Case report

Coeliac artery and splenic artery thrombosis 
complicated with splenic infarction 7 days following 
the first dose of Oxford vaccination, causal 
relationship or coincidence?
Sareesh Bandapaati,1 Hemababu Bobba,1 Mitrakrishnan Rayno Navinan2 

SUMMARY
The novel coronavirus SARS- CoV-2 became a global 
pandemic in late 2019, and is still ongoing in 2021 
causing significant morbidity and mortality. The advent 
of vaccinations heralded the turning of the tide. The 
Oxford jab, a vector- based vaccine was favoured due to 
its low cost and ease of storage. However, its potential 
association with thromboembolic adverse events resulted 
in controversy and disrupted its roll- out and use. The 
aetiopathogenesis of these thromboembolic events 
and its association with the Oxford vaccine are still 
speculative and uncertain, more so in the background 
of SARS- CoV-2 infection being highly thrombogenic in 
its own right. This paper presents a case of an otherwise 
healthy 50- year- old Caucasian man who developed acute 
abdominal pain 7 days following the first dose of Oxford 
vaccine and was found to have coeliac and splenic artery 
thrombosis complicated with splenic infarction.

BACKGROUND
Corona viruses (CoV’s) have resulted in pandemics 
across  Asia  and  the  Middle  East  over  the  last  two 
decades, for example, SARS- CoV-2 and Middle East 
respiratory  syndrome- CoV.  The  novel  coronavirus 
SARS- CoV-2 which originated in late 2019 became 
a global pandemic and has caused significant world-
wide morbidity and mortality, with the global death 
toll reaching 3 million by April 2021.1 The advent 
of  different  vaccinations  heralded  the  turning 
of  the  tide  as  messenger  RNA,  protein  subunit 
and  vector-  based  vaccines  showed  good  immune 
response against SARS- CoV-2. The Oxford vaccine 
(ChAdOx1  nCov-19)  which  is  based  on  a  chim-
panzee adenovirus vector with inclusion of genetic 
sequences of the spike protein in SARS- CoV-2 has 
shown  to  elicit  good  immune  response  with  an 
efficacy of 81.3% with two doses spaced 12 weeks 
apart.2 It became a forerunner among its competi-
tors due to its ease of storage, low cost per dose and 
was being globally deployed as it had been proven 
efficacious  and  safe  by  phase  III  clinical  trials.2 
However,  concerns  have  been  raised  regarding  its 
safety after a number of reports of thromboembolic 
events across Europe following its use.3 The Euro-
pean  Medicine  Agency  (EMA)  recently  acknowl-
edged  the  potential  causal  relationship  between 
the  Oxford  vaccine  and  thromboembolic  events.4 
Cerebral  vascular  accidents  and  cardiopulmonary 
embolic  complications  together  with  deep  vein 

thrombosis  make  up  most  of  these  noted  events.5 
Only one prior splenic infarction was recorded by 
AstraZeneca’s  postmarketing  adverse  event  safety 
database.5  We  report  a  case  of  coeliac  and  splenic 
artery  thrombosis  with  associated  splenic  infarc-
tion a week following the first dose of the Oxford 
vaccine.

CASE PRESENTATION
A  previously  healthy  50- year- old  Caucasian  man 
presented  with  sudden- onset  left- sided  abdominal 
pain of 6 hours’ duration to the emergency depart-
ment.  The  pain  was  sharp  in  nature  and  persisted 
and  worsened  throughout  the  day  to  an  intensity 
of  8/10  with  poor  response  to  oral  paracetamol, 
necessitating hospital admission. He had been well 
prior to his presentation on the same morning with 
no  other  gastrointestinal  or  urological  symptoms. 
He denied constitutional symptoms as well. He had 
not  experienced  any  recent  respiratory  symptoms 
or  fever  and  had  not  had  COVID-19  previoulsy  . 
Other than smoking 5–10 cigarettes per day for a 
decade, he had no significant past medical, surgical 
or family history of relevance and was not on any 
routine  medication,  prescription  or  off- label.  He 
denied any history of palpitations. He had received 
the first dose of the Oxford vaccine 7 days prior to 
his current presentation.

