration

Primary 8 N 5 151 Myo Normal Patient did 
not consent 

Muscle 
wasting, 

hypointensity 
and fibro-fatty 

infiltration

Secondary† 10 Motor delay 2 856 Myo Normal Mitochondrial 
changes in 

shape and size

Normal 

Primary‡ 5 Motor delay 6 147 Myo Normal Non-specific 
Myo

Muscle 
wasting, 

hypointensity 
and fibro-fatty 

infiltration

Primary 12 Motor delay 11 200 Myo Normal Patient did 
not consent

Muscle 
wasting, 

hypointensity 
and fibro-fatty 

infiltration

Primary 15 Motor delay 9 187 Myo Normal Patient did 
not consent

Muscle 
wasting, 

hypointensity 
and fibro-fatty 

infiltration

Primary 15 Motor delay 8 230 Myo Normal Patient did 
not consent

Muscle 
wasting, 

hypointensity 
and fibro-fatty 

infiltration

Primary† 6 Motor delay 10.4 123 Myo Normal Multicore 
disease 

Not performed

Secondary At birth Motor delay 5.6 800 Myo Normal Congenital 
Myo of 

uncertain type

Not performed

EMG = electromyography; ECG = echocardiography; MRI = magnetic resonance imaging ; Myo = myopathy.
*Normal range: 62–302 IU/L. †Genetically confirmed. ‡Genetically negative.



Roshan Koul, Dilip Sankhla, Suad Al-Jahdhami, Renjith Mani, Rana A. Rahim, Saif Al-Yaarubi, Hussein Al-Kindy, 
Khalid Al-Thihli and Amna Al-Futaisi

Clinical and Basic Research | e367

sign was negative in all 10 of these children. MRI scans 
of the spine were diagnostic in cases of primary RSS. 
These scans revealed typical features of muscle mass 
loss in the paraspinal muscles and low signals of fibro-
fatty infiltration were seen replacing the muscle tissue. 
Two children with primary RSS had non-specific 
myopathy while a third child had a multicore type of 
congenital myopathy. The following case may serve as 
a representative example of primary RSS observed in 
this study. 

A 10-year-old boy with breathing difficulties and 
repeated chest infections was referred to SQUH from 
a peripheral hospital. Initial signs of the disease began 
in the first year of life with motor developmental delay; 
his parents noted that, compared to his siblings, the 
child was slower in learning to sit. However, he was 
able to walk by the time he was two years old and 
all social and mental milestones were achieved in an 
appropriate timeframe compared to his siblings. After 
the age of six years, the child contracted repeated 
chest infections requiring ventilatory support and 
was admitted multiple times to the intensive care unit 
(ICU) of a peripheral hospital. In 2014, primary muscle 
disease was suspected and the patient was referred to 
the SQUH ICU. On examination, the boy had normal 
higher mental and cranial nerve function. However, he 
had wasting of the spine muscles and could not bend 
his spine or neck [Figure 1]. His intercostal muscles 
were weak and he had mild difficulty in getting up, 
although after standing he was able to walk normally. 
All deep tendon reflexes were elicited and his serum 
creatine kinase levels were normal.

An electrocardiogram (ECG) and an 
echocardiography scan showed normal results; 
however, myopathy was observed in an electro-
myogram (EMG). A muscle biopsy was performed 
and the diagnosis was confirmed by electron 
microscopy to be a multicore disease in the form 
of congenital myopathy [Figure 2]. Nicotinamide 
adenine dinucleotide staining is diagnostic in RSS; 
however, histochemistry and light microscopy was 
not possible as the muscle biopsy had very limited 
muscle tissue. Genetic testing for SEPN1 was positive. 
Unfortunately, an MRI scan of the spine could not 
be arranged before the child was referred back to the 
peripheral hospital. However, an MRI scan performed 
on a similarly affected male patient revealed wasting of 
the paraspinal muscles [Figure 3]. 

The two children with secondary RSS had mild 
neck rigidity but demonstrated typical features of 
the underlying disease with positive Gowers’ signs. 
Both patients were female. One of the secondary RSS 
patients had mitochondrial myopathy features and 
was found to have mitochondrial deletion. She had 
a single heterozygous mutation in the polymerase 
gamma (POLG) gene (c.803G>C, p.268GLyc>Ala), 
indicating POLG-related mitochondrial depletion 
syndrome. Serum creatine kinase levels were 
elevated in the first child and normal in the second. 
The former was initially diagnosed by electron 
microscopy to have mitochondrial myopathy with a 
mitochondrial deletion. An EMG was myopathic and 
nerve conduction was normal. The second patient had 
features of congenital myopathy although the exact 
type could not be ascertained. MRI scans of the brain 
and spine were normal in both cases of secondary RSS. 

Figure 1: Photograph of a child diagnosed with primary 
rigid spine syndrome showing wasted neck muscles and 
an inability to bend the neck. Respiratory difficulties 
required him to be on nasal oxygen supplementation.

Figure 2: Electron microscopy showing multicore 
bodies in the muscle (arrows). This confirmed the 
diagnosis of primary rigid spine syndrome.



Rigid Spine Syndrome among Children in Oman

e368 | SQU Medical Journal, August 2015, Volume 15, Issue 3

A representative secondary RSS patient is detailed 
below. 

