Abstract
Background
Regular monitoring of HIV patients who are receiving antiretroviral therapy (ART) is required to ensure patient benefits and the long-term effectiveness and sustainability of ART programs. Prompted by WHO recommendations for expansion and decentralization of HIV treatment and care in low and middle income countries, we conducted a systematic review to assess the feasibility of treatment monitoring in these settings.
Methods
A comprehensive search strategy was developed using a combination of MeSH and free text terms relevant to HIV treatment and care, health service delivery, health service accessibility, decentralization and other relevant terms. Five electronic databases and two conference websites were searched to identify relevant studies conducted in LMICs, published in English between Jan 2006 and Dec 2015. Outcomes of interest included the proportion of patients who received treatment monitoring and health system factors related to monitoring of patients on ART under decentralized HIV service delivery models.
Results
From 5363 records retrieved, twenty studies were included in the review; all but one was conducted in sub-Saharan African countries. The majority of studies (15/20) had relatively short follow-up duration (≤24 months), and only two studies were specifically designed to assess treatment monitoring practices. The most frequently studied follow-up period was 12 months and a wide range of treatment monitoring coverage was observed. The reported proportions of patients on ART who received CD4 monitoring ranged from very low (6%; N = 2145) to very high (95%; N = 488). The median uptake of viral load monitoring was 86% with studies in program settings reporting coverage as low as 14%. Overall, the longer the follow-up period, the lower the proportion of patients who received regular monitoring tests; and programs in rural areas reported low coverage of laboratory monitoring. Moreover, uptake in the context of research had significantly better where monitoring was done by dedicated research staff. In the absence of point of care (POC) testing, the limited capacity for blood sample transportation between clinic and laboratory and poor quality of nursing staff were identified as a major barrier for treatment monitoring practice.
Conclusions
There is a paucity of data on the uptake of treatment monitoring, particularly with longer-term follow-up. Wide variation in access to both virological and immunological regular monitoring was observed, with some clinics in well-resourced settings supported by external donors achieving high coverage. The feasibility of treatment monitoring, particularly in decentralized settings of HIV treatment and care may thus be of concern and requires further study. Significant investment in POC diagnostic technologies and, improving the quality of and training for nursing staff is required to ensure effective scale up of ART programs towards the targets of 90-90-90 by the year 2020.
Electronic supplementary material
The online version of this article (doi:10.1186/s12981-017-0131-5) contains supplementary material, which is available to authorized users.
Keywords: HIV, Decentralized care, Task-shifting, Antiretroviral treatment, Treatment monitoring, Viral load, CD4, Systematic review
Background
Increasing access to antiretroviral therapy (ART) for people living with HIV/AIDS has been identified as a key strategy to curb the HIV epidemic and avoid its cost in the future [1]. In 2015, an estimated 15 million people living with HIV/AIDS (PLWHs) were receiving ART, a remarkable milestone in the fight against HIV/AIDS [2]. However, in order to achieve the ambitious sustainable development goal of ending the HIV epidemic by 2030, greater efforts are required in expanding ART coverage and improving quality of services with innovative and effective service delivery models.
In a number of the low and middle income countries (LMICs) most affected by the epidemic, decentralization of HIV treatment and care, linked with task-shifting, has been implemented in response to the need for scaling up service provision [3]. Evidence from existing systematic reviews suggests that relocation of ART services closer to patients’ homes through decentralized care can improve patient access and adherence to HIV treatment with non-inferior quality of care as compared to centralized, hospital-based care [4–6].
Current WHO guidelines on the use of ARV drugs for HIV treatment and prevention strongly recommend virological monitoring as the strategy of choice for monitoring responses to ART [7]. Immunological monitoring (CD4 testing) is being scaled back for assessment of treatment responses where VL testing is available, but will still be required for the foreseeable future in many settings to determine the level of HIV-induced immune deficiency, including the need for screening and prophylaxis for serious co-infections, and to prioritize initiation of HIV treatment. Clinical monitoring is essential for all patients who are receiving ART to monitor patient responses to treatment and diagnose potential treatment failure [8]. In addition, monitoring of ARV drug toxicity is recommended, as delaying drug substitutions when there are adverse drug effects may not only cause harm but also result in non-adherence leading to drug resistance and treatment failure. The latter will compromise the effectiveness of available ART regimens, increase spread of drug-resistant HIV, increase HIV incidence, morbidity and mortality and negatively impact the long-term sustainability and efficacy of ART programs in LMICs.