The  general  examination  was  normal.  He  was 
afebrile  with  a  temperature  of  36.3°C.  His  pulse 
was 73 beats per minute and regular with a blood 
pressure of 125 mm Hg systole and 62 mm Hg dias-
tole.  His  on- air  saturation  was  99%.  His  respira-
tory  and  cardiovascular  system  examination  was 
normal.  The  abdomen  on  inspection  appeared 
normal with no asymmetry or distension. It was soft 
on  palpation  with  tenderness  being  noted  on  left 
flank  and  lower  quadrant  on  deep  palpation  with 
no rebound tenderness. Percussion note was normal 
with  auscultation  revealing  only  bowel  sounds  of 
normal frequency.

INVESTIGATIONS
His  12- lead  electrocardiograph  demonstrated 
normal sinus rhythm. The initial venous blood gas 
demonstrated  a  marginally  elevated  serum  lactate 
level of 2.45 mmol/L (0.2–1.80) with a pH of 7.335 
(7.35–7.45).  The  whole  blood  analysis  revealed 
primarily  an  isolated  leucocytosis  with  elevated 
count  of  18.0×109/L  (4–11)  with  predominant 

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1Emergency Department, 
Kettering General Hospital, 
Kettering, UK
2Cardiology Department, 
Kettering General Hospital, 
Kettering, UK

Correspondence to
Dr Sareesh Bandapaati;  
 sareesh. bandapaati@ nhs. net

Accepted 4 July 2021

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

To cite: Bandapaati S, 
Bobba H, Navinan MR. BMJ 
Case Rep 2021;14:e243799. 
doi:10.1136/bcr-2021-
243799

Bandapaati S, et al. BMJ Case Rep 2021;14:e243799. doi:10.1136/bcr-2021-243799

Case report

Table 1  Baseline laboratory parameters

Investigations and reference ranges

Full blood count

 White blood cells (x109/L (4–11))
 Neutrophil (x109/L (7.5–11))
 Lymphocytes (x109/L (1.5–4.0))
 Haemoglobin (g/dL (11-15))

 PCV (L/L (0.4–054))
 Platelet counts (x109/L (150 000–450 000))

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

 

Renal functions

 Serum sodium (mmol/L (135–145))

 Serum potassium (mmol/L (3.5–5.1))

 Serum creatinine (μmol/L (44–97))

 

 Blood urea (mmol/L (2.5 to 7.1))
 EGFR mL/min/1.73 m2
Inflammatory markers

 

 C reactive protein (<5 mg/dL)

Coagulation screen

 aPTT (23.0–31.0 s)

 PT (9.5–13.5 s)

 TT (13.7–19 s)

 Fibrinogen (1.8–3.5 g/L)

Liver functions

 Bilirubin (0–21 umol/L)

 Alanine transaminase (<41 IU/L)

 Albumin (35–50 g/L)

 Alkaline phosphate (30–130 U/L)

 Total protein (60–80 g/L)

 Amylase (28–100 IU/L)

Thrombotic screening

 Anticardiolipin Ab IgG (GPL U/mL (<10))

 Anticardiolipin Ab IgM (MPL U/mL (<10))

 B 2 glycoprotein IgG Ab (u/mL (<10))

 B 2 glycoprotein IgM Ab (u/mL (<10))

 D –dimer ((ug/L) <500)

 Fibrinogen (g/L (1.8–3.5))

 JAK2 V617F Mutation

Viral screening

 Hepatitis B surface antigen

 Hepatitis C antibodies

 Anti HIV ½

Lipid profile

 SARS- CoV-2 RT polymerase

 Cholesterol (<5.2 mmol/L)

 Triglycerides (0.8–2.3 mmol/L)

 HDL (0.9–1.6 mmol/L)

 Non- HDL

Values

18

15.3

1.9

167

0.469

340

139

4.2

61

4.6

>90

5

21.5

12

15

3.3

10

39

49

105

70

62

0.8

2.7

<1

<3

3026

3.3

Negative

Negative

Negative

Negative

Negative

4.9

1.9

0.8

4.1

Figure 1  Contrast- enhanced CT mesenteric artery angiogram 
(indicated by arrow) demonstrates a thrombus in the proximal coeliac 
axis just before giving off the left gastric artery branch.

