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Category: Volume 07 Issue 05 May 2019
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Title: Guillain Barre Syndrome - A Case Series

Authors: Dr Kush Jhunjhunwala, Dr Gurmeet Singh Sarla

 DOI: https://dx.doi.org/10.18535/jmscr/v7i5.120

Abstract

Objective: To assess retrospectively the clinical profile, nerve conduction velocity studies and outcome of Guillian Barre Syndrome (GBS) in children.

Materials and Methods: The clinical and electrophysiological data of 184 children, who attended Kalawati Saran Children Hospital from Jan 2001 to Sept 2005 and were diagnosed as GBS based on Asbury-Cornblath criteria, were analyzed in the study. Severity of weakness was graded according to Hughes staging. Outcome was determined according to the functional recovery and independent ambulation. It was assessed in follow up at 1 month, 3 months and 6 months after the onset.

Results: A total of 184 patients were diagnosed as GBS during the study period, with an age range from 1-to15 yrs. (Mean-4.99_+ 2.95). Of this 37.4 % of cases were less than 3 years of age. There was a male preponderance with 71.7% of them being males. Seasonal preponderance was evident in more than 50% cases, developing the disease in summer season (May to Aug). Acute respiratory infections in 39/101 (38.61%) were the most common antecedent event followed by diarrhoea in 16/101(15.84%) and others (1-Tuberculosis, 1-measles, 2-skin infection). The most common symptom at the time of presentation was limb weakness, which was seen in all patients, followed by pain/paraesthesia in 31% and respiratory symptoms in 10% of the patients. Bulbar weakness was the most common type of cranial nerve involvement seen in 13%of them. Majority of the patients 140/184(76.08%) presented in stage IV {a-57 (40.71%), b-83 (59.28%)} followed by 29/184(15.76%) in stage III. Respiratory system involvement in the form of respiratory distress with potential respiratory failure was present in 33/184(18.08%), of which 19 (10.32%) patients required ventilator support. Cerebrospinal fluid (CSF) studies could be conducted in 31% of the patients who were admitted in the hospital and 70% of them showed some elevation of protein and cells in the CSF. Nerve conduction study (NCV) could be done only in 94/184(51.09%) patients and demyelination was the commonest finding in 51/94(54.26%). There were total 14(18.42%) deaths among the 76 patients who were admitted in the hospital and the commonest cause for death was respiratory failure. Seventy- nine cases were examined at 1 month out of which 51.89% were ambulatory with/ without support, 65% patients were seen at 3 month of which 50.42% recovered completely and 26.05% were ambulatory with minimum deficit. At 6 months follow-up, only 26 patients reported back, of which 15 (57.70%) had full recovery and rest of them were in the favorable group (100%) i.e. in stage III or less.

Conclusion: The most common symptom at the time of presentation was limb weakness. Respiratory system involvement was seen in only 18 % of the patients and only 10% of them required ventilator support. Seventy percent of the patients in whom CSF study was done showed elevation of proteins. Demylination was the commonest finding in nerve conduction study.  Outcome is good with general supportive care. 

References

  1. WHO
  2. Seneviratne U. Guillian Barre Syndrome. Postgrad Med J 2000; 76:774-82.
  3. McKhann GM. Cornblath DR. Griffin JW. Et al. Acute Motor Axonal Neuropathy; a frequent cause of acute flaccid paralysis in China. Ann Neurol 1993; 33:333-42.
  4. Graffin JW. Li CY. Ho TW. Et al. Guillian Barre Syndrome in Northern China. The spectrum of neuropathological changes in clinically defined cases. Brain 1995; 118:577-95.
  5. Paradiso G. Tripoli J. Galicchio S. Fejerman N. Epidemiological, cliniocal, and electrodiagnostic findings in childhood Guillian Barre Syndrome: A Reappraisal. Ann Neurol 1999; 46:701-7.
  6. Asbury AK. Cornblath DR Assement Of Current Diagnostic Criteria For Guillian Barre Syndrome. Ann Neurol 1990; 27 (Suppl): S21-24.
  7. Hughes RA. Newsom David JM. Perkin GD Pierce JM. Controlled trial prednisolon in acute polyneuropathy. Lancet 1978; 2:750-3
  8. Yakoob M, Rahman A Jamil B, Ali N. Characteristics of patients with Guillian Barre Syndrome At A Tertiary Care Center in Pakistan, 1995-2003. J Pak Med Assoc.  2005; 55(11): 493-6 (ISSN: 0030-9982)
  9. Tosta E, Kuckelhaus C. Guillain Barre Syndrome In A Population Less Than 15 Years Old In Brazil. Arq. Neuro-Psiquiatr. Vol 60 No 2 Sao Paulo June 2002.
  10. Hung P, Chang W el al. A Clinical and Electrophysiologic Survey of Childhood Guillain-Barre Syndrome. Pediatric Neurology Vol.30 No.2, pp86-91.
  11. McKhann GM. Cornblath DR. Ho T. el al. Clinical and electrophysiological aspects of acute paralytic disease of children and young adults in north China. Lancet 1991; 338:593-7
  12. Bradshaw D. Royden J. Guillain Barre Syndrome in Children: Clinical Course, Electrodiagnosis, And Prognosis.Muscle And Nerve 15:500-506 1992
  13. Cornblath DR. Electrophysiology in Guillain Barre Syndrome. Ann Neurol 1990; 27(suppl):  S17-S20.
  14. Singhi SC. Singhi P. Banerjee S. Prabhakar S. Intravenous immunoglobulin in very severe childhood Guillain-Barre syndrome. Annals of Tropical Paediatrics (1999).19, 167-174.
  15. Wu HS. Lie TC. Lu ZL et al. A prospective and electrophysiologic survey of acute paralysis in Chinese children. Neurology 2002; 49:1723-5
  16. Evans OB. Guillian Barre Syndrome in Children. Pediatr Rev 1986; 8:69-74
  17. Hung KL. Wang HS Liou WY et al Guillain-Barre Syndrome in children: A cooperative study in Taiwan. Brain Dev 1994; 16:204-8
  18. Rong-Kuo Lyu. Lok-Ming Tang. Shaw-Yi Cheng. Wen-Chuin Hsu. Sien-Tsong Chen. Guiollain Barre Syndrome In Taiwan. J Neurol Neurosurg Psychiatry 1997; 63:494-500 (October)
  19. Hung KL. Wang HS Liou WY et al Guillain-Barre Syndrome in children: A cooperative study in Taiwan. Brain Dev 1994; 16:204-8.
  20. Das A, Kalita J, Misra UK. Recurrent Guillain Barre’s Syndrome. Electromyogr Clin Neurophysiol. 2004 Mar; 44(2): 95-102.
  21. Grand’Maison F, Feasby TE, Hahn AF, Koopman WJ. Recurrent Guillain Barre Syndrome. Clinical and laboratory features. Brain 1992 Aug; 115 (pt 4): 1093-106.

Corresponding Author

Dr Gurmeet Singh Sarla

Classified Specialist Surgery, Military Hospital Devlali, Nasik, Maharshtra, India, Pin: 422401