Case report

A rare case of COVID-19 vaccine- induced thrombotic 
thrombocytopaenia (VITT) involving the veno- 
splanchnic and pulmonary arterial circulation, from a 
UK district general hospital
Huma Asmat,1 Folusho Fayeye,2 Hameed Alshakaty,3 Jay Patel1 

SUMMARY
A 47- year- old woman presented with a headache to the 
acute medical unit, 10 days after receiving AstraZeneca 
vaccination for COVID-19. Brain imaging was normal, 
but her blood tests showed a remarkably low platelet 
count, mildly deranged liver function tests and a high 
D- dimer. Further within her hospital admission, she 
developed right- sided abdominal pain and chest pain, 
and subsequent cross- sectional imaging confirmed 
a small segmental pulmonary embolism, and an 
acute portal vein thrombosis extending to the splenic 
and superior mesenteric veins. On the basis of her 
investigations, she was diagnosed as a case of vaccine- 
induced thrombotic thrombocytopenia and was treated 
with intravenous immunoglobulins. In a time where there 
is a strategic goal to vaccinate the global population 
from COVID-19 to inhibit the spread of infection and 
reduce hospitalisation, this particular clinical scenario 
emphasises the need of all clinicians to remain vigilant 
for rare complications of the COVID-19 vaccination.

BACKGROUND
The WHO declared the novel corona virus (COVID-
19) outbreak as a global pandemic on 11th March 
2020, following the first identified case in Wuhan, 
China in late December 2019.1 2

Vaccines  offer  a  glimmer  of  hope  in  the  fight 
against  COVID-19,  with  many  types  of  vaccines 
becoming 
increasingly  available  for  use.  One 
such  type,  the  Oxford–AstraZeneca  chimpanzee 
adenovirus- vectored  vaccine  ChAdOx1  nCoV-19 
(AZD1222)  provides  particular  hope  for  equi-
table  access  for  low- income  and  middle- income 
countries.  This  is  in  comparison  to  the  high  cost 
of  mRNA- focused  vaccines  that  require  storage 
in  ultra- low  temperature  freezers  and  ultimately 
impractical for its use in many countries.3

The  AstraZeneca  vaccine  was  approved  by  the 
Medicine  and  Healthcare  products  Regulatory 
Agency (MHRA) on 30th December 20204 and was 
licensed for use in European countries by the Euro-
pean Medical Agency on 29th January 2021.5

In  late  February  2021,  cases  of  unusual  throm-
botic events in combination with thrombocytopenia 
were  emerging,  in  patients  following  vaccination 
with  the  AstraZeneca  vaccine.  As  a  result,  many 
European  countries  initially  suspended  the  use  of 
the  AstraZeneca  vaccine  while  further  analysis  of 
the safety of the vaccine was conducted.6–8

We  present,  below,  a  case  of  an  AstraZeneca- 
induced  vaccine- induced  thrombotic  thrombocy-
topenia  (VITT)  involving  two  separate  systemic 
circulations,  resulting  in  direct  hospitalisation. 
We  highlight  our  radiological  findings  and  the 
immunological- based  management  of  her  throm-
botic disease.

CASE PRESENTATION
A  47- year- old  woman  with  a  comorbidity  only  of 
the occasional migraine was invited to receive her 
first  dose  of  the  AstraZeneca  vaccine  at  the  end 
of  March  2021.  She  received  the  vaccine  into  the 
deltoid muscle of her right arm.

Post  vaccination,  she  reported  no  symptoms  up 
until  day  5,  when  she  then  developed  right- sided 
periorbital  pain,  which  progressed,  gradually,  to 
a  generalised  headache  with  mild  photophobia, 
neck  stiffness  and  lower  back  pain.  There  was  no 
evidence of a neurological deficit, fevers or a new 
rash suggestive of meningitis. Sumatriptan did not 
alleviate  her  symptoms.  Following  a  review  by  an 
out- of- hours  general  practitioner  almost  10  days 
after her vaccination, she was referred to the acute 
medical team.