test was negative. In view of the disproportionate level of symp-
toms,  an  urgent  contrast- enhanced  CT  of  the  abdomen  and 
pelvis was done which demonstrated a non- occlusive thrombus 
in  the  coeliac  trunk  with  50%  luminal  obstruction,  extending 
into the distal splenic artery with concomitant regional splenic 
infarct with no bowel ischaemia and no associated renal abnor-
mality or lymphadenopathy. To further clarify this, a selective CT 
mesenteric angiogram was done which confirmed the thrombus 
in  the  proximal  coeliac  axis  (figure  1)  with  non- opacification 
of left gastric artery, and thrombus involving the splenic artery 
(figure  2)  causing  lower  pole  splenic infarction  (figure  3).  The 
D- dimer  levels  were  checked  in  retrospect  to  imaging  findings 
immediately and was grossly elevated with a value of 3026 ug/L 
(<500).  Subsequent  investigations  with  anticardiolipin  anti-
bodies  and  beta-2  glycoprotein  antibodies  were  found  to  be 
negative  (table  1).  Transthoracic  two  dimensional  echocardio-
gram did not reveal left ventricular thrombus and normal valve 
morphology was noted.

TREATMENT
The  patient  was  given  analgesia  in  the  form  of  oral  codeine 
60 mg,  intravenous  morphine  5 mg  along  with  intravenous 
ondansetron  4 mg  for  pain  relief.  Following  the  discovery  of 
coeliac artery and splenic artery thrombus and after haematology 
consult, he was initiated on anticoagulation with subcutaneous 
low- molecular- weight  heparin  (LMWH)  of  125 mg  as  platelet 
counts remained normal (and the likelihood of anti- PF4/heparin 

aPTT, Activated partial thromboplastin time; EGFR, Estimated glomerular filtration rate; 
GPL, IgG Phospholipid Units; HDL, High- density lipoproteins; MPL, IgM Phospholipid 
Units; PCV, Packed cell volume; PT, Prothrombin time; TT, Thrombin time.

neutrophilia  of  15.3×109/L  (2–7.5).  The  platelet  count  was 
normal with a value of 340×109/L (150–450). The rest of the 
investigations including liver functions, renal functions, coagu-
lation  profile(except  for  a  marginally  prolonged  aPTT)  and  C 
reactive protein were normal (table 1).

Serum  fibrinogen  level  was  normal  with  a  value  of  3.3 g/L 
(1.8–3.5). The urine was dipped and was negative for leukocytes, 
blood,  protein  and  nitrites.  His  SARS- CoV-2  nasal  and  throat 
swab reverse transcription polymerase chain reaction (RT- PCR) 

2

Bandapaati S, et al. BMJ Case Rep 2021;14:e243799. doi:10.1136/bcr-2021-243799

Figure 2  Contrast- enhanced CT mesenteric artery angiogram 
(indicated by arrow) demonstrates a thrombus in the splenic artery.

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Case report

et al, in Norway and Denmark it was noted that the overall risk 
of venous thromboembolism to be overall doubled, with dispro-
portionately higher risk in certain subtypes, for example, CVST 
by as much as 20- fold.14 As this population mainly composed of 
healthcare staff, this could very well be an underestimation when 
extrapolating to the general population as a whole.