Given the current limited health system capacity in many LMICs, meeting WHO’s recommendations regarding regular monitoring of patients’ responses to treatment, including monitoring of drug toxicity, may pose major challenges to the health system with possible negative impacts on quality and sustainability of HIV services in the future [9, 10]. This vulnerable situation is particularly likely while rapid scale up of decentralized provision of ART is being prioritized.
This systematic review assessed the feasibility of ART treatment monitoring in settings of decentralized HIV treatment and care in LMICs.
Methods
Literature search strategy
The preferred reporting item for systematic reviews and meta-analysis (PRISMA statement) [11] was used to guide the conduct of this review. A literature search strategy was developed to identify relevant studies that involve decentralization of HIV treatment and care in low and middle income countries, published in English between Jan 2006 and Dec 2015. Key search terms include MeSH and free text terms relevant to HIV infection, HIV treatment and care, health service delivery models and service accessibility such as: “HIV”, “HIV infection”, “Antiretroviral therapy”, “ART”, “HAART”, “delivery of health care” “primary health care”, “community health services”, “home-based*”, “decentral*”, “task-shift*”. Search terms also included those that refer to treatment monitoring including “treatment outcomes”, “adverse effect” and “toxicity”. The search strategy was first conducted in Medline (see Additional file 1: Annex S1), then adapted to run across CENTRAL, CINAHL, EMBASE, Scopus and Web of science. Conference abstracts were also searched from International AIDS Society and CROI conference websites. Grey literature resources and reference lists of existing systematic reviews were searched to identify relevant studies. For the purpose of this review, “feasibility” is defined as capacity of health system to provide and patient’s accessibility to ART monitoring services following WHO’s recommendations [7].
Study selection
Studies met inclusion criteria for this review if they: (i) involved HIV infected patients requiring ART and treatment follow-up, and/or healthcare workers involved in providing ART services; (ii) involved a decentralized model of HIV treatment and care which was defined as ART initiation and/or ART monitoring services provided at non-hospital settings: primary health facility or community level (through home-based delivery or community outreach including mobile health services); and (iii) reported one or more of the primary outcomes of interest as defined below.
Proportion of patients receiving (with data documented) CD4 count, clinical HIV staging, and/or HIV viral load monitoring at treatment follow-up at regular intervals (6 or 12 months);
Proportion of patients receiving ARV drug toxicity monitoring (clinical and/or biomedical) at treatment follow-up at regular intervals; and/or
Reported enablers, barriers and other implementing issues related to monitoring of ART services, including any of the following (a) human resources (availability and quality of clinical staff; staff competency training); (b) availability of, and access to, clinical, biochemical monitoring tools for monitoring treatment response, diagnosing ARV drug toxicity, and/or treatment failure; (c) supply chain management: reagents, equipment maintenance, etc. under decentralized HIV care; (d) patient and provider’s attitude towards decentralization of HIV treatment and care.
Secondary outcomes included: (1) Proportion of patients with reported treatment failure, and (2) Proportion of patients who switched to a second line ARV drug.
In order to be eligible for inclusion, studies must have been conducted in LMICs and have reported at least one primary outcome or provided data which allowed for calculation of treatment monitoring uptake.
Data extraction and data synthesis
Data were extracted electronically using a pre-constructed, standardized data extraction form. Double data extraction with 20% duplication was performed by two independent reviewers. Extracted information included: study details (author/year, objective, design, number of patient enrolled), study population criteria, mode of ART services and outcome of interest. Data on outcomes of interest were grouped, presented and compared by models of service delivery (decentralized vs centralized), time point of treatment follow-up, and study design/study setting context. Quantitative data were presented and analyzed descriptively and data across studies were pooled, provided study interventions and populations were sufficiently similar. Qualitative data were thematically categorized using main themes relevant to the research questions, which emerged from data extracted.
Results
Study characteristics
The search strategy identified 5363 titles after duplicates were removed. Screening of titles plus abstracts with exclusion of clearly irrelevant studies resulted in 58 eligible studies for full text review, of which 20 studies (19 articles and one abstract [12]) met all of the inclusion criteria, and were included in the review (Fig. 1).