Further  clinical  history  highlighted  no  personal 
or family history of thromboembolic disease. There 
was  no  history  of  miscarriages.  The  patient  had  a 
negative pregnancy urine test, and was not on any 
regular  medications,  in  particular  to  contraceptive 
medications. There was no history of recent travel. 
Finally, she did not smoke tobacco or recreational 
drugs.

INVESTIGATIONS
Her  blood  tests  demonstrated  the  following:  (1) 
severe  acute  thrombocytopenia,  with  a  platelet 
count  of  13  ×  109/L;  (2)  elevated  D- dimer  of 
>5000 ng/mL  and  (3)  mildly  deranged  liver  func-
tion tests with alanine transaminase of 57 U/L and 
alkaline  phosphatase  of  138 U/L.  She  had  normal 
coagulation  profile  (international  normalised  ratio 
(INR) of 1 and an activated partial thromboplastin 
time  (APTT)  of  34.2).  Her  haemoglobin,  white 
blood cell count, renal function tests and albumin 
were  within  normal  parameters.  Her  reverse- 
transcription PCR testing via nasopharyngeal swab 
returned negative for COVID-19.

Considering  her  headache,  a  CT  head  was 
requested  and  showed  no  intracranial  pathology. 

1

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1Gastroenterology, Bedford 
Hospital NHS Trust, Bedford, UK
2Bedford Hospital NHS Trust, 
Bedford, UK
3General/Acute Medicine, 
Bedford Hospital NHS Trust, 
Bedford, UK

Correspondence to
Dr Jay Patel;  
 jay. patel@ bedfordhospital. 
nhs. uk

Accepted 2 September 2021

© BMJ Publishing Group 
Limited 2021. No commercial 
re- use. See rights and 
permissions. Published by BMJ.

To cite: Asmat H, Fayeye F, 
Alshakaty H, et al. BMJ Case 
Rep 2021;14:e244223. 
doi:10.1136/bcr-2021-
244223

Asmat H, et al. BMJ Case Rep 2021;14:e244223. doi:10.1136/bcr-2021-244223

Case report

Figure 1  MRI- venogram: highlighted clear patency of cerebral vessels. 
A, anterior; P, posterior.

Figure 2  CTPA axial image showing a filling- defect in the right lower 
lobe pulmonary artery consistent with a pulmonary embolism.

Investigations (bloods tests), treatment and response to treat-

ment are summarised in table 1.

OUTCOME AND FOLLOW-UP
The  patient  completed  an  outpatient  upper  gastrointestinal 
endoscopy, which excluded oesophageal or gastric varices. She 
will remain under the dual care of hepatology and haematology 
teams.

Anticoagulation will be continued for a minimum of 3 months, 
with  repeat  cross- sectional  imaging  of  her  chest  and  abdomen 
scheduled in 3 months’ time.

The  full  thrombotic  screen  that  was  sent  additionally 
(including  anticardiolipin,  lupus  anticoagulant  antibodies  and 
thrombophilia screen), prior to IVIG treatment and use of anti-
coagulation, has come back as negative.

HIT antibodies came back as positive with percentage activa-

tion=31.57% (cut- off for positive reactions >8%).

DISCUSSION
We describe a rare case of an immune- mediated severe throm-
bocytopenia  and  thrombosis  involving  the  splanchnic  and 

Further cross- sectional imaging via a MRI- venogram (figure 1) 
confirmed  no  evidence  of  a  cerebral  or  dural  thrombosis. 
Fundoscopy  examination  was  normal.  A  lumbar  puncture 
was  muted,  but  not  performed,  considering  her  profound 
thrombocytopaenia.

Considering  her  haemostasis  parameters,  a  discussion  with 
our haematology team ensued and she was quickly diagnosed as 
having a vaccine- associated thrombocytopenia. A PF4 antibody 
assay  (ELISA)  heparin- induced  thrombocytopenia  (HIT)  assay 
was requested, and this returned as positive.

