- Research article
- Open Open Peer Review
Routine monitoring and assessment of adults living with HIV: results of the British HIV Association (BHIVA) national audit 2015
BMC Infectious Diseasesvolume 17, Article number: 619 (2017)
The clinical care of people living with HIV changed fundamentally as a result of the development of effective antiretroviral therapy (ART). HIV infection is now a long-term treatable condition. We report a national audit to assess adherence to British HIV Association guidelines for the routine investigation and monitoring of adult HIV-1-infected individuals.
All UK sites known as providers of adult HIV outpatient services were invited to complete a case-note review and a brief survey of local clinic practices. Participating sites were asked to randomly select 50–100 adults, who attended for specialist HIV care during 2014 and/or 2015. Each site collected data electronically using a self-audit spreadsheet tool. This included demographic details (gender, ethnicity, HIV exposure, and age) and whether 22 standardised and pre-defined clinical audited outcomes had been recorded.
Data were collected on 8258 adults from 123 sites, representing approximately 10% of people living with HIV reported in public health surveillance as attending UK HIV services. Sexual health screening was provided within 96.4% of HIV services, cervical cytology and influenza vaccination within 71.4% of HIV services. There was wide variation in resistance testing across sites. Only 44.9% of patients on ART had a documented 10-year CVD risk within the past three years and fracture risk had been assessed within the past three years for only 16.7% patients aged over 50 years.
There was high participation in the national audit and good practice was identified in some areas. However improvements can be made in monitoring of cardiovascular risk, bone and sexual health.
In 2014, an estimated 103,700 people were living with HIV (PLWH) in the UK, with 85,489 seen for HIV care during the year [1, 2]. Improvements in treatments for HIV mean that life expectancy for PLWH has increased dramatically . However with longer life expectancy we are seeing an increasing proportion of people living with co-morbidities including cardiovascular disease, metabolic complications, and malignancy [4, 5]. As such, to ensure optimal health outcomes for our patient cohort, primary and secondary health promotion and disease prevention extending beyond the virological and immunological control of HIV is required. The British HIV Association (BHIVA) produces guidelines for the management of HIV infection, in the UK. The process used by the BHIVA has been accredited by the National Institute for Health and Clinical Excellence (NICE). Guidelines are drafted by BHIVA Writing Groups and then placed on the BHIVA website for consultation by all interested parties. The BHIVA guidelines for routine investigation and monitoring of adult HIV-1 infected individuals 2011 recognised the paradigm shift in the treatment of HIV infection and provided guidance on the appropriate monitoring and assessment of adults living with HIV . These guidelines present a consensus regarding the standard assessment and investigation of HIV infection from the time of diagnosis and describe the appropriate monitoring of HIV-positive individuals both on and off ART.
In 2015, as part of the national audit programme of the British HIV Association (BHIVA), we audited adherence to the BHIVA guideline on monitoring and assessment of HIV infected individuals, and where relevant, immunisation guidelines. This article reports our findings.
All UK sites known to BHIVA as providers of adult HIV services were invited to complete a case-note review and a brief survey of local clinic practices. During June to August 2015 participating sites were asked to randomly select from the local list, 50–100 adults (aged 16 or over), who attended for specialist HIV care during 2014 and/or 2015. The selection was random and was not stratified. The number of cases was selected to ensure maximum participation of sites with varying patient populations. Data at each site were collected electronically using a self-audit spreadsheet tool. This included demographic details (gender, ethnicity, HIV exposure, and age) and whether audited outcomes as listed in Table 1 had been recorded. Some of these were modified from outcomes as specified in guidelines for ease of assessment. To allow for varying appointment dates, monitoring/procedures recommended as “annual” were interpreted as within 425 days (14 months). Similarly six monthly was taken to mean within 243 days (8 months), except in the case of HIV viral load testing where the guideline recommendation is to test 3–6 monthly i.e. within six months, rather than at 6 month intervals. As some HIV clinics do not provide influenza vaccination or cervical cytology, information was sought as to whether individuals had been advised to obtain these elsewhere.