All but one of these 20 studies were conducted in sub-Saharan Africa (SSA): 10 studies were from various urban, peri-urban and rural settings in South Africa (SA), one study was from rural and urban Ethiopia, one from rural Lesotho, one from rural and urban Kenya, two from rural Rwanda, one from urban Mozambique, one from rural Zimbabwe, two from rural Swaziland, and one from Asia (Thailand). Only two studies were specifically designed to assess the coverage of HIV treatment monitoring services in a decentralized setting; other studies evaluated and reported treatment outcomes. Only one study reported the proportion of patients who developed drug toxicity and two studies provided qualitative data (Table 1).
Table 1.
First author, year | Study design | Study participant | Study location/country | Study objective | Model of ART services | Additional resources provided | Study duration/period | Number of patient enrolled | Outcomes of interest | |
---|---|---|---|---|---|---|---|---|---|---|
Primary | Secondary | |||||||||
Assefa, 2011 [30] | Mix method: retrospective cohort and qualitative study | HIV patient started ART at health facilities providing ART services | 55 health facilities 25 health centers and 30 hospitals representing different regions of Ethiopia | To evaluate outcomes of ART services at health centers vs hospital | ART services led by health officer, nurses and CHWs at health center | Community health workers: adherence counseling, defaulter tracking referral and linkage between facilities | Sep 2006–Mar 2009 | 6206 at health centers; 31,929 at hospitals | Proportion of patient with CD4 count documented Stakeholder’s perspectives on new decentralized model of care |
|
Bedelu, 2007 [17] | Retrospective cohort | Adult HIV patient | Primary care clinics and hospitals/Lusikisiki, South Africa (SA) | To assess the effect of decentralization and task-shifting on treatment outcomes | ART service led by nurses at health clinic | MSF supported through mobile team visit, training/mentoring of nurse; engage community through support groups | Apr 2004–Apr 2006 | 1025 (595 at clinic; 430 at hospital) | Proportion of patient with CD4 count and VR data documented | |
Boulle, 2010 [19] | Retrospective cohort | Adult treatment naïve HIV patient ≥14 years old | HIV treatment program at three public primary care clinics (PHC) Khayelitsha, SA | To describe outcomes of ART program for adult up to 5 years | Nurse based care with stable patients seen by a nurse 2–3 monthly | Program established/supported by MSF | 2001–2007 | 7323 | Proportion of patient with CD4 count and viral load data available | Proportion of patient reported treatment failure; % patient switch to 2nd line ART |
Brennan, 2011 [16] | Retrospective cohort | ART naive patient >18 years old | Urban HIV clinic and local PHC in Johannesburg SA | To compare one year outcomes between patient down-referred and maintained at central clinic | ART initiated at hospital and then follow-up at PHC by nurse | Nurse received down-reference training; supervise by doctor, plus advice by electronic treatment algorithm | Apr 2004–Sep 2008 | 2772 | Proportion of patient with 12 month CD4 and VL available | |
Fatti, 2010 [41] | Retrospective cohort | ART naïve adult patient >16 years | 59 public facilities: 47 PHCs, nine district and three regional hospitals in four provinces of SA | To compare treatment outcomes at different levels of health system (primary health care, district and regional hospital) | ART services led by doctor at different levels | Community-based adherence counselor; all sites supported by NGO (absolute return to kids) with free services to HIV patients | Dec 2004–Dec 2007 | 29,203 | Proportion of patient with viral load results | |
Fairall, 2012 [13] | Randomized control trial | Adult patient who had received ART for at least 6 months and were on ART at time of enrollment | 31 clinics (16 intervention and 15 control) in free state of SA | To assess effects of task-shifting program on treatment outcomes | ART service led by nurse at primary care clinics (intervention) vs doctor at hospital OPC (control) | Outreach training for nurses with doctor support | Jan 2008–Jun 2010 | 3029 (intervention) 3202 (control) | Proportion of patient with VR data available | |
