December 2008 no white pages.indd


ABSTRACT Varicella zoster infections are considered to be mild and ubiquitous infections predominantly affecting the paediatric
population. However, in adults and in specific groups of patients, such as those who are immunosuppressed, varicella infections can
be fulminant and life threatening.  We here present a case report of a young female patient with a normal immune system who had a 
fulminant varicella infection with multiorgan involvement.

Key words: Chickenpox; Herpes virus 3, human; Rhabdomyolysis; Disseminated intravascular coagulation; Pneumonia; Case report; 
Oman

Fulminant Varicella Zoster Infection with  
Multiorgan Involvement 

A Case Report 

*Sudheer P S Ahamed,1 Abdullah Balkhair,2 Rajan Krishnan2

SULTAN QABOOS UNIVERSITY MEDICAL JOURNAL 
NOVEMBER 2008, VOLUME 8, ISSUE 3, P. 339-343
SULTAN QABOOS UNIVERSITY©
SUBMITTED - 10TH FEBRUARY 2008
ACCEPTED - 29TH JUNE 2008

Varicella virus infection in humans can result in two distinct clinical syndromes:  chicken-pox and herpes zoster. Chickenpox, which 
develops after initial exposure to the virus, is a com-
mon trivial illness of childhood characterised by typi-
cal exanthem and a self-limited course. However, in 
adults, varicella can behave differently with much
more severity and involvement of different organ sys-
tems. 1, 2 This is more common in immunosuppressed
patients and those on chemotherapy.3 In the following 
case report,  we present a case of fulminant varicella 
infection with multiorgan involvement in an immuno-
competent young adult.

C A S E  R E P O R T

Our patient was a 22 year old, unmarried, female uni-
versity student; a non-smoker with no history of any 
significant medical illness.  The patient first presented
to her local health centre in Ibri, Oman with a history 
of sudden onset of severe back ache radiating to both 
lower limbs. She also had had a mild fever of 2 days 
duration. The patient was prescribed analgesic medi-
cations and discharged home from the primary centre. 
She presented the next day to the local hospital in Ibri 
with the characteristic rash of chickenpox involving 
her face and trunk. She continued to be febrile dur-
ing this presentation and also continued to have severe 
back ache. The patient had been exposed two weeks
previously to chickenpox in her family. She was seen 

1Department of Medicine, Armidale Rural Referral Hospital, Armidale, New South, Wales, Australia; 2Department of Medicine, Sultan Qaboos 
University Hospital, Muscat, Sultanate of Oman

*To whom correspondence should be addressed. Email: sudheerahamed@hotmail.com

أعضاء لعدة املصيب اخلاطف يّ  املعدي احلُماقِ ي اقِ النُّطَ يْروس الفَ مرض
حالة تقرير

كريشنان راجان باخلير، اهللا عبد احامد، سودير

الكبار، في لكن ــال. األطف تصيب ما غالبا والتي ــار االنتش ــعة واس املعدية اخلفيفة من األمراض احلماقي النطاقي الفيروس ــدوى ع ــر ــص: يعتب امللخ
في نقص من تعاني ال ــابة ش حلالة امرأة تقرير هنا ندرج للحياة. ومهددا خاطفا بالفيروس العدوى يكون املناعة، بنقص املصابني املرضى ــد ــة عن خاص

احلماقي. النطاقي بالفيروس جسدها في عديدة أعضاء أصيبت والتي املناعة

عمان. الرئة، التهاب يَة، األَوعِ لَ داخِ ُنْتَثِرُ امل ثُّرُ التَّخَ ات، الرُّبَيْدَ الَلُ انْحِ إنسان، ،٣ احلَأل فَيروسُ اق، الكلمات: احلُمَ مفتاح