On day 5 of her admission, she developed acute right hypo-
chondrial  abdominal  pain  and  lower  chest  pain.  This  resulted 
in an urgent triple phase scan of her liver, in addition to a CT 
pulmonary angiogram (CTPA).
Subsequent  cross- sectional 

imaging  highlighted  a  small 
segmental right- sided pulmonary embolism (PE) (figure 2), and 
a completely occluded, dilated portal vein (figures 3A and 4A) 
with  acute  thrombosis  extending  into  the  superior  mesenteric 
vein  (figure  4B)  and  splenic  vein  (figures  3  and  4B),  and  the 
development  of  peri- portal  collaterals.  There  was  no  evidence 
of  underlying  cirrhosis,  with  a  preserved  liver  volume.  There 
were no arterial enhancing liver lesions to suggest a primary liver 
tumour. There was no evidence of small or large bowel ischemia. 
Her final diagnosis was VITT.

TREATMENT
Considering  her  immunological- driven  thrombotic  disease,  she 
was commenced on intravenous immunoglobulins (IVIGs) at a 
dose of 0.5 g/kg, over 2 days (days 3 and 5 of admission), and she 
received further IVIG on days 6 and 8 of admission.

Her platelet count improved rapidly, with a concomitant fall in 
her D- dimer levels. Symptomatically, she also improved in terms 
of her headache and abdominal pain. She was later commenced 
on  Fondaparinox  (day  7  of  admission)  and  then  switched  to 
Apixaban  (day  9  of  admission)  for  further  management  of  her 
thromboembolic  disease.  She  was  discharged  after  12  days  of 
admission.

2

Asmat H, et al. BMJ Case Rep 2021;14:e244223. doi:10.1136/bcr-2021-244223

Figure 3  CT triple phase liver axial images showing (A) portal venous 
phase: distended and non- opacified portal vein (portal vein thrombosis) 
and (B) splenic vein thrombosis.

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Case report

clinically  resembles  a  severe  HIT,  but  without  the  prior  use  of 
heparin.8 11

The hallmark of VITT is the presence of antibodies directed 
against  PF4/heparin  complexes.  By  their  Fc  domains,  these 
immune  complexes  bind  to  FcγRIIA  on  the  surface  of  plate-
lets  and  thus  cross- link  these  receptors  and  induce  platelet 
activation.7

Cases  emerging  have  shown  that  patients  are  presenting 
5–28 days  after  vaccination  and  are  characterised  by  severe 
thrombocytopenia, raised D- dimer levels, occasional low fibrin-
ogen  levels  and  progressive  thrombosis  at  unusual  sites.  There 
is also evidence of the presence of antibodies to PF4, which can 
only be identified by ELISA HIT assay.

Current guidance provided by the Expert Haematology Panel 
(EHP;  affiliated  with  the  British  Society  of  Haematology), 
focused on the management of COVID-19 VITT cases through 
past  experience  of  managing  similar  (but  not  AstraZeneca- 
related)  vaccine- associated  conditions  and  the  theoretical  risks 
and  benefits  of  interventions.  IVIG  is  recommended  to  be 
commenced on an urgent basis at a dose of 1 g/kg (divided into 
2 days  if  needed),  irrespective  of  the  degree  of  thrombocyto-
penia,  and  reviewing  the  clinical  course  closely.  Further  IVIG 
may  be  required  balancing  bleeding  and  thrombotic  risk,  with 
ongoing discussion with the haematologist. Platelet transfusion 
should  be  avoided.  Once  platelet  counts  improve  >30×109/L, 
anticoagulation with non- heparin- based therapies such as direct- 
acting anticoagulants, argatroban, fondaparinux or danaparoid 
should be commenced. Steroids can be considered, in particular 
if there is a delay in giving IVIG.8 Plasma exchange may also be 
considered.