Humphreys, 2010 [27] | Prospective cohort | Adult patient on ART at least 4 weeks CD4 >100 | Primary care clinics and district hospital in rural Swaziland | To assess effect of nurse led primary care based ART program | ART service led by nurse at primary care clinics vs doctor at hospital | Training for primary care nurses by hospital followed by monthly outreach support visits | Jan–Nov 2007 | 474 | Patient experience with primary based ART program | |
Hansudewe-chakul, 2012 [15] | Retrospective cohort | HIV infected children | Tertiary hospital and community hospital in rural Thailand | To assess effects of decentralization of pediatric HIV care model | ART initiated at tertiary hospital, monitored at community hospital | Training and mentoring for CH staffs; trained PLHIV: adherence, psychological support | Feb 2002–Mar 2008 | 410 | Proportion of patient with VL data recorded | |
Janssen, 2010 [21] | Prospective cohort | HIV patient <15 years on ART | Primary care clinics, KwaZulu-Natal, SA | To assess clinical outcomes of children in a decentralized model | Nurse/counselor led ART program | Home-based care program with nurse/community volunteer providing first aids, nutrition, adherence support at home | Jun 2004–Jun 2008 | 477 | Proportion of patients receiving CD4 and VL monitoring | |
Jobanputra, 2014 [26] | Retrospective cohort | HIV patient on ART | Primary health care clinics in rural poor Shiselweni region of Swaziland | To assess program quality, cost and outcomes of routine VL monitoring | Nurse led ART program | MSF support (laboratory equipment, reagent, training of staff) | Oct 2012–Mar 2013 | 5563 | Proportion of patients receiving routine VL monitoring | Reported treatment failure rate; % patient switch to 2nd line ART |
Labhardt, 2012 [29] | Retrospective cohort | HIV patient >16 years old on ART with at least three drugs | Two hospital and 12 health centers of Botha-Bothe ad Thaba-Tseka districts of Lesotho | To assess the effectiveness of decentralized ART program | Nurse led ART program | ART program supported by a Swiss NGO through the SolidarMed ART project | Jan 2008–Apr 2011 | 3747 | Availability of treatment monitoring tools at decentralized settings | |
Mutevedzi, 2010 [20] | Retrospective cohort | Adult patient >16 years old | 16 primary care clinic in rural SA | To describe and assess scale-up of decentralized HIV treatment program | ART initiated by doctor and monitored by nurse | Support for program provided by PEPFAR | Oct 2004–Sep 2008 | 3010 | Proportion of patient with VL data recorded | |
Rich, 2012 [22] | Retrospective cohort | HIV patient on ART | ART clinics at health centers in rural Rwanda | To assess clinical outcomes of HIV treatment program | Community-based ART program with directly observed ART and psychosocial supported provided by CHWs | Ongoing HIV education, nutritional assistance, travel allowance for clinic visits, diagnosis and treatment of TB; additional doctor/provider support | Jun 2005–Apr 2006 | 1041 | Proportion of patient with CD4 and VL monitoring data available | Proportion of patient change treatment regimen due to toxicity; % patient switch to 2nd line ART |
Selke, 2010 [14] | Randomized control trial | HIV patient, 18 years stable on ART at least 3 months | HIV clinic in rural health center of Kenya | To assess impact of task shifting | Nurse led ART service with home based visit by community care coordinator (CCCs) vs standard of care (no CCCs) | Electronic device support tool (PDA) for patient monitoring; program supported by USAID | Mar 2006–Apr 2008 | 208 (96 intervention; 112 control) | Proportion of patient monitored with clinical, immunological, virological data | |
Shumbusho, 2009 [24] | Retrospective cohort | HIV treatment-naïve adult patients | Three rural primary health centers in Rwanda | To evaluate results of pilot task-shifting model for ART service provision | Nurse centered ART services (initiation management and referral of complex cases | Additional personnel provided for intervention (specific number not reported) | Sep 2005–Mar 2008 | 1076 (641 pre-ART and 435 on ART) | Proportion of patient with CD4 count documented | Proportion of patient change treatment regimen due to toxicity; % patient switch to 2nd line ART |
