antibiotic prophylaxis in sickle cell disease baba inusa · some facts sickle cell spleen 1....
TRANSCRIPT
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Baba InusaPaediatric Haematology, Evelina London Children’s Hospital King’s Health Partners Women
and Children’s Health Faculty of Life Sciences & Medicine King’s College London
Antibiotic prophylaxis in Sickle cell disease
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Outline
1. Spleen and SCD - increased risk of infection
2. Epidemiology of bacterial infection in SCD Strep pneumoniae and Salmonella Osteomyelitis
3. The case for Penicillin prophylaxis
4. Cochrane Review /Recommendations
5. The unfinished business in SCD
a) When to withdraw prophylaxis
b) Other pathogens
6. Single Centre Audit
7. Recommendation
Disclaimer: My remit is Antibiotic prophylaxis
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Some Facts Sickle Cell Spleen
1. Children and adults with sickle cell disease have increased susceptibility to severe bacterial infections
2. Main risk factor is functional hyposplenism/asplenism
3. Spleen has combined function of immune defence and quality control
4. SCD children are essentially hyposplenic by 5 years of age
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Splenic function• Phagocytic filter removing damaged cells
and micro-organisms and is involved in antibody production
• Red pulp - filtering function
• White pulp – adaptive immunity
• Marginal or perifollicular zone – innate and adaptive roles
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Splenic function – red pulp
• Spleen filters ~5% of cardiac output each minute
• Much of the blood entering the spleen drains directly into the parenchymal of the red pulp
• Here the blood cells and blood-bourne bacterial are in close and prolonged contact with resident macrophages – phagocytosis of damaged RBCs and pathogens
• Only some bacteria are recognised
• Some require coating by complement components which interact with receptors
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Asplenia
1. Effect on both innate and adaptive immune response
2. Poor clearance of bacteria directly from circulation
3. Delay in adaptive immune responses
4. Specific difficulty clearing encapsulated bacteria
5. Resulting in rapid progression of bacterial infection to severe disease
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Further immunodeficiency in SCD
1. SCD associated with a background of complement dysregulation caused by genetic susceptibility or autoantibodies
2. an inverse correlation between complement activity and the number of crises suffered by SCD patients
3. Compliment activation in Sickle cell is increased with vaso-occlusive crisis, haemolytic reactions
4. Zinc deficiency may affect 60—70% of SCD patients; Zinc is known to be important for immune function may contribute susceptibility to infection
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Bacterial Infection ins sickle cell disease
• Fever is common in SCD patients presenting to health care setting – bacterial, viral, parasitic infection and other causes
• Actual incidence of invasive bacterial infection is not well defined; varies with
• Geographical setting (developed vs undeveloped) e.g. 1.1% of all febrile children presenting A+E (USA) vs 28% Ugandan study
• Age Infection highest in <3years (0.6 per 100 person years vs 10 per 100 in >10yrs)
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Encapsulated bacteriaStrep pneumoniae story
• Increased susceptibility to invasive infection with encapsulated bacteria –commonest is pneumococcus (don’t forget H influ, N meningitides)
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Encapsulated bacteriaStrep pneumoniae story
1. Pre 1990s developed world data: invasive pneumococcal infection 7-10 per 100 person years
2. Case fatality rate as high as 35%
3. 2 things have made a huge difference4. Prophylactic penicillin5. Vaccination – specifically conjugate vaccines
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USA multi-centre
Children 3-36 months old
SS pattern
Randomised to 125mg Pen V bd vs 50mg Vit C bd
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• USA multi-centre
• Children 3-36 months old
• SS pattern
• Randomised to 125mg Pen V bd vs 50mg Vit C bd
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Trial terminated 8 months early after 15 episodes of
pneumococcal septicaemia (3 deaths) – 13 placebo vs 2 Rx
arm
8 of these events in children < 2 yrs of age
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Current Recommendations
(AAP)
1. Penicillin Prophylaxis: SS, SbºThalassemia
• 2 months to 3 years: 125 mg PO BID
• Over 3 years: 250 mg PO BID
• When to discontinue is controversial
2. Penicillin Prophylaxis: SC and Sb+ Thalassemia
• SC warrants penicillin prophylaxis similar to SS
• Sb+ Thalassemia: penicillin prophylaxis can be safely discontinued at 5 years
• Routine use in infants and children is controversial
3. Special Circumstances
• History of repeated sepsis, surgical splenectomy
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CID 2007
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Prophylactic antibiotics for
preventing pneumococcal
infection inchildren with sickle
cell disease. Cochrane Database
of Systematic Reviews 2017.