C A S E  R E P O R T



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340

by the internist on call who made a clinical diagnosis 
of chickenpox. Routine investigations were done and 
showed elevated liver enzymes with a severely altered 
profile. Her chest radiograph was normal. The patient
was admitted to the Ibri Hospital and started on oral 
famcyclovir and intravenous ceftriaxone. The patient
continued to be febrile throughout her stay in this 
secondary care institution. The repeat liver function
tests showed a further rise and in her liver enzymes 
and  worsening coagulation with high prothrombin 
time (PT) and activated partial thromboplastin time 
(APTT). Her fibrin degradation product (FDP) value
was reported as very high at 640; however, there was no 
bleeding from any sites of the body. She received fresh 
frozen plasma (FFP) and the antibiotics and antiviral 
drug were continued. The patient was transferred the
next day to our institution, Sultan Qaboos University 
Hospital, for further care. On arrival, she was febrile, 
drowsy and severely tachycardic and tachypneoic with 
a pulse rate of 140 and respiratory rate of 30. Pulse 
oxymetry revealed her saturation to be 70% in room 
air. The polymorphic rash with vesicles and swabs was
still present, but limited to the face and trunk. The
chest examination revealed fine crepitations bilaterally.
There were no focal neurological deficits and abdomi-
nal examination did not reveal any organomegaly. The
liver span was found to be 7 cm clinically. The patient
was immediately admitted to the Intensive Care Unit 
and was started on noninvasive ventilation. Blood 
investigations and an urgent chest X-ray  were done 
revealing bilateral nonhomogenous haziness extend-
ing up to the mid zone. The liver functions revealed
very high enzymes with aspartate aminotransferase 
in the range of 5555u/l and alanine aminotransferase  
2225 u/l with normal bilirubin. The coagulation profile
showed gross derangement with high PT time, APTT 
and thrombin time values. A complete blood count 

revealed severe polymorphonuclear leucocytosis with 
thrombocytopenia. Her blood was sent for varicella 
serology and polymerase chain reaction (PCR) and 
also for serology for other viral haemorrhagic fevers 
such as dengue and Crimean-Congo.  The provisional
working diagnosis at this stage was fulminant varicella 
infection with pneumonia, hepatitis and disseminated 
intravascular coagulation with consumptive coagu-
lopathy along with super added sepsis. The patient
was started on acyclovir at a dose of 10 mg/kg 8 hourly 
and the antibiotics were upgraded to meropenem and 
amikacin. Cryoprecipitate, FFP and platelet concen-
trate were administered on suggestion of the haema-
tologist. The patient tolerated the noninvasive ventila-
tion for the next 24 hours, but on the second day of 
admission she desaturated and had to be intubated 
and mechanically ventilated. She also started to have 
fresh bleeding from the Foley catheter and the na-
sogastric tube. This was associated with a drop in her
haemoglobin. Her coagulation profile continued to
be deranged in spite of repeated cryoprecipitate and 
FFP transfusions. Her liver functions also continued to 
worsen. An ultrasound of her abdomen did not reveal 
any evidence of obstruction to the biliary tract or re-
duction in liver size. Vancomycin was added to cover 
the possibility of staphylococcal sepsis. Her varicella 
serology was negative for immunoglobulins (IgG and 
IgM) indicating the susceptibility for infection and the 
Varicella zoster virus polymerase chain reaction (VZV 
PCR) in her blood was reported as positive indicating 
ongoing viraemia. Other serological tests, including 
human immunodeficiency virus (HIV), dengue and
Crimean-Congo fevers were negative. A peripheral 
smear examination showed evidence of disseminated 
intravascular coagulation (DIC) and suggested sepsis, 
with no underlying haematological abnormalities. On 
the third day of admission, the patient continued to 

Complete Blood count Coagulation Profile Liver Function Tests Renal function tests

Haemoglobin(Hb)11.2gram/
Prothrombin Time (PT) 18.8 
seconds

Alanine amino transferase 
(ALT) 1278 U/L

Sodium (Na ) 132mmol/l

Neutrophil 80%
International Normalised Ratio 
(INR) 1.65

Aspartate aminotransferase 
(AST) 2550 U/L

Potassium (K+ ) 4.3mmol/l

Lymphocyte 16.4%
Activated Partial 
thromboplastin time (APTT) 
40 seconds

Alkaline phosphatase  
(ALP) 316 U/L

Urea  1.92 mmol/l (5.4mg/dl)

Platelets 235 cells/mm3
Bilirubin  
44.6 micromol/litre (27mg/dl)

Creatinine 38.89 micromol/litre 
(0.44mg/dl)