Sanne, 2010 [25] | Randomized control trial | Adult HIV-1patient (>16 year old, CD4 <350 or previous AIDS defining illness; not pregnant) | Two primary health care sites in Cape town and Johannesbur, SA | To compare outcomes of nurse vs doctor management of ART | ART services led by nurses (vs doctor led): full decentralization | Not reported | Feb 2005–Jan 2009 | 812 | Proportion of patient reported drug toxicity | |
Uzodike, 2015 [18] | Cross-sectional | Adult HIV patient on ART | Primary healthcare (PHC) clinics in Kwazulu-Natal, SA | To assess monitoring and referral of patient on ART managed at PHC clinics | ART services led by nurses | Not reported | Jun 2011–Jun 2012 | 488 | Proportion of patients with CD4 VL monitoring data available | % patient reported virological failure |
Vogt, 2015 [23] | Retrospective cohort | HIV patient >18 years old initiated on ART at district hospital and rural health clinics (RHCs) | Beitbridge district hospital and six RHCs in Matabeleland South province, Zimbabwe | To compare coverage of CD4 testing between rural and urban HIV patient during 1st year of treatment | HIV care services provided by nurses at RHCs through weekly outreach visits | Services provision supported by MSF (MSF nurse and phlebotomy equipment) | Jan 2011–Dec 2012 | 2145 | Proportion of patients receiving CD4 testing | |
Walter, 2014 [12] | Before–after (decentralization) comparison | HIV adult patients initiated on ART at primary health centers | To compare treatment outcomes before and after decentralization | ART service led by nurses at primary health care center | Not reported | 2003–2006 (before) 2009–2011 (after) | 3936 (before); 13,505 (after) | Proportion of patient with CD4 count documented | ||
Georgeu, 2012 [28] | Qualitative | HIV patient, service providers (physician, nurse) | Primary health care clinics in free state of SA | To explore experience, perceptions of various stakeholders on implementation process of decentralization of ART services | ART service led by nurses | Not reported | Oct 2007–Jun 2008 | 16 FGDs, 26 in-depth and key informant interview | Implementing issues related to decentralization Stakeholder’s perspective on decentralization |
HIV viral load (VL) monitoring
Twelve studies (Table 2) provided data regarding the proportion of patients who received regular VL monitoring, among which 11 studies reported the proportion of patients receiving VL monitoring at 12 months follow-up, with a median service uptake of 86%. The highest coverage of virological monitoring services was reported from two randomized control trials (RCT) conducted in SA [13] and Kenya [14] with 92% (2582/2823) and 99% (86/87) uptake; both studies were conducted by dedicated research staff who were not part of the routine clinical service. The lowest reported proportion of patients with VL monitoring data came from a retrospective cohort study conducted between 2002 and 2008 in rural Thailand [15] with only 14.3% (22/154) of patients having VL data available at baseline and at least one treatment follow-up 12–48 months after treatment initiation. The authors reported that routine VL testing was not available, baseline VL data were available only for a subset of the study participants and VL was determined at 12 months intervals during the 48 months of study.
Table 2.
First author, year | Follow-ups | Number of patient retained in care | Proportion of patient monitored for treatment response n (%) by # monitoring approaches | Laboratory testing services | Testing site | Notes | ||
---|---|---|---|---|---|---|---|---|
Virological | Immunological | Clinicala | ||||||
Assefa, 2011 [30] | 6 months | Health center: 5072/6197 Hospital: 24,821/31,269 |
Not report (NR) | 54% | NR | Not stated | Not stated | Number of patients received immunological monitoring with CD4 count documented was not reported. Data (proportion of patient monitored) was not reported separately for each level of care |
12 months | Health center: 3042/4022 Hospital: 17,037/23,039 |
NR | 51% | |||||
24 months | Health center 650/856 Hospital : 4419/6595 |
NR | 51% | |||||
Bedelu, 2007 [17] | 12 months | Health clinic: 482/595 Hospital: 289/430 |
Health clinic: 296/482 (61.4%) Hospital: 41/289 (14.2%) |
Health clinic: 348/482 (72.2%) Hospital: 81/289 (28%) |