Persons with sickle cell disease (SCD) are particularly susceptible to infection. Infants and very young children are especially vulnerable. The 'Co-operative Study of Sickle Cell Disease' observed an incidence rate for pneumococcal septicaemia of 10 per 100 person years in children under the age of three years.
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Objectives: To assess the
effects of antibiotic
prophylaxis against
pneumococcus in children with
SCD in relation
1. incidence of infection;
2. mortality;
3. drug-related adverse events (as reported in the included studies) to the individual and the community;
4. the impact of discontinuing at various ages on incidence of infection and mortality.
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Types of outcome
measures
Primary outcomes
1. Number of participants developing Streptococcus pneumoniae (S pneumoniae) infection, confirmed with cultures
2. Deaths
Secondary outcomes
1. Adverse drug effects
2. Antibiotic-resistant organisms isolated
3. Requirement for other courses of antibiotics
4. Compliance with antibiotic prophylaxis, measured by counting doses and urine samples
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Five trials were identified by the
searches, of which three trials
(880 children randomised) met
the inclusion criteria.
1. All of the included trials showed a reduced incidence of infection in children with SCD (SS or S𝓑o) receiving prophylactic penicillin.
2. In trials which investigated initiation of penicillin on risk of pneumococcal infection, the odds ratio was 0.37 (95% confidence interval 0.16 to 0.86) (two trials, 457 children) (low-quality evidence), while for withdrawal the odds ratio was 0.49 (95% confidence interval 0.09 to 2.71) (one trial, 400 children) (low-quality evidence).
3. Adverse drug effects were rare and minor.
4. Rates of pneumococcal infection were found to be relatively low in children over the age of five.
5. The evidence examined suggests that prophylactic penicillin significantly reduces risk of pneumococcal infection in children with homozygous SCD
6. Further research may help to determine the ideal age to safely withdraw penicillin and how commonly bacteria develop that are resistant to treatment and how clinically important this is.
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Invasive pneumoccoccal diseasesRetrospective review, USA, 2002-2014 (Martin OO, Pediatr Blood Cancer 2018)
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The infection preventive care among patients with SCD in developed countries does not easily translate to the adoption of these recommendations globally, which must take into account the local epidemiology of infections, available vaccines and population-specific vaccine efficacy, environment, health care behaviours, and cultural beliefs, as these are all factors that play a complex role in the manifestation of SCD and the prevention of infectious disease morbidity
Obaro SK, Iroh Tam PY. PBC 2016
Preventing Infections in Sickle Cell Disease: The Unfinished Business
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Invasive pneumococcal disease: key messages
• Repeated parental information: fever in young children → urgent medical examination
• Start antibiotics targeting Pneumococcal infections before results of biological analyses
Should we revisit our current recommendations regarding the duration of penicillin prophylaxis in children with SCD?
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Pneumococcal vaccine
Currently 2 types of vaccine –
Polysaccharide ‘PPV’ (23 valent)
conjugate vaccine ‘PCV’ (13 valent)
Polysacharride vaccine has been around for decades
Conjugate vaccines only since 2007
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Pneumococcal vaccine
Despite PPV and pen V prophylaxis pneumococcal breakthrough infection incidence was still ~3-4 per 100 patient years <3 years
Feb 2007 – PCV 7
licensed
Highly successful in all
reducing incidence of IPI in
all children
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Serotype unique to PCV13
Serotypes contained in both vaccines
Serotypes unique to PNEUMOVAX 23
Pneumococcal vaccination in SCD
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Salmonella story
Invasive infection with gram negative organism is common
SCD is specifically associated with infection with non-typhoidal salmonella
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Salmonella storyInvasive infection with gram negative organism is common
SCD is specifically associated with infection with non-typhoidal salmonella
WHY??
related to areas of devitalised mucosa in the GI tract lead to increased bacterial translocation
Impairment in phagocytosis and bacterial clearance in SCD
Salmonella may target dendritic cells and macrophages favouring dissemination to BM and spleen
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Salmonella story
How common is Salmonella infection in UK practice?
Is it relevant to our SCD population?