Anticoagulation should be continued for at least 3 months. All 
cases  require  formal  reporting  to  the  EHP  and  Public  Health 
England and a yellow card needs to be filled for the Medicines 
and Healthcare products Regulatory Agency (MHRA).11

As discussed above, VITT involves development of antibodies 
against PF4/heparin complexes. When these immune complexes 
bind  to  FcγRIIA  on  the  surface  of  platelets,  platelet  FcγRIIA 
stimulation  leads  to  downstream  activation  of  Bruton  tyrosine 
kinase (Btk) as a decisive signalling pathway for subsequent steps 
of platelet activation. IVIG, which is a current approved treat-
ment, inhibit platelet activation by shielding from FcγRIIA.

Philipp  von  Hundelshausen  et  al7  proposed  in  their  recent 
article  that  inhibitors  of  Btk,  which  are  used  for  B- cell  malig-
nancies,  may  become  another  therapeutic  option  for  VITT, 
as  they  are  expected  to  target  multiple  pathways  downstream 
of  FcγRIIA- mediated  Btk  activation,  including  effective  inhi-
bition  of  platelet  aggregation,  dense  granule  secretion,  P- se-
lectin  expression  and  platelet- neutrophil  aggregate  formation 

The patient herself expressed a wish to provide a statement for 
this report.

I was not expecting that I will get such severe side effects 
from COVID-19 vaccination. I heard about the side effects but 
I thought it is very rare and would not happen to me as I am 
healthy. It has made me very scared for myself, and also for my 
family. The scariest part was that I did not get many symptoms 
except for the headache and I kept on thinking for first 5 days 
that I should not go to hospital, as it was not severe and seem 
insignificant. I would like people to know that one has to be 
vigilant after vaccination.

3

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Figure 4  CT triple phase liver: coronal images showing (A) dilated 
portal vein with complete thrombosis in the main branch, (B) splenic 
vein thrombosis and (C) normal appearing IVC and normal patency of 
the hepatic veins IVC, inferior vena cava.

pulmonary  vessels  after  the  AstraZeneca  vaccine  (ChAdOx1 
nCoV-19).

This  case  highlights  the  importance  of  recognition  and 
management of rare complications in patients receiving the new 
COVID-19 vaccinations.

There  are  no  previous  case  reports  of  COVID-19  vaccine- 
related  splanchnic  vein  thrombosis  within  the  UK;  however, 
similar  cases  are  reported  in  other  parts  of  the  world.  Schultz 
et al9 reported case series of five patients in Norway with VITT 
after first dose of ChAdOx1 nCoV-19 adenoviral vector vaccine 
(AstraZeneca).  These  patients  presented  with  venous  throm-
bosis of unusual sites and concomitant thrombocytopenia within 
7–10 days after receiving the first dose of the AstraZeneca vacci-
nation.  All  patients  had  positive  antibodies  to  platelet  factor 
4  (PF4)–polyanion  complexes  with  no  previous  exposure  to 
heparin. Four of five patients had severe cerebral venous throm-
bosis with intracranial haemorrhage, and the outcome was fatal 
in three of them. One of the patient presented with thrombosis 
of  splanchnic  circulation  involving  portal  vein,  splenic  vein, 
azygos vein and hemiazygos vein. These five cases occurred in a 
population of >130 000 vaccinated persons.

Another  such  case  was  reported  in  Austria,  whereby  a 
51- year- old  woman  developed  PE  and  thrombus  formation  in 
the left internal iliac and common iliac veins, with extension into 
the inferior vena cava, after 11 days of receiving the AstraZeneca 
vaccination.  This  was  associated  with  thrombocytopenia.  HIT 
antibodies were not done in her case but the clinical picture fits 
with VITT.10

VITT  following  vaccination  against  SARS- CoV-2  with  the 
AstraZeneca  vaccine  is  an  immune- mediated  condition,  that 

Table 1  Blood tests, dates of administration of IVIG and 
anticoagulation and summarises the response of treatment

Day of 
admission

IVIG

Anticoagulation

D- dimer

ALT

ALP

Platelets 
(x 109/L)

Day 1

Day 2

Day 3

Day 4

Day 5

Day 6

Day 7

Day 8

Day 9

Day 10

Day 11

Day 12

 

 

 

 

 

 

 

 

 

 

 

 

0.5 g/kg

0.5 g/kg

0.5 g/kg

0.5 g/kg

Fondaparinox

Fondaparinox

Apixaban

Apixaban

Apixaban

Apixaban

13

16

19

19

26

77

132

190

263

282

105

115

100

88

59

46

38

29

27

154

167

188

219

198

317

419

380

>5000

>5000

>5000

3375

2150

2423

1621

ALP, alkaline phosphatase; ALT, alanine transaminase; IVIG, intravenous immunoglobulin.

