Syringomyelia

• Introduction
• Pathogenesis
• Etiology
• Symptoms
• Imaging
• Differential Diagnosis
• Therapy
• Complications of Surgery
• Prognosis
• Conclusion
• References

Abstract

Syringomyelia is an etiologically diverse affliction caused by disturbance of normal cerebrospinal fluid flow dynamics. An evaluation by comprehensive imaging, using advanced three-dimensional constructive interference in steady state and four-dimensional phase contrast imaging techniques, should be focused on finding the causative lesion because this determines which surgical strategy could be employed. This review discusses the pathogenesis and various etiologies of syringomyelia, and focuses on the specific surgical approach for each, mentioning aspects of surgical complications and prognosis. Particular attention is given to the “persistent central canal,” a normal anatomical variant of the persistent fetal configuration of the central canal, as this is increasingly seen nowadays on routine magnetic resonance imaging.

Syrinx (Gr. Συρινξ) was a Naiad fresh-water nymph who lived on the cold mountainsides of Arcadia. One day she was amourously pursued by the Greek god Pan, and fleeing from her chaser, she was barred by the river Ladon. She asked for assistance from her Sorores Liquidae (Watery Sisters), who transformed her into a hollow water reed. When the god's frustrated breath blew over the river, it made a haunting sound. Pan cut the reeds to fashion the first set of pan pipes, which were thenceforth known as syrinx.

Ovid, Metamorphoses 1. 689 ff (trans. Melville) (Roman epic C1st BC to C1st AD)

Introduction

Syringomyelia literally means “cavity within the spinal cord” and is typically a progressive chronic condition. The syrinx is either a fluid-filled, gliosis-lined cavity within the spinal cord parenchyma or it is a focal dilatation of the central canal, in which case it is called hydromyelia.[1] In everyday clinical practice, the term syringomyelia is commonly used for both conditions. Most lesions are located between C2 and T9, but they can descend down to the conus medullaris, or extend upward into the brain stem (i.e., syringobulbia). The estimated prevalence varies widely from 1.94 per 100,000 in Japan to 8.4 per 100,000 in Western countries and the cause for this wide variety is unknown.[2] [3]

In children, syringomyelia usually occurs in the setting of congenital anomalies, most commonly the Chiari-I malformation and tethered cord, but it can also develop years after meningitis and spinal trauma or with intramedullary and extramedullary tumors. Several clinical aspects relevant for the diagnosis and treatment are reviewed.

Pathogenesis

Congenital syringomyelia is seen as an abnormality of primary neurulation and can be distinguished into two forms.[4] The embryonic form consists of an abnormal dilatation of the central canal of the spinal cord, with a thin and elongated roof plate, and lack, or near-absence, of mesenchymal tissue between the spinal cord and the surface ectoderm, causing a gap in the posterior vertebral arches—an open neural tube defect. The fetal form on the contrary does not affect mesenchymal tissue development and is therefore associated with an intact vertebral column—a closed neural tube defect.

Acquired syringomyelia is thought to be caused by disturbance in normal cerebrospinal fluid (CSF) circulation. In Chiari-I malformation, this disturbance is caused by the downward herniation of the cerebellar tonsils, obstructing normal CSF flow from the cranial to spinal compartment during the normal cardiac cycle or normal Valsalva maneuvers, such as coughing, laughing, etc. These abnormal pressure gradients eventually lead to accumulation of fluid in either the central canal or the spinal cord parenchyma. The same mechanism is thought to be responsible for syringomyelia after infection (e.g., meningitis), inflammation (e.g., sarcoidosis and multiple sclerosis), trauma (adhesive arachnoiditis), and extramedullary lesions (e.g., tumors and arachnoid cysts). Syringomyelia in association with intramedullary tumors may have a similar pathogenesis, but it can also be the result of tumor activity per se, as seen in ependymomas and hemangioblastomas ([Figs. 1] and [2]).

New formation of a syrinx, or enlargement of an already present syrinx, in a child with a tethered spinal cord can also be caused by an accompanying Chiari-II malformation, causing likewise obstruction of normal CSF flow dynamics as in Chiari-I malformations. Mechanical effects of spinal cord tethering or metabolic and ischemic changes in the distal spinal cord have also been suggested as contributing factors in syrinx formation in these patients.[5]

Etiology

The etiology of syringomyelia can be deduced from its presumed pathogenesis such as, a congenital malformation, any acquired lesion, or disease, causing disturbance of normal CSF flow dynamics.