The  exact  aetiopathogenesis  resulting  in  these  thrombotic 
events  following  the  Oxford  vaccine  are  still  under  investiga-
tion  and  are  speculative.  However,  certain  associations  are 
being  more  frequently  observed.  Greinacher  et  al,  in  a  paper 
in  preprint,  postulates  the  role  of  anti- PF4/heparin  antibodies 
and a mechanism similar to heparin- induced thrombocytopaenia 
with an alternate serological profile as a potential cause for the 
Oxford vaccine to cause thrombosis in those with simultaneous 
presence  of  thrombocytopaenia  complicated  with  a  thrombo-
embolic  event.15  Additionally,  in  certain  cases  the  presence  of 
thrombocytopaenia  associated  with  bleeding  complicated  with 
thromboembolism  questions  the  potential  role  of  disseminated 
intravascular  coagulation  in  its  aetiology.11  A  novel  alternate 
mechanism has also been suggested by Kowarz et al, in a paper 
in  pre- print  who  hypothesise  that  after  vaccination,  a  coded 
protein  precipitates  thromboembolic  events  when  it  binds  to 
ACE-2 expressed in endothelial cells in the blood vessel. They 
named this ‘vaccine- induced COVID-19 mimicry’.16 Regardless 
of the mechanism, this potential association of thromboembolic 
events following the use of the Oxford vaccine has eroded the 
faith  of  the  public  and  governments  alike  and  resulted  in  the 
disruption of the vaccine roll- out in Europe and Canada as some 
nations ceased its deployment pending further investigation.3 13 
The European Medicine Authority and the WHO both initially 
independently  impressed  on  the  lack  of  causal  association  of 
these events due to the Oxford vaccine and encouraged its use as 
the overall benefit of the vaccine outweighed its risks.3 Further-
more,  an  independent  analysis  of  the  Danish  National  patient 
registry by Østergaard et al, comparing the incidence of throm-
boembolic  events  in  the  prevaccine  era  and  following  the  use 
of  Oxford  vaccine  roll- out  concluded  that  the  use  of  Oxford 
vaccine  did  not  increase  the  relative  incidence  of  thromboem-
bolic events in comparison to the expected incidence among the 
general population.12

It is not possible to unequivocally associate an adverse event 
following  immunisation  to  the  vaccine  directly.  The  event  can 
be  due  to  the  vaccine  product  itself  or  quality  of  the  product. 
It  can  be  due  to  inappropriate  handling  of  the  product  or  can 
even be anxiety related. Otherwise it can be completely coinci-
dental. To arrive at a conclusion there has to be an assessment at 
individual and the population level with data analysis in a struc-
tured pathway as specified by the WHO.17 18 However, a recent 
update  by  the  EMA  in  April  2021  suggested  a  causal  relation-
ship between thrombotic events in the presence of low platelet 
count  as  plausible,  while  still  re- enforcing  that  the  overall  the 
benefit  outweighs  the  risk.4  This  has  led  to  recognition  of  the 
phenomenon  of  SARS- CoV-2  vaccine  induced  immune  throm-
botic  thrombocytopaenia.19  Based  on  available  evidence  an 
initial  guidance  was  released  where  time  since  vaccination 
(between  4  and  28  days  since  vaccination)  and  low  platelet 
counts  (<150×109/L)  were  the  key  determining  factors  for  at 
risk individuals. This was followed by a release of a broad guid-
ance  for  investigating  and  overall  management  of  gastrointes-
tinal  manifestations  secondary  to  vaccine- induced  thrombosis. 
The  guidelines  however  suggest  to  establish  definitive  throm-
bocytopaenia  before  proceeding  with  further  haematological 
and imaging investigations in pursuit of thromboembolic events 
suspected  of  being  vaccine  induced.  The  role  of  D- dimer  and 

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Figure 3  Contrast- enhanced CT mesenteric artery angiogram 
(indicated by arrow) demonstrates splenic infarction of the lower pole.

antibody mechanism being the primary pathology was less likely). 
He was reviewed by the surgical team and the vascular team and 
as he remained clinically stable it was decided for conservative 
management.  He  was  observed  for  3 days  as  an  inpatient  and 
with no further evolution of symptoms he was discharged with 
a plan for follow- up with haematology and vascular team as an 
outpatient with the continuation of LMWH at the same dose.

OUTCOME AND FOLLOW-UP
Following discharge, he was asymptomatic. He was reviewed in 
the vascular surgical clinic and he remains well to date.

DISCUSSION
Coeliac artery thrombosis is very uncommon. It can occur due 
to  embolic  phenomenon  by  atrial  fibrillation,  or  thrombosis 
due to atherosclerosis, vasculitis, malignancies and coagulation 
disorder.6 7 Advanced age is considered a risk for this phenom-
enon. The spectrum of presentation can also be highly variable, 
for example, from dyspeptic symptoms to acute abdomen, and 
symptoms  depend  on  the  extent  of  ischaemic  territory  and 
collateral  perfusion.8  9  This  can  lead  to  misdiagnosis,  stressing 
the  importance  of  imaging  in  its  accurate  diagnosis.8  Below 
we consider the possible mechanisms that may have led to this 
phenomenon  which  includes  vaccine  mediation,  thrombotic 
event  due  to  asymptomatic  post- COVID-19,  inherent  risk 
factors including atherosclerosis resulting in plaque rupture and 
prothrombotic states and discuss their individual merits in our 
patient.