This is the first national audit of adherence to the BHIVA monitoring and assessment guidelines. Data were compared to the targets set in the guidelines where applicable. Individual participating sites received their results via the self-audit spreadsheet tool and could compare them with national results which were presented at the BHIVA Autumn conference 2015 . Statistical analysis was performed using Microsoft Excel. Further analyses assessing the effect of adjusting for patient mix on site-level outcomes and summarising outcomes into meaningful groups and presenting results as a visual dashboard have been performed and reported elsewhere .
Case-note review data was provided for 8258 patients from 123 sites, but only 112 services completed the survey of clinic practices. The 8258 individuals included in the case-note review represent approximately 10% of PLWH reported in public health surveillance as attending UK HIV services . Two thirds were male, just over half (52.3%) acquired their HIV heterosexually, the majority were of white ethnicity (58.8%) and 60.6% were in the 30–49 year age group (see Table 1). 62.0% (5119/8258) of patients had been reviewed within three months up to audit data extraction in June–August 2015 and 96.5% (7971/8258) had been reviewed within 1 year. While it is difficult to perform a direct comparison, the characteristics of our study population are similar to the reported demographic data on people living with HIV in the UK .
Table 2 shows the proportion of individuals achieving the audit standards for all audited recommendations.
Baseline resistance testing
While the majority of audited cases met the national standard for baseline resistance testing (see Table 1), almost 1 in 5 (19.2%, n = 1586/8258) individuals did not. However baseline resistance testing was recorded as “not possible” for 47.3% (750/1586); 7.1% (112/1586) had neither been tested nor had a sample stored; and for 45.4% (720/1586) it was not known whether this had been done or the question was not answered.
Of 89.5% (7395/8258) audited individuals who were on ART, 90.1% (6660/7395) had a HIV viral load measurement within the past 6 months, exceeding the guideline target of 80%, and 93.4% (6908/7395) had had ART adherence assessed in the last year, which outperformed the target of 70%. However, only 89.0% (6584/7395) had all other medications recorded within the last year, despite a target of 100% to avoid drug-drug interactions.
Among audited individuals, 61.2% (5053/8258) were hepatitis A vaccinated, immune, or seropositive, 11.9% (n = 983/8258) were seronegative, 0.02% (2/8258) equivocal, and for 26.9% (2220/8258) it was not known whether this had been done or the question was not answered.
In terms of hepatitis B, 82.1% (6781/8258) individuals had serology fully reported (hepatitis B surface antigen HBsAg, hepatitis B core antibody (anti-HBc) and hepatitis B surface antibody (anti-HBs)); 0.9% (72/8258) were HBsAg positive with incomplete antibody status; 10.2% (841/8258) were HBsAg negative with incomplete antibody status; 6.8% (564/8258) had unknown HBsAg status or the question was not answered. Among 306 chronic hepatitis B infected (HBsAg+) individuals, 7.8% (24/306) were apparently unvaccinated and seronegative for hepatitis A. Among 3605 individuals whose status was consistent with vaccination (anti-HBs+, anti-HBc- and HBsAg-), 67.0% (2416) had had an annual anti-HBs measurement.
Hepatitis C antibody (anti-HCV) status was negative for 91.3% (7539/8258) individuals, positive for 5.3% (439/8258), equivocal for 0% (1), not known or the question was not answered for 3.4% (279/8258). Among the 7539 seronegative individuals, 65.4% (4928) had had an annual re-test including 74.1% (2423/3270) men who have sex with men (MSM) and 61.8% (21/34) injecting drug users (IDU), groups in whom this is recommended. Hepatitis C RNA (ribonucleic acid) testing had been done for 91.1% (400/439) anti-HCV positive patients. Data on HCV genotyping were not collected.
Only 44.9% (3318/7395) of patients on ART had a documented 10-year CVD risk within the past three years. Of those not on ART, 32.3% (279/863) had 10-year CVD risk recorded at any time, despite targets of 70% for both groups. ART status was unclear for 18 patients. Among 1582 patients aged >50 years on ART, with no documentation of established CVD, almost half (48.7%; 770) had CVD risk calculation recorded within the last 3 years.