Table 1: Laboratory investigations at Ibri Hospital



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341

be sick and her ventilatory requirements rose signifi-
cantly. A repeat chest X-ray showed extension of the 
haziness bilaterally, especially on the left side. An ur-
gent pulmonology opinion was sought and the patient 
underwent an emergency bronchoscopy during which 
thick gelatin like mucous  plugs were removed from 
both sides. The lungs cleared significantly after this
procedure and the ventilatory requirements in terms 
of oxygen requirement and positive end-expiratory 
pressure (PEEP) started decreasing over the next few 
days. However, her coagulation continued to be ab-
normal for the next 3 days although the liver function 
tests showed a progressive decline in the enzymes, 
but with a rising bilirubin level. This bilirubin was
predominantly unconjugated and was thought to be a 
result of the ongoing haemolysis. A PCR performed 
on a bronchoalveolar lavage specimen revealed the 
deoxyribonucleic acid of the Varicella zoster virus. On 
advice of the haematologist, the patient continued to 
receive packed red blood cells concentrate, platelet 
concentrates, FFP and cryoprecipitates based on her 
coagulation profile. The patient started showing signs
of improvement in terms of coagulation profile by the
7th day of admission and over the next few days her FFP 
and cryoprecipitate requirements came down. Bleed-
ing from the catheter and nasogastric tube stopped by 
the 10th day and the ventilatory parameters showed a 

steady improvement. The liver function test also grad-
ually improved with normalization of her enzymes and 
bilirubin. She was extubated on the 14th day of admis-
sion, but had a resurgence of fever the next day and a 
repeat sputum culture grew Pseudomonas aeruginosa. 
She was continued on antibiotics and vigorous chest  
physiotherapy. She became afebrile two days later and 
was shifted to the ward on 17th day of admission. The
patient continued to improve steadily and was dis-
charged on the 21st day of admission. Her varicella 
serology was repeated in the second week and came 
out to be positive indicating an acute infection. A re-
peat VZR PCR was negative. The final diagnosis at dis-
charge was severe Varicella zoster infection with vari-
cella hepatitis, pneumonia and coagulopathy. 

D I S C U S S I O N

Varicella zoster  is a DNA virus belonging to the family 
of Herpes viridae and causes the two distinct clinical 
syndromes of varicella chickenpox and herpes zoster. 
The attack rate for varicella is approximately 90% in
susceptible individuals. In the majority of the cases, 
especially in children, varicella is a very mild infection 
characterised by skin lesions, low grade fever and ma-
laise. The skin lesions include maculopapules, vesicles
and swabs in various stages of development and ap-
pear on the trunk and face initially, before spreading 

Date Day-1 Day-2 Day-3 Day-5 Day-10 Day-12 Day-15 Day-17

Compelete Blood Count

Haemoglobin
Total Count
Neutrophil
Lymphocyte
Platelets

10.9
30.9
76.6
18.7
75

6.7
23.2
79
16.8
76

8.3
27.7
88.4
8.7
90

8.4
16.1
77.1
11.3
32

8.2
9.9
61.2
18.8
72

10.2
10.2
72
11.4
203

11.2
12.2
74.9
10.6
494

9.9g/dl 
10.7cells/mm3
74.9%
13.4%
495 cells/mm3

Liver Function Test

ALT
AST
ALP
Albumin
Bilirubin
Protein

2524
5555
357
280
530.1
520

2327
4360
416
270
649
490

860
2958
185
310
906.3
540

245
540
160
280
2907
500

87
89
161
300
1333
600

67
49
155
320
1060
630

49U/L
49 U/L
170 U/L
350 G?L
974 Чmol/litre
710 g/l

Coagulation profile

PT
INR
APTT
Thrombin Time

18.2
1.77
76
54.6

14.6
1.42
58
59.4

13
1.25
48
34.6

11
1.05
39
24

11.1
1.06
38
13.8

11.4
1.09
36
13.8

11 seconds
1.05
32.7 seconds
13.9 seconds

Varicella serology -ve IgM+

ALT = alanine aminotransferase; AST = aspartate aminotransferase; ALP = alkaline phosphatase; PT = prothombin time;  INR = international 
normalized ratio; APTT = activated partial thromboplastin time

Table 2: Results of laboratory investigations on the patient



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to other parts of the body. The patient is infectious 48
hours before the onset of the rash and throughout the 
vesicle development until all the vesicles are crusted. 
The severity of rash varies from person to person. Im-
munocompromised patients tend to have a more se-
vere rash and are more prone to visceral involvement.3 

