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Hematology & Transfusion International Journal

Case Report Volume 5 Issue 3

Fulminant guillain barre syndrome (GBS) refractory to intravenous immunoglobulin (IVIG) treated with therapeutic plasma exchange

Debasish Gupta,1 Nair Revathy,1 Raina Abhinav,2 Nair Muralidharan2

1Department of Transfusion Medicine, Sree Chitra Tirunal Institute for Medical Sciences and Technology, India
2Department of Neurology, Sree Chitra Tirunal Institute for Medical Sciences and Technology, India

Correspondence: Dr. Debasish Gupta, Professor, Department of Transfusion Medicine, Sree Chitra Tirunal Institute for Medical Sciences and Technology, Trivandrum 695017, India, Tel 0471-2524177, 902012010

Received: August 16, 2017 | Published: October 12, 2017

Citation: Revathy N, Abhinav R, Muralidharan N, et al. Fulminant guillain barré syndrome (GBS) refractory to intravenous immunoglobulin (IVIG) treated with therapeutic plasma exchange. Hematol Transfus Int J. 2017;5(3):245-248. DOI: 10.15406/htij.2017.05.00120

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Abstract

A 53year old man was brought to the Neurology Intensive Care Unit, on a ventilator with a Glasgow Coma Scale (GCS) of 5T (E-Eye opening, V-Verbal response, M-Motor response, T-Intubated-E4VTM1) which later worsened to 2T (E1VTM1). On detailed evaluation, a diagnosis of Fulminant Guillain Barré Syndrome (Hughes score 5) was made and Intravenous Immunoglobulin (IVIG) was instituted. No response was noted even seven days after IVIG administration. Plasma exchange was initiated. A total of 14 exchanges were performed over a period of 13weeks wherein 21.8 liter of plasma was exchanged. Patient started showing signs of improvement by the 6th week of illness. By the 19thweek of illness, he could be completely weaned off the ventilator. At the time of discharge (27th week of illness), the power in his upper limbs was 4 and 2 in his lower limbs. Hughes score was 4 and GCS was 15(E4V5M6). This case illustrates the significant role of plasma exchange in the management of Fulminant Guillain Barré Syndrome.

Keywords: fulminant guillain barré syndrome, plasma exchange, neuromuscular paralysis, gangliosides, peripheral nerves

Abbreviations

ASFA, american society for apheresis; CMAPs, compound muscle action potentials; CSF, cerebrospinal fluid; EEG, electroencephalogram; EMG, electromyogram; EVM, eye opening, verbal response, motor response; GBS, guillain barré syndrome; GCS, glasgow coma scale; IVIG, intravenous immunoglobulin; NCS, nerve conduction study; NMICU, neuro-medical intensive care unit; NSTEMI, non ST segment elevation myocardial infarction; SNAPs, sensory nerve action potentials

Introduction

Guillain-Barré Syndrome (GBS) is an important cause of acute neuromuscular paralysis characterized by acute areflexic paralysis with albumin-cytological dissociation (i.e. high levels of protein in the cerebrospinal fluid and normal cell counts). Molecular mimicry and a cross-reactive immune response play a crucial role in its pathogenesis, at least in those cases with a previous Campylobacter jejuni infection and with antibodies to gangliosides.1 Guillain-Barré Syndrome is currently the most frequent cause of acute flaccid paralysis worldwide and constitutes one of the serious emergencies in neurology.2 We report our observation in a patient who presented in a state mimicking cerebral death. The patient’s efferent nerves were completely affected and he developed Fulminant GBS with inexcitable peripheral nerves.