The most common congenital causes are neural tube defects (myelomeningocele and tethered cord syndrome) and Chiari malformations. Magnetic resonance imaging (MRI) reveals syringomyelia in 30 to 50% of these patients, ranging from localized, segmental cavities to severe holocord cavities.[6] Most syringes are present since birth, and others develop (or enlarge) during life. Other congenital spinal anomalies, such as, Klippel–Feil syndrome, that cause spinal canal narrowing may also lead to CSF flow disturbances with resulting syringomyelia.[7]

Acquired causes of syringomyelia are plentiful and include the following:

• Hydrocephalus, leading to pegging of the cerebellar tonsils, and therefore mimicking Chiari-I malformation.

• Postinfectious, after any kind of meningitis, as this invariably leads to arachnoid scarring.

• Postinflammatory after, for example, transverse myelitis, sarcoidosis, and multiple sclerosis.[8] [9] [10]

• Posttraumatic, including postsurgical, arachnoid scarring.

• Spinal cord tumors, especially ependymomas and hemangioblastomas.

• Extramedullary tumors and arachnoid cysts.

• Spinal canal stenosis, especially cervical, usually seen only in adults.

Symptoms

A syrinx can be asymptomatic and then it is only discovered on incidental spinal cord imaging. In symptomatic patients with syringomyelia, bilateral motor and sensory symptoms and signs that do not involve the head or face can be seen as in any other spinal cord lesion.

Patients often present with pain, weakness, and stiffness in the back, shoulders, and extremities. Loss of the ability to feel extremes of hot or cold, especially in the hands, is frequently seen, with a cape-like loss of pain and temperature sensation along the back and arms, caused by damage to the centrally crossing fibers of the spinothalamic tract. Symptoms of autonomic bladder and bowel dysfunction are very uncommon until end-stage spinal cord dysfunction. The course of the symptoms often fluctuates in severity and duration, and each patient experiences a different combination of these symptoms, typically varying depending on the extent and the location of the syrinx within the spinal cord.

The clinical picture in patients with a neural tube defect is somewhat different. Usually they present with new neurological deficits in the lower extremities, bowel, and bladder dysfunction (often asymptomatic and only found on urological dynamic examinations), or pain, and this actually cannot be distinguished from clinical deterioration caused by the tethered cord itself, rather than by the syringomyelia. However, scoliosis seems to be a prominent feature in those patients who have a terminal syrinx, independent of the size of the syrinx.[11] Syringomyelia extending upward into the cervical spinal cord can present with hand weakness and sensory symptoms, and this can be difficult to distinguish from symptomatic Chiari-II malformation, which is invariably present in these patients. Fortunately, the surgical therapy is the same for both.

In closed neural tube defects, the syrinx is usually located immediately rostral to the tethering lipoma or bony spur and remains localized to the lower thoracic and lumbar levels. In meningomyelocele patients, the syrinx can be quite extensive and reach up to the cervical spinal cord.[12]

Imaging

Visualization of intramedullary cavities or perimedullary CSF flow disturbances used to be very difficult. Invasive contrast myelography was required and the images obtained were quite “crude”. This was improved upon by computed tomographic (CT) myelography, until the advent of MRI, which can easily identify the location and extent of any intramedullary cavity. To detect, sometimes subtle, extramedullary arachnoid adhesions or membranes, advanced imaging techniques, such as, three-dimensional (3D) constructive interference in steady state (CISS) sequences, can be very helpful and often indispensable. Using electrocardiographically gated flow-sensitive techniques, such as four-dimensional (4D) phase contrast (PC) MRI, CSF flow dynamics can be studied to distinguish physiological from complex pathological flow patterns at the craniocervical junction and cervical and thoracic spine, and to detect cystic spaces not communicating with normal CSF spaces.[13] [14] [15]

For the complete work-up of a patient with syringomyelia, one should keep in mind that all possible causes should be eliminated, so MRI of the lumbar-sacral spine to rule out a tethered cord is mandatory, as is an MR scan of the head and craniocervical junction to rule out hydrocephalus and Chiari malformation. The administration of contrast medium is essential to diagnose any associated conditions, such as, intramedullary and extramedullary tumors.