Smoking status had been documented within the past two years for 65.9% (5445/8258) audited patients, well below the target of 90%. Only 45.2% (862/1905) of current smokers had been offered a cessation service although this is recommended . Current smokers were not more likely to have CVD risk calculated than ex or never smokers.
Sexual and reproductive health
An annual sexual health screen was recorded as offered for 65.7% (5424/8258) of all patients, including 72.7% (2581/3550) MSM, and 60.8% (2627/4320) heterosexuals. Syphilis serology was recorded within the past eight months (243 days) for 63.0% (5201/8258) of all patients, 73.4% (2604/3550) MSM, and 55.3% (2390/4320) heterosexuals.
Out of 2763 women, 53.2% (1471) had annual cervical cytology done and 21.9% (604) had been advised to attend a GP or sexual health clinic for this. The self-audit spreadsheet tool did not provide an option for women ineligible for cervical cytology. Contraception was reported not relevant for 31.7% (877/2763) of women. It had been discussed for 63.0% (1188/1886) women for whom it was relevant.
Fracture risk had been assessed within the past three years for only 16.7% (430/2568) patients aged over 50 years. Bone mineral density had been measured in 17.4% (29/167) individuals aged over 70 years and receiving ART. For simplicity, the spreadsheet recorded this from age 70 for both sexes although guidelines recommend it from age 65 in females.
Variation in monitoring between participating sites
There was wide variation in resistance testing across sites. 27% (33/123) sites met the target, having a recorded resistance test or stored sample for >90% of audited individuals while 27% (33/123) sites achieved this outcome for <75% of audited individuals, including 4.9% (6/123) sites who did so for <60%.
There was variation between sites in the proportion of patients for whom HBsAg status was not known, and for 8 sites this exceeded 20%. There was wide variation across sites in provision of influenza vaccination with 16/123 sites having administered or advised obtaining influenza vaccination at their general practitioner (GP) or Pharmacy for fewer than 10% of patients and 17/123 sites for more than 90% of patients.
There was wide variation in CVD risk calculation between sites; of 122 sites submitting data for patients receiving ART, 21.3% (26) met the 70% target for CVD risk recording within three years but 27.9% (34) achieved this for fewer than 20% of patients. There was also variation across sites for fracture risk assessment.
Most survey respondents routinely reviewed patients who were stable on antiretroviral therapy every 6 months, when HIV viral load (VL) was also checked. CD4 counts were less frequently measured (see Table 3). Sexual health screening was provided within 96.4% (108/123) of HIV services, cervical cytology within 71.4%(80/123) of HIV services and influenza vaccination within 71.4%(80/123) of services.
There was high participation in the national audit and the data showed good practice in some areas. Monitoring of ART was performed well; the proportions of individuals with viral load measurement and adherence assessment exceeded the expected standard. CD4 counts were less frequently measured in line with recent evidence on CD4 count monitoring frequency . The proportion of individuals with all medications recorded was high. Sexual health screening was performed well, perhaps due to the availability of this service in the same or adjacent clinics. Overall recording of hepatitis serology was high but with wide variation between sites. There was also wide variation in influenza vaccination, recording of baseline resistance testing, and monitoring of CVD risk factors and bone health. Some sites reported very low rates of baseline resistance testing though it is possible that this may reflect patients diagnosed and commenced on ART before routine resistance testing was available or recommended [10, 11].
Cardiovascular disease and smoking are major causes of morbidity and mortality in people living with HIV [4, 12]. However, low recorded rates of monitoring of cardiovascular health were noted and smoking status was not reported for one in seven patients, and less than half of current smokers were offered cessation support. The growing population of older patients living with HIV were also overlooked in terms of bone health, with very low rates of fracture risk assessment and bone mineral density recording. It is not clear if low recorded rates of monitoring of bone density was due to a lack of availability of bone densitometry measurement.