Case presentation

A 53 year old, Type II diabetic and hypertensive gentleman was admitted in the Neuro Medical Intensive Care Unit (NMICU) following a rapidly progressive, acute ascending paralysis of all four limbs with dysphagia and regurgitation. He underwent intubation for acute respiratory distress at a local hospital and was shifted to our centre on the fifth day post intubation. No sedative drug had been administered. On examination, vital signs were stable. Patient was conscious, obeying and comprehending commands. Glasgow Coma Scale (GCS) at admission was E4VTM1 (E-Eye opening, V-Verbal response, M-Motor response, T-Intubated).3 He was noted to have ophthalmoparesis with bilateral ptosis. Pupils were bilaterally 4mm, sluggishly reactive to light. In addition, he had bifacial paresis with flaccid, areflexic quadriplegia. Nerve Conduction Study (NCS) showed ineluctable Compound Muscle Action Potentials (CMAPs) from bilateral peroneal, tibial, median and ulnar nerves. F waves and Sensory Nerve Action Potentials (SNAPs) were also absent from bilateral upper and lower limb nerves. GM1 antibody was borderline positive. Rest of the antiganglioside antibody profile including anti GQ1b was negative. Intra Venous Immunoglobulin (IVIG) was initiated at the local hospital since GBS was suspected and the course was completed at our centre. The reports of the haematological investigations done are as follows: Hemoglobin: 10.7g/dL, Total Count: 13,900/cumm, Serum Albumin: 4.2g%, Serum gamma globulins: Elevated, INR: 1.2, Serum Creatinine: 0.57mg/dL, Serum Calcium: 8.9mEq/L, Sodium: 136mEq/L, Potassium: 3.8mEq/L, Hepatitis A (IgM)/HIV/HBsAg/HCV: Negative Within 3 days of admission, patient developed complete ophthalmoplegia with fixed dilated pupils. Vestibulo-ocular reflexes were also absent and Electroencephalogram (EEG) showed generalised delta range slowing with occasional sleep spindles. There was no reactivity to noxious/visual stimulus. GCS worsened to E1VTM1. The possibility of central demyelination in addition to peripheral demyelination consistent with Bickerstaff encephalitis with Guillain Barré Syndrome overlap was considered. MRI performed on the 5th day of admission to rule out mesencephalic/diencephalic pathology was found to be normal. Cerebrospinal Fluid (CSF) analysis performed 2weeks after onset of symptoms showed a sterile CSF with albumino-cytological dissociation. Needle electromyogram performed on the 4thweek of admission showed evidence of denervation from all sampled muscles. Since the patient had worsening despite initiating IVIG, it was decided to switch over to plasma exchange (1week post last IVIG dose).

He received a total of 14 Plasma exchanges. His body weight was 80Kg and plasma volume was calculated as 3.48 litre (Total Plasma Volume=Total Blood Volume (1-Hematocrit)). 6.82 litre of plasma were exchanged over 4days (alternate days) by the intermittent type of apheresis machine. In each session only less than half the plasma volume was exchanged in view of autonomic instability. Further exchanges had to be avoided for the next 3weeks as there were frequent episodes of hypotension and bradycardia. NCS repeated after 1month of illness showed the same result.

By the 6thweek of hospitalisation, the patient started responding to painful stimulus by moving his head. After stabilisation of hemodynamic parameters, 4 exchanges were performed, wherein 6.26 litre of plasma were exchanged. All the 4 were of the intermittent variety. By the 10thweek of hospitalisation, there was partial opening of eyes to commands and flexion of interphalangeal joints of both upper limbs. The GCS improved to E4VTM6. 6 more sessions of plasma exchange were performed, of which 5 were continuous apheresis. Hypotension was experienced in two such continuous exchanges and the procedure had to be discontinued. 8.7 litre plasma was exchanged at the end of 6 exchanges. The type of plasma exchange performed depended on the availability of the kits. The details of the plasma exchanges have been enlisted in Table 1. On the 19thweek of hospitalisation, he could be weaned off the ventilator support. On the 25thweek, the tracheostomy tube was changed to speaking tracheostomy tube following which he could vocalise.

S.No

Type of Plasma Exchange

Volume of Plasma Exchanged (mL)

Plasma Volumes Exchanged

Adverse Reactions

A1

Intermittent

1407

0.4

Nil

A2

Intermittent

1825

0.5

Nil

A3

Intermittent

1700

0.48

Hypotension

A4

Intermittent

1888

0.54

Nil

B1

Intermittent

1070

0.3

Nil

B2

Intermittent

1800

0.51

Nil

B3

Intermittent

1890

0.54

Nil

B4

Continuous

1500

0.43

Nil

C1

Continuous

1000

0.28

Hypotension & Bradycardia

C2

Continuous

1600

0.45

Nil

C3

Continuous

1200

0.34

Nil

C4

Continuous

1900

0.54

Nil

C5

Continuous

1300

0.37

Hypotension

C6

Intermittent

1706

0.48

Nil

Total

21,786

Table 1 Details of the plasma exchanges performed

14 plasma exchanges were performed wherein 21.79 litre plasma were exchanged.

  1. Exchanges in the 4th week of illness
  2. Exchanges in the 8th week of illness
  3. Exchanges in the 16th and 17th weeks of illness.

His course in the hospital was complicated by 2 episodes of cardiac arrest, probably related to autonomic dysfunction. The ST-T wave changes noted were treated as Non-ST-Segment Myocardial Infarction (NSTEMI) as per attending Cardiologist. He had Ventilator Associated Pneumonia which was treated as per the antibiotic sensitivity report. At the time of discharge, the power in both upper limbs was 4/5 and in lower limbs 2/5. The Hughes score was 4 and GCS 15 (E4V5M6). He was advised continued rehabilitation in a physiatry till such time that he would be able to walk. The neurological parameters are tabulated in Table 2.