Differential Diagnosis

When evaluating a patient with syringomyelia it is important to first identify the etiology, as any therapeutic strategy will most certainly focus on a causative lesion rather than on the syrinx itself. This means that hydrocephalus, or shunt malfunction, should be ruled out by MR scanning of the head, and tethered cord should be excluded by MR scanning of the lumbosacral spine, as should any other lesion as discussed in the “etiology” section. In the absence of a causative lesion, there are not many alternatives. However, nowadays widespread MR availability and pre-emptive screening of asymptomatic individuals is increasingly leading to incidental MR findings of intramedullary cavities in all forms, shapes and sizes, and in a significant percentage of these patients no causative lesion or mechanism can be found, even with all advanced imaging techniques. In these cases, a diagnosis of “idiopathic localized hydromyelia” is sometimes made, but as this condition probably represents persistence into adult life of a fetal configuration of the central canal of the spinal cord, it is probably wiser to refer to this condition as the “persistent central canal.”[16] [17] The central canal of the spinal cord is present at birth and usually becomes progressively obliterated, but we now know that it can persist partially or completely. To make a diagnosis of “persistent central canal,” there should not be any factors predisposing to syringomyelia and the syrinx should be located at the junction of the ventral one-third and dorsal two-third of the spinal cord and filiform in shape ([Fig. 3]) and not eccentrically located ([Fig. 4]).

Therapy

As the persistent central canal is considered a normal anatomical variant, this requires no treatment. (There is no etiological cause to be “removed or corrected” and the cavity is usually so small that surgical treatment is not even possible.) Large clinical series have not yet been reported, but initial findings show that these cavities do not change in size in time.[16] [17] Therefore as it is a normal anatomical variant, they can be considered an incidental finding, and likewise, follow-up imaging is not warranted. The exact size and extent of these persistent canals is not (yet) known, as increasingly sophisticated MR techniques are enabling an increased visualization of cavities that were not visible before.

In asymptomatic syringomyelia, an expectant policy seems justified, although sometimes this can prove quite difficult especially in those cases where a large syrinx extends all the way up to cervical spinal cord and the brain stem. Nevertheless, it should be noted that spontaneous resolution of syringomyelia has been observed, albeit infrequently.

Nonsurgical treatment of symptomatic syringomyelia focuses either on management of pain and (painful) paresthesias with analgesics, antidepressants, antiepileptic drugs, or gamma-aminobutyric acid-analogs, or on maintaining functional ability and quality of life with physical medicine and rehabilitation.

In patients with neural tube defects, syringomyelia, and symptoms, such as, progressive scoliosis, urological problems, pain, and motor or sensory defects, shunt malfunction should be excluded first, even if this entails empirical shunt revision. If this is not successful, untethering of the cord is usually considered before specific surgical treatment of the syringomyelia. In many cases, untethering leads to improvement in the neurologic deficits. However, one should be aware that a syrinx can appear larger on follow-up MRI after successful untethering.[18]

Patients with tonsillar herniation of less than 5 mm but normal CSF flow dynamics on 4D-PC MRI and only mild symptoms suggestive of symptomatic syringomyelia are probably best treated conservatively as decompressive surgery in these patients probably will not meaningfully change an already normal CSF flow.

In all other cases, the goal of surgery is restoration of normal CSF flow dynamics. The surgical strategy then varies according to the etiological cause of the syringomyelia. In Chiari-I malformation, a craniocervical decompression will be performed, often combined with an augmentation duraplasty to restore normal craniospinal CSF flow ([Fig. 5]). Normal fourth ventricle CSF outflow must also be restored, if necessary by placing a fourth ventricular-spinal or ventriculopleural catheter ([Fig. 6]). In Chiari-II malformation, the foramen magnum is typically enlarged and decompression usually consists of the removal of cervical laminae until the level of the normal spinal cord (depending on the extent of tonsillar descent), section of constricting fibrous bands (usually at the C0–C1 level), and again, normal fourth ventricle CSF outflow must be restored, if necessary, by placing a fourth ventricular-spinal catheter. In the case of spinal canal stenosis, a laminectomy without opening of the dura will suffice to restore normal CSF flow dynamics and subsequent syrinx resolution. Syringomyelia caused by intramedullary or extramedullary tumors or arachnoid cysts is treated by resection of the tumors or fenestration or marsupialization of the cysts.