At some sites, a significant proportion of patients had unknown HBsAg status and many patients remain susceptible to hepatitis A, including those with documented chronic hepatitis B infection, for whom hepatitis A could be more serious. There was very low reported coverage of influenza and pneumococcal vaccination, perhaps indicating an issue for patients when responsibility and funding is shared between primary and secondary care.
Participating sites were asked to select individuals randomly from those attending during 2014 and/or 2015, but it is possible that more recent, and perhaps more regular, attenders were over-sampled as suggested by the fact that 62.0% of individuals had been reviewed within three months and 96.5% within one year preceding the audit. This may have led to over-estimation of rates of performance and recording of routine interventions.
There was also difficulty in interpreting some targets in the BHIVA guidelines. For example the 90% target for baseline resistance testing (or sample storage) is applicable for new incident diagnoses but less clear for individuals established in HIV care. As baseline resistance has ongoing clinical relevance, it is important this information remains accessible, including when individuals transfer care between clinics. We considered the target not met (80.8% individuals having recorded test or sample stored) although only 1.4% were known to be untested and some of these may have started ART before resistance testing was in use. As for all the monitoring outcomes some findings may reflect incomplete recording or reporting rather than performance.
Clinical services should review and develop systems to prompt both performance and recording of recommended interventions. Some sites have an ‘annual review’ system or electronic reminders for monitoring and, if adopted more widely, these may improve compliance with the monitoring guidelines. There may be a perception that primary care is responsible for certain monitoring and services such as cardiovascular risk and providing most vaccinations. Hence greater clarity from commissioners about where responsibility lies in these areas, particularly in what the forthcoming tariffs for HIV care cover, will help HIV services focus on areas they are responsible for. Improved communication between HIV and primary care services would streamline and improve care for people living with HIV. Clinical services should also develop improved strategies to care for older patients living with HIV .
Hepatitis B core antibody
Hepatitis B surface antibody
Hepatitis C antibody
British HIV Association
Estimated glomerular filtration rate
Hepatitis B surface antigen
Human immunodeficiency virus
Injecting drug users
Liver function tests
Men who have sex with men
National health service
People living with HIV
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Members of the BHIVA Audit and Standards Sub-Committee: A Freedman (chair), B Angus, D Asboe, F Burns, R Byrne, D Chadwick, D Churchill, H Curtis (co-ordinator), V Delpech, K Doerholt, A Molloy, J Musonda, N Naous, O Olarinde, E Ong, S Raffe, C Sabin, A Sullivan. The committee and authors would like to thank all HIV clinical services who submitted audit data, and S Michael, M May and M Gompels of Bristol University for conducting further analyses.
Participating clinical services: Area Infection Unit, Monklands Hospital, Airdrie; Tameside and Glossop Centre for Sexual Health, Ashton Primary Care Centre, Ashton-under-Lyne; Department of GU Medicine, Ysbyty Gwynedd Hospital, Bangor; Department of Integrated Sexual Health and HIV Medicine, Barking Community Hospital, Barking; Clare Simpson Clinic, Barnet General Hospital, Barnet; Department of GU Medicine, Barnsley Hospital NHS Foundation Trust, Barnsley; Department of Sexual Health, Solent NHS Trust, Basingstoke; Department of GU Medicine, Royal United Hospital, Bath; Beckenham Beacon Sexual Health Clinic, Beckenham Hospital, Beckenham; Department of GU Medicine, Bedford