Based  on  the  updated  release  of  the  COVID-19  vaccine 
summary of yellow card reporting on the 9th of June 2021 by 
the  Medicine  and  Healthcare  products  Regulatory  Authority, 
390  thromboembolic  events  were  documented  across  the  UK 
following  the  use  of  AstraZeneca  vaccine.  The  affected  age  of 
these patients ranged from 18 to 93 years with most being less 
than 60 years. The events were also relatively more notable in 
females  (53%).10  The  spectrum  of  events  was  extensive  and 
included cerebrovascular accidents, acute myocardial infarction, 
deep  vein  thrombosis,  pulmonary  embolism,  multiple  throm-
bosis and cerebral venous sinus thrombosis (CVST).5 11 12 Coeliac 
artery thrombosis following AstraZeneca vaccine has only been 
reported rarely.5 The mean age for CVST was 46 years and for 
all  other  thromboembolic  events  combined  it  was  54  years.10 
Thromboembolic  events  have  been  noted  even  during  initial 
clinical trials of the Oxford vaccine, although the number was 
overall lower in the vaccinated group without an increased risk of 
bleeding.13 But in a population based cohort study by Pottergård 

Bandapaati S, et al. BMJ Case Rep 2021;14:e243799. doi:10.1136/bcr-2021-243799

Case report

fibrinogen levels have been relegated to a second tier for confir-
mation  rather  than  being  used  for  initial  primary  workup.20  21 
However, the mechanism and relationship of the Oxford vaccine 
causing thromboembolic events in the population in the absence 
of thrombocytopaenia is still uncertain and remains to be eluci-
dated  despite  the  number  of  reported  incidences.  Our  patient 
had a normal platelet count, but grossly elevated D- dimer levels 
in the presence of thrombosis. This brings into question the role 
of extending the spectrum of initial screening mechanisms when 
clinical  suspicion  is  high  to  ensure  a  clinical  diagnosis  is  not 
missed,  given  the  relative  lack  of  information  on  the  different 
potential  mechanisms  that  maybe  leading  to  thromboembolic 
phenomenon following use of the Oxford vaccine.

It  is  also  established  that  COVID-19  infection  is  prothrom-
botic. An extensive spectrum of arterial and venous thrombotic 
and thromboembolic events have been documented in literature 
during  acute  infections,  even  when  adequately  anticoagulated, 
impressing on the role thrombogenesis plays in the aetiopatho-
genesis of COVID-19.22 A case report by Del Nonno et al, docu-
ments  an  asymptomatic  patient  who  was  initially  positive  and 
subsequently repeatedly tested negative who thereafter went on 
to develop a fatal arterial thrombotic event a month following 
initial diagnosis,23 further stressing the role of thrombogenicity 
and its duration of impact following COVID-19 even in asymp-
tomatic patients. Thus, it is not unreasonable to question these 
episodes of thrombo- embolism as a spectrum of post- COVID-19 
syndrome or period,11 occurring incidentally in the postvaccina-
tion context. Our patient had no symptoms preceding his vacci-
nation period and was well. Furthermore, he was rapid antigen 
negative on admission and when subsequently tested he was also 
SARS- CoV-2 RT- PCR negative thus making an active infection 
unlikely and asymptomatic post- COVID-19 period less likely as 
well.