The most difficult form of syringomyelia to treat surgically is that caused by arachnoid scarring, whether it is caused by infection, inflammation, or trauma. Localized, constrictive bands of fibrosis can be quite safely sectioned (i.e., adhesiolysis), with restoration of CSF flow. But in widespread arachnoiditis, the dura, arachnoid, and pia matter can all be completely opaque white and adherent to one another, making it virtually impossible during surgery to distinguish normal anatomical structures, even when using the operating microscope. In these cases, adhesiolysis is not possible and the only remaining option then is direct drainage of the syrinx.

There are three options for direct drainage of a syrinx: syringoarachnoid, syringoperitoneal, and syringopleural. Syringoarachnoid drainage is effective in localized arachnoid scarring, it more or less restores normal CSF dynamics as the CSF is absorbed through normal pathways and obviates the need to open the peritoneum or the pleura, but it is also fraught with shunt obstruction caused by new arachnoid scarring. Syringoperitoneal drainage is analogous to ventriculoperitoneal drainage but, in everyday practice, not very practical, as virtually all patients with syringomyelia are operated on in a prone position, making the abdomen not very accessible. It is reserved for those patients in whom the pleural cavity is not an option. Syringopleural drainage has several advantages: the CSF is drained away from the arachnoid space, which is often compromised by the extensive scarring causing the syrinx in the first place; the pleural cavity is readily accessible in the prone position using a small incision below the right scapula; and the negative intrapleural pressure gently “sucks out” the CSF from the syrinx ([Fig. 7]).

Complications of Surgery

Besides general complications in neurosurgery such as anesthetic and general complications, infections, and postoperative hematomas, the most prominent problems in syringomyelia surgery are scar formation around the spinal cord and any implanted shunts, wound leakage of CSF, and shunt obstruction. For direct drainage of a syrinx, a micromyelotomy is required. In paraplegic or tetraplegic patients, this is performed below the functional level so no additional neurological deficit will be made. In intact patients, the micromyelotomy will be placed at the level where the posterior part of the spinal cord is thinnest to minimize any additional sensory disturbances from posterior column damage.

Prognosis

Syringomyelia is a chronic, often slowly, progressive disease, with remissions, and exacerbations. Invariably, progressive loss of function will be incapacitating and often this necessitates surgical intervention. Although the progression of neurologic deficits usually stabilizes after intervention, and patients sometimes improve, they often remain symptomatic. Especially, a debilitating central pain syndrome may prove to be quite therapy-resistant, despite adequate surgical therapy and collapse of the syrinx on imaging.

Conclusion

Fluid-filled cavities within the spinal cord can be found on routine MR investigation in asymptomatic subjects, probably represent persistence into adult life of a fetal configuration of the central canal of the spinal cord, and should be regarded as a variant of normal anatomy—the persistent central canal.

In symptomatic patients with syringomyelia (a gliosis-lined cavity within the spinal cord parenchyma), or hydromyelia (a focal dilatation of the central canal), an extensive work-up should be done to find the etiology causing a disturbance in normal CSF dynamics. In shunted patients, a shunt dysfunction should be ruled out first. Treatment should primarily be directed at restoring the normal CSF dynamics rather than at the syrinx itself. Neurologic deficits usually stabilize after surgical intervention, although patients often remain symptomatic. Pain can be a persisting problem.