Hospital, Bedford; Department of GU Medicine, Royal Hospitals Trust, Belfast; Department of GU Medicine, Birmingham Heartlands Hospital, Birmingham; Department of HIV Medicine, Queen Elizabeth Hospital, Birmingham; Department of GU Medicine, Blackburn Royal Infirmary, Blackburn; The Pannel Suite Clinic, Royal Bournemouth Hospital, Bournemouth; Lawson Unit (HIV) Outpatients, Royal Sussex County Hospital, Brighton; Department of Immunology, Southmead Hospital, Bristol; Department of GU Medicine, West Suffolk Hospital, Bury St Edmunds; Department of GU Medicine, Frimley Park Hospital, Camberley; Infectious Diseases & HIV/GU Medicine Clinic 1A, Addenbrooke’s Hospital NHS Trust, Cambridge; The Gate Clinic, Kent & Canterbury Hospital, Canterbury; Department of GU Medicine, Cardiff Royal Infirmary, Cardiff; Infectious Diseases Unit, University Hospital of Wales, Cardiff; Department of GU Medicine, St Helier Hospital, Carshalton; Department of GU Medicine, Mid Essex Hospital Services NHS Trust, Chelmsford; The Blanche Heriot Unit, St Peter’s Hospital, Chertsey; Department of GU Medicine, Countess of Chester Hospital NHS Trust, Chester; Department of GU Medicine, Chesterfield Royal Hospital NHS Foundation Trust, Chesterfield; Fletcher Unit of Sexual Health, St Richard’s Hospital, Chichester; Department of GU Medicine, Essex County Hospital, Colchester; Department of Sexual Health, Leighton Hospital, Crewe; Department of GU Medicine, Croydon University Hospital, Croydon; Department of GU Medicine, Derbyshire Royal Infirmary NHS Trust, Derby; Department of GU Medicine, Dewsbury and District Hospital, Dewsbury; Department of GU Medicine, Downe Hospital, Downpatrick; Department of GU Medicine, Russells Hall Hospital, Dudley; Department of GU Medicine, University Hospital of North Durham, Durham; Department of Sexual Health, Avenue House Sexual Health Clinic, Eastbourne; Department of GU Medicine, Lothian University Hospitals, Edinburgh; Regional Infectious Diseases Unit, Western General Hospital, Edinburgh; Exeter NHS Walk-in Centre, Exeter; Borders Sexual Health, Galashiels; Trinity Square Health Centre, Gateshead; Department of GU Medicine, Gartnaval General Hospital, Glasgow; Department of GU Medicine, Gloucestershire Royal Hospital, Gloucester; Department of GU Medicine, Orsett Hospital, Grays; Department of GU Medicine, Bure Clinic, James Paget Hospital NHS Trust, Great Yarmouth; Department of Sexual Health, Buryfields Clinic, Guildford; Department of GU Medicine, Northwick Park Hospital, Harrow; Sexual Health Clinic, Station Plaza Health Centre, Hastings; Gaol Street Health Centre, Wye Valley NHS Trust, Hereford; Department of GU Medicine, Wycombe General Hospital, High Wycombe; Department of GU Medicine, Huddersfield Royal Infirmary, Huddersfield; Sexual Health Clinic, Wilberforce Health Centre, Hull; The Oak Tree Centre, Huntingdon; Orwell Clinic, Ipswich; Department of Sexual Health, West Middlesex University Hospital, Isleworth; Department of Infectious Diseases, Worcestershire Acute Hospitals NHS Trust, Kidderminster; Department of GU Medicine, Queen Elizabeth Hospital, King’s Lynn; The Wolverton Centre, Kingston Hospital, Kingston upon Thames; Department of Sexual Health, Whytemans Brae Hospital, Kirkcaldy; Leatherhead GUM Clinic, Leatherhead Hospital, Leatherhead; Department of GU Medicine, Leeds General Infirmary, Leeds; Infection and Travel Medicine Unit and GU Medicine, Leeds Teaching Hospitals NHS Trust, Leeds; Tropical and Infectious Disease Unit, Royal Liverpool University Hospital, Liverpool; Department of GU Medicine, Royal Glamorgan Hospital, Llantrisant; 56 Dean Street, Chelsea and Westminster Hospital, London; Caldecot Centre, King’s College Hospital, London; Centre for Sexual Health and HIV Research, Mortimer Market Centre, London; Department of GU Medicine, University Hospital Lewisham, London; Department of GU Medicine/HIV, Newham University Hospital, London; Department of HIV Medicine, Royal Free London NHS Foundation Trust, London; Department of