Since 2016 we have been running a joint microbiology / urology clinic for recurrent UTI. This is a summary of what we do, and the what it's done for first 36 patients. Main conclusions are :
- This is a group of patients who have been poorly served with high morbidity
- Bearing witness to the impact on their lives is the first step in developing a therapeutic alliance
- Attention to basics is important. This includes drinking plenty. It does not include advice on how to wipe.
- Self start strategies with patient defined course length works well for most people
- There are a few really complex patients who need ongoing support and this includes a different approach by the laboratory to do this - eg. next day sensitivities; interpreting mixtures in a way that is helpful; working up low numbers of "non pathogenic" organisms; looking for "atypical" organisms
This is what has happened :
- 24 patients with self start
- 18 better (less than 3 MSUs in year after clinic)
- 13 with follow up data from primary care
- 11 patients with prolonged high dose abx
- 4 better
- 9 with follow up data from primary care
- 1 patient continued prophylaxis
- 1 better
- 1 with follow up data from primary care
In patients with primary care data :
- 1978 DDDs of abx in year before clinic appt; 586 DDs in year after
- 324 consultations in year before; 169 in year after
- 187 UTI consultations in year before; 51 in year after
E coli most predominant pathogen
Some probable genuine mixtures
Some poorly defined
Some with no positive specimens
Although
most patients have pyuria in specimens in the
year before clinic, this is not universal, and may not be
consistent over time
Complex anatomy main reason for failure.
eg. cystoplasty; vaginal tapes; trauma
Some patients appear to have problems
with prostate but not clearly defined - no abscesses
Underlying conditions may be an issue -
particularly if immunosuppressed / steroids
Patient
engagement with early self start may be an issue
About
50% of patients who fail lost to follow up
Significant
number with complex micro work closely with lab
results to define each infection and optimise Rx using early self start
One patient with RA appears to have had
no problems since RA under control
Prescribing data on 3 of 5 complex patients
working with lab on early self start shows reduction in abx usage from 287 DDDs
to 67 DDDs.
What we do
Effect
on life
- How often between episodes?
- Is start of episode clear? What are main symptoms?
- Completely well or not between episodes?
- Nocturia often useful as a gauge of impact
- Flow symptoms
- In men – prostatitis and orchitis symptoms
Microbiology
- Proven with positive MSUs?
- Same organism?
- If same organism then more likely to consider prolonged high dose combination eradication
- E coli?
- D mannose may be effective
- Proteus?
- May be particularly important to maintain acidic pH and look for stones
If
MSUs are negative :
- is there pyuria?
- Have fastidious organisms or non-typical organisms been looked for?
- Is this non-infective? Eg. interstitial cystitis.
Note
that not all patients have pyuria, although an absence of pyuria makes
diagnosis of infection more questionable.
If
repeated mixed cultures, or other diagnostic uncertainty, then get higher
quality specimen
- Peezy
- In out catheter
Other laboratory tests
Inflammatory
markers are not generally helpful and we don’t measure
Creatinine
- Evidence of pyelonephritis (Flank pain / rigors)
- may push away from nitrofurantoin
- may push towards more interventional approach
Anatomical
problems
All
patients need USS to assess for clear structural abnormalities and residual
volume
If
significant residual volume then this needs managing.
Most
patients probably need cystoscopy at some point, although low pick up, and may be
able to avoid if normal USS and no visible or non-visible haematuria between
episodes.
Stents
and stones are hard to manage – will be colonised.
Pneumaturia
requires urgent investigation
Catheters
Is
patient catheterised or intermittent catheterisation?
Why?
Things
to try :
Review technique especially if ISC.
Consider
prophylactic abx at change and change frequency
Washouts
Intravesicular gentamicin
Maintenance of mildly acidic pH
Coated catheters
Precipitating
factors
Sex
- Post coital voiding
- Post coital prophylaxis (guided by previous cultures; nitrofurantoin as default)
Periods
- Consider prophylaxis at this time
- Possibly explore options for suppressing menstrual cycle
Anything
else (eg. dehydration, especially if fear of drinking before going out or at
night)
Encourage
to drink at least 2 litres of water per day – Fill 2 jugs with water in
morning)
Aggravating
factors that may need addressing
Constipation
Diabetes
Iron
overload states
Steroids
General
approaches to management
Tell
patients to drink plenty. At least 2 litres per day. Fill jugs in morning and
make sure finished by evening.
In
post menopausal women, topical oestrogens should be tried for at least 6/12
Double
voiding
Post-coital
voiding
Explore
alternative antibiotic management options, with a view to stopping prophylaxis,
and/or reducing regular visits. Options include :
- Prescribe standby antibiotics and provide patients with redtop tube to submit MSU if symptomatic; and then immediately start a course of antibiotics (based on previous sensitivities – discuss with micro if complex) and continue until the day after symptoms have resolved.
- If related to sexual activity, consider post-coital prophylaxis.
- Prescribe a prolonged treatment course (at least 3/12) of two antibiotics based on previous results. This option may be good if consistently same organism / antibiogram. Probably less good if not consistent. Options include
- Cefalexin 500mg QDS
- Nitrofurantoin 100mg MR BD
- Trimethoprim 200mg BD
- Azithromycin 500mg OD
If
breakthrough infections then continue baseline antibiotics and add new agents
based on MSU results
Consider
hipuric acid for 6/12. Prolonged courses probably should be avoided due to
theoretical risk of bladder cancer.
If
recurrent E coli consider D mannose (not if diabetic)
Consider
intravesicular gentamicin if limited oral options and self-catheterises
Consider
urinary pH monitoring both as a means of diagnosis and an aid to antibiotic
optimisation (note particularly gentamicin favours high pH; nitrofurantoin
lower pH).
Consider
dietary modification. Generally promote vegetarian diet. Consider things like
high dose vitamin C.
Ensure
aggravating conditions managed appropriately, especially diabetes
Consider
bladder washouts with eg. SubyG if ISC.
Consider
cystistat (although rarely do this now)
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