• References

• 1 Milhorat TH. Classification of syringomyelia. Neurosurg Focus 2000; 8 (3) E1
  PubMedGoogle Scholar
• 2 Sakushima K, Tsuboi S, Yabe I , et al. Nationwide survey on the epidemiology of syringomyelia in Japan. J Neurol Sci 2012; 313 (1-2) 147-152
  CrossrefPubMedGoogle Scholar
• 3 Brickell KL, Anderson NE, Charleston AJ, Hope JK, Bok AP, Barber PA. Ethnic differences in syringomyelia in New Zealand. J Neurol Neurosurg Psychiatry 2006; 77 (8) 989-991
  CrossrefPubMedGoogle Scholar
• 4 Ikenouchi J, Uwabe C, Nakatsu T, Hirose M, Shiota K. Embryonic hydromyelia: cystic dilatation of the lumbosacral neural tube in human embryos. Acta Neuropathol 2002; 103 (3) 248-254
  CrossrefPubMedGoogle Scholar
• 5 Sade B, Beni-Adani L, Ben-Sira L, Constantini S. Progression of terminal syrinx in occult spina bifida after untethering. Childs Nerv Syst 2003; 19 (2) 106-108
  PubMedGoogle Scholar
• 6 La Marca F, Herman M, Grant JA, McLone DG. Presentation and management of hydromyelia in children with Chiari type-II malformation. Pediatr Neurosurg 1997; 26 (2) 57-67
  CrossrefPubMedGoogle Scholar
• 7 Guille JT, Miller A, Bowen JR, Forlin E, Caro PA. The natural history of Klippel-Feil syndrome: clinical, roentgenographic, and magnetic resonance imaging findings at adulthood. J Pediatr Orthop 1995; 15 (5) 617-626
  CrossrefPubMedGoogle Scholar
• 8 Ravaglia S, Bogdanov EI, Pichiecchio A, Bergamaschi R, Moglia A, Mikhaylov IM. Pathogenetic role of myelitis for syringomyelia. Clin Neurol Neurosurg 2007; 109 (6) 541-546
  CrossrefPubMedGoogle Scholar
• 9 Charles JA, Berger M, Cook SD. Thoracic syringomyelia and suspected multiple sclerosis: cause and effect or coincidence?. Neurology 2004; 63 (1) 185-186
  CrossrefPubMedGoogle Scholar
• 10 Marangoni S, Argentiero V, Tavolato B. Neurosarcoidosis. Clinical description of 7 cases with a proposal for a new diagnostic strategy. J Neurol 2006; 253 (4) 488-495
  CrossrefPubMedGoogle Scholar
• 11 Iskandar BJ, Oakes WJ, McLaughlin C, Osumi AK, Tien RD. Terminal syringohydromyelia and occult spinal dysraphism. J Neurosurg 1994; 81 (4) 513-519
  CrossrefPubMedGoogle Scholar
• 12 Koyanagi I, Iwasaki Y, Hida K, Abe H, Isu T, Akino M. Surgical treatment of syringomyelia associated with spinal dysraphism. Childs Nerv Syst 1997; 13 (4) 194-200
  CrossrefPubMedGoogle Scholar
• 13 Chavhan GB, Babyn PS, Jankharia BG, Cheng HL, Shroff MM. Steady-state MR imaging sequences: physics, classification, and clinical applications. Radiographics 2008; 28 (4) 1147-1160
  CrossrefPubMedGoogle Scholar
• 14 Roser F, Ebner FH, Danz S , et al. Three-dimensional constructive interference in steady-state magnetic resonance imaging in syringomyelia: advantages over conventional imaging. J Neurosurg Spine 2008; 8 (5) 429-435
  CrossrefPubMedGoogle Scholar
• 15 Bunck AC, Kröger JR, Jüttner A , et al. Magnetic resonance 4D flow characteristics of cerebrospinal fluid at the craniocervical junction and the cervical spinal canal. Eur Radiol 2011; 21 (8) 1788-1796
  CrossrefPubMedGoogle Scholar
• 16 Holly LT, Batzdorf U. Slitlike syrinx cavities: a persistent central canal. J Neurosurg 2002; 97 (2, Suppl) 161-165
  CrossrefPubMedGoogle Scholar
• 17 Jinkins JR, Sener RN. Idiopathic localized hydromyelia: dilatation of the central canal of the spinal cord of probable congenital origin. J Comput Assist Tomogr 1999; 23 (3) 351-353
  CrossrefPubMedGoogle Scholar
• 18 Vandertop WP. Progression of terminal syrinx in occult spina bifida. Childs Nerv Syst 2003; 19 (5-6) 267 , author reply 268
  CrossrefPubMedGoogle Scholar