The  other  potential  differential  which  could  have  caused 
coeliac  artery  thrombosis  in  our  patient  was  atherosclerotic 
plaque  rupture  as  this  is  an  established  risk  factor  for  this 
phenomenon.  Our  patient  had  no  other  risk  factor  predis-
posing him to atherosclerosis other than a history of smoking. 
He was not a known vasculopath nor did he have any sugges-
tive  symptoms  and  he  had  no  prior  cardiac  symptoms  of  rele-
vance.  Furthermore,  coeliac  artery  thrombosis  secondary  to 
this aetiology is usually in the setting of chronic atherosclerosis, 
which casts doubt of it being the primary aetiopathogenesis in 
our  patient.24  Another  alternate  consideration  is  an  intrinsic 
prothrombotic state. Our patient had no family history and his 
prothrombotic  screen  was  negative,  making  an  intrinsic  cause 
less likely. But he did have a mildly shortened aPTT, which is a 
recognised risk factor for mostly venous but also arterial throm-
bosis.25 26 However, this hypothesis and association has also been 
challenged.27 Furthermore, our patient never had prior venous 
embolic events and incidences of low aPTT being the sole cause 
for coeliac artery thrombosis have not been previously reported 
making this association rather unlikely although not impossible.
Our  patient  had  overlapping  risk  factors  for  both  coeliac 
trunk  thrombosis  (age  and  potential  atherosclerosis)  as  well  as 
postvaccine thromboembolism (age and timeline of vaccination) 
and hence falls into the spectrum of a candidate who could be 
considered as at risk for thromboembolic complications due to 
the AstraZeneca vaccine. However a definitive causal relation-
ship cannot be proven in our case report other than to speculate 
based on the association between the time of vaccine adminis-
tration and the thromboembolic presentation in this otherwise 
healthy subject. Regardless, there is a scarcity of data in terms of 
demographics  of  the  populace  affected  by  these  events  (which 

may be skewed by the mechanism of vaccine roll- out dependant 
on  age  and  priority),  the  time  since  vaccination  to  symptom 
onset  and  the  varying  presentation  of  the  clinical  picture  due 
to  lack  of  reporting  or  under- recognition.12  Thus,  it  would  be 
prudent to document these thromboembolic events in literature 
as it would hopefully contribute to greater understanding of this 
potential phenomenon in future.

LIMITATIONS
Given the infancy of the state of vaccine roll- out and the knowl-
edge on potential spectrum of postmarketing adverse events, it is 
still too early to either associate or disregard this arterial throm-
boembolic  event  as  associated  with  the  Oxford  vaccine.  As  of 
now, it is still not definitive in its association given the absence 
of  thrombocytopaenia,  which  is  currently  the  only  acknowl-
edged  scenario  where  the  Oxford  vaccine  has  been  found  to 
cause  thrombo- embolic  events.  However,  guidance  is  rapidly 
changing  and  greater  recognition  of  these  rare  incidences  may 
aid in achieving a better understanding of the potential incidence 
and  spectrum  of  thromboembolic  events  following  the  use  of 
Oxford vaccine.

Patient’s perspective

I initially thought it was trapped wind or constipation. After 
hearing the diagnosis I thought it could be due to the vaccine. 
I felt better after receiving the enoxaparin and the pain rapidly 
subsided. I am feeling better postdischarge, though I still feel 
anxious.

Learning points

 ► Risk stratification and clinical assessment should be used for 
postvaccine presentations suggestive of thromboembolism. 
However, if the presentation is highly suggestive, clinical 
judgement should take precedence to broaden the scope of 
initial investigation so as to arrive at a diagnosis while still 
considering alternate aetiologies.

 ► There is a possible causal relationship between the Oxford 

vaccine and thromboembolic phenomenona. However, the full 
spectrum of mechanisms causing this complication need to be 
better understood and further defined in order to streamline 
the choice of screening and diagnostic investigations and to 
decide on appropriate initial management.

 ► The spectrum of postvaccine thromboembolism both in 
its manifestations and presentation can be extensive. 
Reporting of such clinical events will help further our overall 
understanding of this phenomenon.

Acknowledgements  We would like to thank the nurses and health care team at 
Kettering General Hospital for their dedication and passion towards patient welfare.

Contributors  HB and SB diagnosed the clinical condition. All authors contributed 
for the care of the patient. MRN and SB researched and drafted the manuscript. All 
authors read, edited and approved the manuscript.

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, 

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Bandapaati S, et al. BMJ Case Rep 2021;14:e243799. doi:10.1136/bcr-2021-243799

Case report

non- commercial purpose (including text and data mining) provided that all copyright 
notices and trade marks are retained.

AstraZeneca ChAdOx1- S in Denmark and Norway: population based cohort study. 
BMJ 2021;373:n1114.

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Bandapaati S, et al. BMJ Case Rep 2021;14:e243799. doi:10.1136/bcr-2021-243799