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Salmonella in SCD: A single centre study
• GSTT data over 40 years (1969-2008)
• 14,432 bacteraemic episodes 95 (0.7%) SCD
• Of these 69.5% were community acquired bacteraemia
• 4 organisms accounted for 80% of all SCD bacteraemias
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This time period
spans both
introduction of Pen
V prophylaxis and
PPV and PCV
Salmonella 3rd
commonest
12 cases at GSTT
in 40 years
Don’t know number
of febrile SCD
admission
episodes over this
time period
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• Total of 174 episodes of salmonella bacteraemia (12 SCD 162 non-SCD)
• All 12 SCD were non-typhoidal compared to 82/162 (51%) of non-SCD
• Closer look at 11 SCD case• age range 2-41 yrs
• 4 had Hx tropical travel in preceding 3 months
• Absence of diarrhoea
• 4/11 had bony focus for infection
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• Further London (north mid) study 2010 ‘bacterial infection in SCD’
• 88 SCD Children <16 years old admitted with fever
Bacteraemia 3.4%
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Predictors of bacterial infection
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Take home message
• Suspected bacterial infection in up to 40% of SCD admission (children)
• Bacteraemic infection accounts for <5% of SCD admissions
• Salmonella one of commonest pathogens in bacteraemic illness but not only pathogen
• Salmonella is associated with bone and joint infection in 40-50% cases
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Osteomyelitis and SCD• Remarkable lack of good epidemiological data
in literature
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Osteomyelitis and SCD• We looked at admission from
June 2009 – Oct 2012 at GSTT (adult and paed)
• 1220 sickle cohort at GSTT
• 1660 admissions
• 701 (42%) bone issue
• 19 (3%) BJI
SCD database1660 admissions
1 Jun 2009-31 Oct 2012
701 (42%)Acute bone problem
651 (93%)Vasocclusive crisis
31 (4%)Elective
orthopaedic intervention
19 (3%)INFECTION
959 (58%)Other problem
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• Trigger for Ix was clinical suspicion e.g. on going bony pain in association with persistently raised fever, WCC or CRP
Method of diagnosis
0
2
4
6
8
10
12
Micr
obiol
ogica
l
MRI a
lone
MRI +
BC
MRI +
tissu
e
USS alon
e
XR alon
e
XR+USS
Nu
mb
er
of
pati
en
ts
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• Causative organism was only identified in 6/19 cases
Organism Specimen
Bordetella holmseii
Joint aspirate (prosthetic hip
joint)
Escherichia coli Bone, pus & aspirate (femur)
Escherichia coli Bone (tibia)
Salmonella dublin Blood culture
Salmonella enteritidis
Bone, deep tissue & aspirate
(humerus)
Klebsiella pneumoniae Bone (prosthetic hip joint)
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• Oct 2003 – Dec 2010 (7 years)
• Radiology information system cross checked with SCD database
• Chronic OM excluded
• 41 SCD with D/C dx of acute OM
• Compared to 58 SCD with Dx of VOC
PLOS 2013
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Microbiological information – limited info presented in this study
• 2 bacteraemic on admission – Mycoplasma sp and Morganella sp
• 18/41 proceeded to surgical incision and drainage
• 3 grew salmonella on drainage
• No data presented on remaining 36 patients
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Advocating the role of Ultrasound as first line Ix in children
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Summary
• The spleen or lack of function
• Importance of Strep pneumo in SCD and success in reducing invasive disease
• High incidence of invasive Salmonella infection but not the only cause of OM
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Protocol for prevention of invasive pneumococcaldisease
Conjugate vaccine must precede polysaccharide vaccine since polysaccharide vaccine might induce hyporesponsiveness.
• 4 doses of conjugated vaccine between 2 and 15 months of agefollowed by a polysaccharide vaccine at 2 and 7 years
• Daily prophylactic penicillin
Martin OO et al. Pediatr Blood Cancer 2018
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Current UK vaccination schedule for children
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Recommended Immunization Schedule for Sickle Cell Disease
Pneumococcus Meningococcus and Haemophilus Influenza
Influenzae type b
Under 2 years Routinea Routinea AnnualAge 2-5 years (fully immunized) Single dose PPV Booster does given as the Hib/MenC Annual
vaccineAge 2-5 years (unvaccinated or Two doses of PCV Two doses of the Hib/MenC Annualpartially vaccinate) given 2 months apart, vaccine given 2 months apart
followed 2 monthslater by PPV
Age > 5 years (fully vaccinated) Single dose PPV Two doses of the Hib/MenC Annualgiven 2 months apart
Age > 5 years (fully unvaccinated) Single dose PPV Two doses of the HIB/MenC Annualvaccine given 2 months apart
Reinforcing immunization PPV every 5 years MenC vaccine every 5 years, Hib Annualvaccine not currently recommended
Note: Schedule summarized from Salisbury D, Ramsay M, Noakes K, Immunization against infectious disease (The Green Book). London: Department of Health; 2006.78 National childhood immunization in most developing countries does not currently include Hepatitis B, Hib or meningococcal vaccines. These should be strongly encouraged for children with SCD. In endemic settings consideration should also be given for immunization with typhoid vaccine.Hib, Haemophilus Influenzae type B; MenC, meningococcus group C; PCV, pneumococcal conjugate vaccine, PPV, pneumococcal polysaccharide vaccine.aRoutine UK immunization schedule.