Address for correspondence

• References

• 1 Milhorat TH. Classification of syringomyelia. Neurosurg Focus 2000; 8 (3) E1
  PubMedGoogle Scholar
• 2 Sakushima K, Tsuboi S, Yabe I , et al. Nationwide survey on the epidemiology of syringomyelia in Japan. J Neurol Sci 2012; 313 (1-2) 147-152
  CrossrefPubMedGoogle Scholar
• 3 Brickell KL, Anderson NE, Charleston AJ, Hope JK, Bok AP, Barber PA. Ethnic differences in syringomyelia in New Zealand. J Neurol Neurosurg Psychiatry 2006; 77 (8) 989-991
  CrossrefPubMedGoogle Scholar
• 4 Ikenouchi J, Uwabe C, Nakatsu T, Hirose M, Shiota K. Embryonic hydromyelia: cystic dilatation of the lumbosacral neural tube in human embryos. Acta Neuropathol 2002; 103 (3) 248-254
  CrossrefPubMedGoogle Scholar
• 5 Sade B, Beni-Adani L, Ben-Sira L, Constantini S. Progression of terminal syrinx in occult spina bifida after untethering. Childs Nerv Syst 2003; 19 (2) 106-108
  PubMedGoogle Scholar
• 6 La Marca F, Herman M, Grant JA, McLone DG. Presentation and management of hydromyelia in children with Chiari type-II malformation. Pediatr Neurosurg 1997; 26 (2) 57-67
  CrossrefPubMedGoogle Scholar
• 7 Guille JT, Miller A, Bowen JR, Forlin E, Caro PA. The natural history of Klippel-Feil syndrome: clinical, roentgenographic, and magnetic resonance imaging findings at adulthood. J Pediatr Orthop 1995; 15 (5) 617-626
  CrossrefPubMedGoogle Scholar
• 8 Ravaglia S, Bogdanov EI, Pichiecchio A, Bergamaschi R, Moglia A, Mikhaylov IM. Pathogenetic role of myelitis for syringomyelia. Clin Neurol Neurosurg 2007; 109 (6) 541-546
  CrossrefPubMedGoogle Scholar
• 9 Charles JA, Berger M, Cook SD. Thoracic syringomyelia and suspected multiple sclerosis: cause and effect or coincidence?. Neurology 2004; 63 (1) 185-186
  CrossrefPubMedGoogle Scholar
• 10 Marangoni S, Argentiero V, Tavolato B. Neurosarcoidosis. Clinical description of 7 cases with a proposal for a new diagnostic strategy. J Neurol 2006; 253 (4) 488-495
  CrossrefPubMedGoogle Scholar
• 11 Iskandar BJ, Oakes WJ, McLaughlin C, Osumi AK, Tien RD. Terminal syringohydromyelia and occult spinal dysraphism. J Neurosurg 1994; 81 (4) 513-519
  CrossrefPubMedGoogle Scholar
• 12 Koyanagi I, Iwasaki Y, Hida K, Abe H, Isu T, Akino M. Surgical treatment of syringomyelia associated with spinal dysraphism. Childs Nerv Syst 1997; 13 (4) 194-200
  CrossrefPubMedGoogle Scholar
• 13 Chavhan GB, Babyn PS, Jankharia BG, Cheng HL, Shroff MM. Steady-state MR imaging sequences: physics, classification, and clinical applications. Radiographics 2008; 28 (4) 1147-1160
  CrossrefPubMedGoogle Scholar
• 14 Roser F, Ebner FH, Danz S , et al. Three-dimensional constructive interference in steady-state magnetic resonance imaging in syringomyelia: advantages over conventional imaging. J Neurosurg Spine 2008; 8 (5) 429-435
  CrossrefPubMedGoogle Scholar
• 15 Bunck AC, Kröger JR, Jüttner A , et al. Magnetic resonance 4D flow characteristics of cerebrospinal fluid at the craniocervical junction and the cervical spinal canal. Eur Radiol 2011; 21 (8) 1788-1796
  CrossrefPubMedGoogle Scholar
• 16 Holly LT, Batzdorf U. Slitlike syrinx cavities: a persistent central canal. J Neurosurg 2002; 97 (2, Suppl) 161-165
  CrossrefPubMedGoogle Scholar
• 17 Jinkins JR, Sener RN. Idiopathic localized hydromyelia: dilatation of the central canal of the spinal cord of probable congenital origin. J Comput Assist Tomogr 1999; 23 (3) 351-353
  CrossrefPubMedGoogle Scholar
• 18 Vandertop WP. Progression of terminal syrinx in occult spina bifida. Childs Nerv Syst 2003; 19 (5-6) 267 , author reply 268
  CrossrefPubMedGoogle Scholar