A five-year-old girl was referred to SQUH from a 
local orthopaedic hospital in 2014 for an evaluation 
of foot deformities. Although she had a normal birth 
and mental and social milestones, her parents noted a 
delay in motor skill development. On examination, the 
cranial nerves were normal. Her face had a myopathic 
look with jaw drop. She had proximal muscle weakness 
and was positive for Gowers’ sign. She had difficulty in 
bending and turning her neck fully. Both upper and 
lower limb strength was grade 4/5. Bilateral mild foot 
inversion with mild weak dorsiflexion of both feet was 
observed. Her serum creatine kinase level was normal. 
ECG and echocardiography showed no abnormal 
findings. The EMG was myopathic and nerve 
conduction was normal. A muscle biopsy resulted in 
an initial diagnosis of congenital myopathy, awaiting 
confirmation via electron microscopy.

Discussion 

There are several childhood muscle dystrophies 
and congenital myopathies that may present with a 
rigid spine in the late stages of the primary disease. 
This is due to the progression of the disease to the 
paraspinal muscles and is referred to as secondary 
RSS.5 In these cases, serum creatine kinase levels may 
be elevated and the respiratory muscles affected in 
the terminal stage of the disease.15 Muscle biopsies 
and genetic studies help to confirm the diagnosis of 
the original disease. An MRI scan of the spine does 
not show the same changes as those seen in primary 
RSS.15 Of the two children with secondary RSS in the 
current study, one had congenital myopathy while the 
other had mitochondrial myopathy. The latter was 

found to have POLG-related mitochondrial depletion 
syndrome; this mutation is pathogenic and has been 
reported elsewhere.16 

In primary RSS, the disease starts in the paraspinal 
muscles and then spreads to the other muscles.8 
Serum creatine kinase levels and echocardiography 
scans are usually normal in these children.13 There 
is no proximal weakness at the onset of the disease 
and the diagnosis is usually made by features of spine 
stiffness, an inability for the patient to bend their neck 
and imaging evidence of the loss of muscle mass in the 
erector spinae muscles.13 Primary RSS appears to have 
a genetic basis as mutations in the SEPN1 gene have 
been found to be associated with primary RSS, with 
four siblings mapped to the 1p35-36 chromosome 
bands.9,13 However, in a previous cases series of seven 
children with RSS in Oman, SEPN1 testing was negative 
in one patient.5 In the current study genetic testing 
for SEPN1 for one patient was positive. Primary RSS 
among children is rarely reported in the literature.12,13 
A regional genetic factor may be responsible for the 
number of primary RSS cases observed in this current 
single centre study from Oman. 

Differential diagnosis of secondary RSS is not 
difficult as the underlying primary condition often 
dominates the clinical picture. However, primary RSS 
needs to be differentiated from other rare conditions 
such as X-linked Emery-Dreifuss muscular dystrophy, 
generalised dystonia and stiff person syndrome.15,17 In 
cases of Emery-Dreifuss muscular dystrophy, there 
is proximal wasting of the upper limb muscles with 
contractures and early cardiac involvement. Serum 
creatine kinase levels are high and an ECG usually 
shows abnormal findings.15 Muscle biopsies and 
genetic testing are used to confirm the diagnosis. 
Dystonia can be differentiated from RSS due to the 

Figure 3: Low signal intensity magnetic resonance image of the spine in a case of paediatric primary rigid spine syndrome. 
There was wasting of the back muscles of the spine, particularly the erector spinae. The muscle tissue was replaced by 
fibro-fatty tissue (arrowheads). 



Roshan Koul, Dilip Sankhla, Suad Al-Jahdhami, Renjith Mani, Rana A. Rahim, Saif Al-Yaarubi, Hussein Al-Kindy, 
Khalid Al-Thihli and Amna Al-Futaisi

Clinical and Basic Research | e369

rigidity of the entire body—as opposed to the localised 
stiffness seen in RSS—and abnormal posture.17 Stiff 
person syndrome may be the initial diagnosis given in 
cases of primary RSS; indeed, one of the patients in the 
current study was initially diagnosed with stiff person 
syndrome while abroad. Generalised body stiffness 
involving even the abdominal muscles helps in making 
the correct diagnosis. Stiff person syndrome is very 
uncommon in children.17

Physiotherapy and occupational therapy are the 
main treatments currently available for RSS. The early 
involvement of the respiratory muscles in children 
with primary RSS can be rapid and fatal. In these cases, 
prompt respiratory care with pulmonary bi-level 
positive airway pressure non-invasive ventilation—a 
common mode of respiratory support for patients 
with respiratory muscle weakness—can prolong 
life expectancy.18

A possible limitation of this study was the fact 
that histopathological and genetic testing was only 
performed for a few patients. Further studies are 
recommended to confirm the histopathological and 
genetic findings of cases of paediatric RSS in Oman. 
The development of local advanced genetic facilities 
is recommended.

Conclusion

This study aimed to report on cases of RSS among 
children in Oman. Only 12 children who presented to 
SQUH during the 18-year study period were reported 
to have this condition. A total of 10 patients were found 
to have primary RSS while the remaining two had the 
secondary form of the disease. As the two forms of this 
disease have different aetiologies, cases of primary RSS 
should be differentiated from the secondary type.

c o n f l i c t o f i n t e r e s t
The authors declare no conflicts of interest.

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