Neurological Parameters

Day 1

Day 3

10th Week

25th Week

GCS

E4VTM1

E1VTM1

E4VTM6

E4V5M6

Hughes Score

5

5

5

4

Muscle Power

UL- 0/5

UL-0

UL-2

UL-4

LL- 0/5

LL-0

LL-0

LL-2

Reflexes

Areflexia

Areflexia

Areflexia

Rt AJ +

Lt AJ +

Rt Plantar-F

Lt Plantar-F

Table 2 Improvements in the Neurological parameters3

UL: Upper Limb; LL: Lower Limb; Rt: Right; Lt: Left; AJ: Ankle Jerk; F: Flexor

Ethical clearance

Ethical clearance was obtained from the Institutional Ethics Committee

Discussion

The diagnosis of GBS in our patient was based on a rapidly progressive ascending, flaccid, areflexic quadriparesis with albuminocytological dissociation and ineluctable CMAPs on NCS. Fulminant GBS is a rare entity. Only 20cases have been reported in the literature. The occurrence rate is higher for men than for women.4 Out of the 12cases reported by Vargas et al.,4 albumino-cytological dissociation was found in 9 cases out of the 12. In the other three cases, cerebrospinal fluid was found to be normal or showed pleocytosis. Of the 12 cases, the therapeutic methods are described in only seven cases. Three patients died, two from cardiac arrest related to dysautonomia and one from a massive anterior myocardial infarction. Two patients showed poor recovery, with permanent disabling weakness. The others could walk with persistent minor problems.4–16 Our patient recovered with residual weakness in the lower limbs.

American Society for Apheresis (ASFA) classifies GBS under Category I, Grade 1A for therapeutic apheresis. Exchange of 1-1.5 plasma volumes for 5-7 procedures is recommended by ASFA for management of GBS but management of Fulminant GBS might not be feasible with the above dosage. The hemodynamic instability in the patients leads to early termination of the procedure thereby necessitating more number of procedures in total. GBS (Post IVIG) has been classified under Category III, Grade 2C.17 Our patient, after a failure with IVIG (30g OD for 5 days), responded well to plasma exchange.

In a study by Hadden et al.,18 the outcomes in response to plasma exchange or infusion of gamma globulin, or a combination of both treatments, did not differ.18 Chaves et al.1 reported a case of Fulminant Guillain Barré Syndrome who was treated first with 5days of IVIG 35g/day, with no response. Thereafter, he received 6 plasma exchanges. IVIG was repeated for 5 more days, followed by slow and steady improvement 2 months later. Fulminant GBS has a poor recovery rate and a high mortality, particularly in relation to dysautonomia. Nerve inexcitability on EMG, the need for ventilatory support for more than 1 month and severe rapidly progressive are bad prognostic features.19 Our patient had two episodes of cardiac arrest owing to dysautonomia from which he was successfully revived. Susuki et al.20 mentions that Axonal forms of GBS with positive Anti GM1 ganglioside antibodies respond well to a combination of Intravenous methyl prednisolone and IVIG20 but our patient (Anti GM1 borderline positive) responded to intensive plasma exchange.

Conclusion

Guillain-Barré Syndrome can, in rare cases, present with signs of coma and absent brainstem reflexes. This is an important variant of GBS to be considered, because it is potentially easy to make a misdiagnosis without proper evaluation and the potential consequences would be disastrous.4 It is essential to conduct electrophysiological tests, laboratory and imaging studies in patients with suspected brain death where a cause is not clearly determined.1 After evaluation, our patient was refractory to IVIG but responded to intensive plasma exchange. We recommend plasma exchange in such a scenario albeit a requirement of large number of cycles. The diagnosis and management of Fulminant GBS is a challenge and we recommend a multidisciplinary approach comprising of Neurologists, Transfusion Medicine specialist and Anaesthesiologist.

Acknowledgements

The authors would like to express profuse gratitude to Mr. Subhash Baiju, Terumo BCT for training the NMICU staff and Transfusion Medicine residents in Continuous apheresis. We would also like to thank the Nursing staff of NMICU and the staff of Dept of Transfusion Medicine for their continuous support.

Patient consent form

As per the guidelines of Institutional Ethics Committee, the consent of every patient is taken prior to publication.

Conflict of interest

The author declares no conflict of interest.

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