>5000

57

138

Patient’s perspective

Asmat H, et al. BMJ Case Rep 2021;14:e244223. doi:10.1136/bcr-2021-244223

Case report

Learning points

 ► For general and acute physicians, the most important 

take home message is simply awareness of the condition. 
Mild- to- moderate constitutional symptoms such as fever, 
lethargy, myalgia and headache are common for up to 48 
hours post vaccine. New or intense headache, symptoms 
of raised intracranial pressure (such as nausea, vomiting, 
visual changes or reduced consciousness), breathlessness, 
chest pain, abdominal pain, back pain, or leg pain, 
petechiae, prolonged bleeding or easy bruising all need to be 
investigated.

 ► A strong recommendation is made to involve the 

haematology team early, to help guide management of 
suspected vaccine- induced thrombotic thrombocytopenia. 
Intravenous immunoglobulin is the first- line treatment and 
further doses may be needed if the platelet count continues 
to fall or D- dimer rise. Close follow- up will also be required 
with these patients.

 ► Always report any cases identified using the yellow card 

system online.

 ► Finally, if VITT is diagnosed or suspected, patients should not 

receive a second dose of the AstraZeneca vaccine.

stimulated  by  FcγRIIA  cross- linking.  Moreover,  C- type  lectin- 
like receptor CLEC-2- mediated and GPIb- mediated platelet acti-
vation;  the  interactions  and  activation  of  monocytes;  and  the 
release of neutrophil extracellular traps, as encountered in HIT, 
could all be attenuated by Btk inhibitors (Btki). In short, several 
activation  mechanisms  at  the  centre  of  VITT  pathophysiology 
inhibited the Btki. Therefore, Btki might be regarded as a safe 
alternate for off- label use in selected cases of VITT.

Acknowledgements  We thank Dr Murty Vusirikala, Consultant Radiologist, 
Bedford Hospital, for providing the radiological images.As Bedford Hospital and 
Luton and Dunstable Hospital have merged together to become one trust, we have 
used the Luton Hospital Fellowship code.

Contributors  The case was diagnosed and managed by gastroenterology and 
acute medial team, with JP and HA being the consultants and HA and FF being the 
registrars for the respective teams. HAs: she designed and wrote first draft of the 
manuscript including summary, introduction, case and discussion. She also complied 
the table of results and treatment and edited the manuscript as per her supervisor 
(JP) guidance and added images. Moreover, she spoke to the patient and took her 

personal statement and got her consent. She is also responsible for submitting the 
report to the BMJ. JP pointed out the case to be reported and supervised each step. 
He did critical revision of the manuscript, edited and approved the final version. 
He also provided the images by liaising with the radiologist. FF: he contributed to 
manuscript writing. HAl: he supervised and contributed to editing the manuscript 
and approved the final approval. All four authors approved the final version.

Funding  The authors have not declared a specific grant for this research from any 
funding agency in the public, commercial or not- for- profit sectors.

Competing interests  None declared.

Patient consent for publication  Obtained.

Provenance and peer review  Not commissioned; externally peer reviewed.

This article is made freely available for use in accordance with BMJ’s website 
terms and conditions for the duration of the covid-19 pandemic or until otherwise 
determined by BMJ. You may use, download and print the article for any lawful, 
non- commercial purpose (including text and data mining) provided that all copyright 
notices and trade marks are retained.

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Asmat H, et al. BMJ Case Rep 2021;14:e244223. doi:10.1136/bcr-2021-244223

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