Sexual Health, Homerton University Hospital NHS Foundation Trust, London; Harrison Wing, St Thomas’ Hospital, London; HIV/GUM Directorate: St Stephen’s Centre, Chelsea and Westminster Hospital, London; Jefferiss Wing Centre for Sexual Health, Imperial College Healthcare NHS Trust, London; Patrick Clements Clinic, Central Middlesex Hospital, London; The Ambrose King Centre, The Royal London Hospital, London; Trafalgar Clinic, Queen Elizabeth Hospital, London; West London Centre for Sexual Health, Charing Cross Hospital, London; Department of GU Medicine, Luton & Dunstable Hospital NHS Trust, Luton; Rubin Clinic, Department of GU Medicine, Maidstone Hospital, Maidstone; Department of GU Medicine, Manchester Royal Infirmary, Manchester; Department of Infectious Diseases, James Cook University Hospital, Middlesbrough; Department of GU Medicine, New Croft Sexual Health Centre, Newcastle upon Tyne; Department of Infection & Tropical Medicine, Royal Victoria Infirmary, Newcastle upon Tyne; Department of GU Medicine, Cordell Centre, Royal Gwent Hospital, Newport; Sexual Health Service, St Mary’s Hospital, Newport; Department of Sexual Health, Northampton General Hospital, Northampton; Department of GU Medicine, Grove Clinic, Norfolk & Norwich University Hospital, Norwich; Department of GU Medicine and HIV, Nottingham City Hospital, Nottingham; Department of GU Medicine, George Eliot Hospital NHS Trust, Nuneaton; Oldham Sexual Health Service, Royal Oldham Hospital, Oldham; Department of GU Medicine, Oxford Radcliffe NHS Trust, Oxford; Department of Infectious Diseases, Oxford Radcliffe NHS Trust, Oxford; iCaSH Peterborough, Peterborough and Stamford NHS Foundation Trust, Peterborough; Department of GU Medicine, St Mary’s Hospital, Portsmouth; Florey Unit, Royal Berkshire Hospital, Reading; Department of GU Medicine, Doncaster & Bassetlaw Hospitals NHS Foundation Trust, Retford; Department of Sexual Health, Glan Clwyd District General Hospital NHS Trust, Rhyl; Department of GU Medicine, Rotherham NHS Foundation Trust, Rotherham; Department of GU Medicine, Hospital of St Cross, Rugby; Sexual Health Department, Salisbury District Hospital, Salisbury; Department of GU Medicine, Royal Hallamshire Hospital, Sheffield; One to One Centre, Shiremoor; HIV/GUM Directorate, Upton Hospital, Slough; Department of GU Medicine, Ealing Hospital, Southall; Department of GU Medicine, Royal South Hants Hospital, Southampton; Department of GU Medicine, Southport & Ormskirk NHS Trust, Southport; Department of GU Medicine, St Helen’s and Knowsley Hospital, St Helens; Department of Microbiology and GU Medicine, Jersey General Hospital, St Helier; Department of GU Medicine, Sunderland Royal Hospital, Sunderland; Department of GU Medicine, Sherwood Forest Hospitals NHS Foundation Trust, Sutton-in-Ashfield; Department of GU Medicine, Singleton Hospital, Swansea; Department of GU Medicine, Musgrove Park Hospital, Taunton; Department of GU Medicine, Royal Cornwall Hospital, Truro; Department of GU Medicine, The Hillingdon Hospital, Uxbridge; Josephine Butler Centre, King Street Health Centre, Wakefield; Department of GU Medicine, South Warwickshire General Hospitals NHS Trust, Warwick; Department of GU Medicine, Weymouth Community Hospital, Weymouth; Department of GU Medicine, Arrowe Park Hospital, Wirral; Sexual Health Services, Worthing; Department of GU Medicine, York Hospitals NHS Trust, York.
The authors received no financial support.
Availability of data and materials
The datasets generated and analysed for this study are not publicly available due to the risk of breaching participant confidentiality via deductive disclosure, particularly as some groups within our dataset are very small.
Ethics approval and consent to participate
Ethical approval and informed consent were not required as this study was a clinical audit based on routinely collected data.
Consent for publication
The authors declare that they have no competing interests.
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