Our patient was a 22 year old healthy female student 
and the reason for the fulminating  nature of her vari-
cella remains unclear. The diagnosis of varicella was
confirmed serologically as well as with VZV PCR. She
initially had severe back ache, which is not a charac-
teristic presentation of varicella. The cause for this
symptom could be a myeloradiculopathy which has 
been reported as a neurological complication of vari-
cella infection. 3 The rapidity of clinical deterioration
and involvement of multiple organ systems of the body 
was the most striking feature in this patient. The pa-
tient had a clear chest X-ray initially, only developing 
features of pneumonia on the 4th day of admission,  fol-
lowed by rapid respiratory deterioration needing ur-
gent intubation. Special emphasis has to be placed on 
the role of bronchoscopy in these patients, which will 
help in clearing the thick gelatin like mucous plugs, 
especially in cases of nonresolving pneumonias. The
severe coagulopathy leading to disseminated intravas-
cular coagulation needed constant support with cryo-
precipitate and FFP along with platelet concentrates. 
The use of appropriate antibiotics to prevent bacterial
infections, especially by streptococcus and staphyloco-
ccus, also helped in controlling the features of sepsis in 
this patient. Our case emphasizes the fact that varicella 
infection in immunocompetent adults can be  severely 
complicated and potentially fatal. Various studies have 
shown the rate of  visceral involvement in varicella in-

fection in the immunocompromised to be around 30-
50% and, in the absence of treatment, 15% of cases can 
be fatal.1, 4 However, there are no authoritative studies 
to show the magnitude of visceral involvement or fa-
tality with varicella infection in immunocompetent in-
dividuals. In a recent study conducted in Saudi Arabia, 
the complication rate in varicella infection was found 
to be 1.5% and the overall fatality rate was found to 
be 0.05%.5 Another study in Germany, done to assess 
the epidemiological pattern of varicella complications, 
revealed the majority as neurological with encepha-
litis leading the list.6 This was followed by infectious
complications; in particular infection by streptococcus 
pyogenes was associated with a worse outcome. Other 
known complications of varicella include myocardi-
tis, hepatitis, rhabdomyolysis with renal failure, acute 
glomerulonephritis and arthritis.7, 8 The possibility of
these complications and the unpredictability of the se-
verity of varicella infection in adults indicates the need 
for early treatment with antivirals and immunisation 
in seronegative adults.9

C O N C L U S I O N

Our case demonstrates the fact that varicella infections 
can be life threatening even in  immunocompetent 
adult patients. The pattern of involvement of multiple
systems is also of interest and made the management 
of this patient quite challenging. The importance of
supportive care  and significance of early bronchos-

Figure 1: Gelatinous plugs from the lung being 
removed bronchoscopically

Figure 2: Chest X-ray on the day of admission



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copy for the removal of gelatinous mucous plugs  in 
the management of varicella pneumonia needs to be 
stressed in addition to antiviral therapy. Our case also 
rightly raises the question of the importance of vacci-
nation against varicella virus infections at least in pa-
tients with high risk of developing a severe disease.10

R E F E R E N C E S

1. Whitley RJ. Varicella zoster virus infections. In: Harri-
sons Principles of Internal Medicine. 16th ed. New York: 
McGraw Hill, 2006. p. 1042-1045.

2. Hollensten U, Thalahamer F, Burggmann H. DIC and
rhabdomyolysis in fulminant varicella infection - case 
report and review of literature. Infection 1998; 306-
308.

3. Arvin. A. Ageing, Immunity and Varicella zoster virus-
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4. Brunnel PA. Varicella zoster infections. In: Cecil Text 
book of Medicine. Philadeplhia: WB Saunders & Co, 
1985. p. 88

5. Almuneef M, Memish ZA, BalkeyHH, Altoaiby B, 
Helmy M. Chickenpox complications in Saudi Arabia: 
Is it time for routine varicella vaccinations? Int J Inf Dis-
eases 2006; 10:156-161.

6. Ziebold C, Vonkries R, Lang R, Weigl J, Schmitt HJ. 
Severe complications of varicella in previously healthy 
children in Germany - A 1 year survey. Paediatrics 
2001;108:E79

7. Al Langawi M, Al-Marri MR, Al Soub H. Rhabdomy-
olysis associated with varicella infection. Int J Clinical 
Practice 2001; 55:484-485.

8. Cameron JC, Allan G, Johnston AGF. Severe complica-
tions of chickenpox in hospitalized children in UK and 
Ireland. Arch Dis Childhood; 2007; 92:1051-1052.

9. Gershon AA, Katz SL. Perspective on varicella vaccine. 
J Infect Dis 2008; 1:197.

10. Varicella vaccine information. Centre for Disease Con-
trol. From www.cdc.gov.  Accessed December 2007.