NR | Not stated | Not stated | |
Boulle, 2010 [19] | 1 year | 4512 | 3932/4512 (87%) | 3823/4512 (85%) | NR | CD4 and VL provided 6-monthly after staring ART | Not stated | VL: NucliScens EasyQHIV-1 assay CD4: single-platform panleucogating method Type of blood used not reported |
2 years | 2561 | 2198/2561 (86%) | 2108/2561 (82%) | |||||
3 years | 1235 | 983/1235 (79.6%) | 931/1235 (75.4%) | |||||
4 years | 458 | 351/458 (76.6%) | 341/458 (74.5%) | |||||
5 years | 191 | 148/191 (77.5%) | 127/191 (66.5%) | |||||
Brennan, 2011 [16] | 12 months | Hospital : 1958/2079 Primary health care: 681/693 |
Hospital: 1774/1958 (90.6%) PHC 676/681 (99.2%) |
PHC: 95% Hospital: 81% |
Clinical monitor performed every 2 months by nurse at PHC; 6 monthly by doctor at hospital | CD4 and VL test measured every 6 month | Not stated | Inconsistency in data on % patients with CD4 and VL data available between text and table. Number of patients with 12 months CD4 count available not reported |
Fatti, 2010 [41] | 12 months | 11,960 | 6725 (56.2%) | NR | Patients attend monthly clinical checks | CD4 count and VL monitored 6 monthly for patient on treatment by SA NHL services | Off-site except for large hospital | Data (n/N) on proportion of patient received and had VL available was reported for all level of care |
24 months | 4029 | 2525 (62.6%) | ||||||
36 months | 545 | 342 (62.8%) | ||||||
Fairall, 2012 [13] | 12 months | Primary care: 2823/3029 Hospital: 2981/3202 |
Primary care: 2582/2823 (91.5%) Hospital: 2656/2981 (89.1%) |
NR | NR | Not stated | Not stated | |
Hansudewe-chakul, 2012 [15] | 12, 24, 36, 48 months (VL data available at baseline and at least 1 follow-up) | Community hospital: 154 Tertiary hospital : 133 |
CH: 22/154 (14.3%) TH: 38/133 (28.6%) |
NR | Clinical monitoring using CDC classification; | CD4% assessed 6 monthly, routine VL testing not available. VL measured at 12 month intervals for 48 months | Not stated | No time point specific provided for % patient with VL data available. Scheduled clinic visit 6 monthly at tertiary hospital |
Janssen, 2010 [21] | 6–12 months | 447 | 193/447 (43.2%) | CD4%: 310/447 (69.3%); CD4: 315/447 (70.5%) | NR | Laboratory tests (CD4, VL, Hemoglobin/albumin) repeated 6 monthly | VL testing at referral hospital (75 km away); other tests at local hospital | |
Jobanputra, 2014 [26] | 12 months | 5563 | 4767/5563 (86%) | NR | NR | VL measured annually using a Generic HIV VL platform (Biocentric) | VL testing at regional virology laboratory | |
Mutevedzi, 2010 [20] | 12 months | 2527/3010 | 758/2527 (30%) | NR | NR | CD4 count and VL measured every 6 months | VL testing at provincial lab | VL measured by Nucli-Sens Easy HIV-1 assay). Type of blood used not report |
Rich, 2012 [22] | 24 months | 926 | 275/926 (29.7%) | 710/926 (76.7%) | NR | CD4 count measured 6 monthly using BD fluorescence-activated cell sorting count system | Not stated | |
Selke, 2010 [14] | 12 months | Intervention: 87 Control: 102 |
Intervention: 86/87 (99%) Control: 96/102 (94.1%) |
Intervention: 87/87 (100%) Control: 96/102 (94.1%) |
Intervention: 74/87 (85%) Control: 87/102 (85.3%) |
VL and CD4 count obtained at initial and close out research visit. Additional CD4 count at 6 months | Not stated | |
Shumbusho, 2009 [24] | 6 months | 217 | NR | 193/217 (88.9%) | 83.4%: side effect screening at all visits (frequency not reported) | CD4 count measured every 6 month using BD FACS Count | District hospital laboratory | |
12 months | 123 | NR | 104/123 (84.5%) | |||||
18 months | 43 | NR | 31/43 (72.1%) | |||||
24 months | 10 | 10/10 (100%) | ||||||
Uzodike, 2015 [18] | Jun 2011 | 488 | 407/488 (83.4%) | 461/488 (94.5%) | 412/488 (84.4%) | CD4 and VL monitored 6 monthly | Not stated | Clinical monitoring carried out monthly by nurses |
Dec 2011 | 466/488 (95.5%) | 464/488 (95.1%) | NR | |||||
Jun 2012 | 444/488 (91.0%) | 430/488 (88.1%) | 381/488 (78%) | |||||
Vogt, 2015 [23] | 6 months | 1250 | NR | 194/1250 (15.5%) | 1250/2145 (58%) | Whole blood collected in EDTA tube for testing by BD Fascount and Partect Cyflow | District hospital laboratory | Data is presented for both hospital and RHCs |
12 months | 1199 | NR | 74/1199 (6.2%) | 1199/2145 (56%) | ||||
Walter, 2014 [12] | 6 months | 11,243 | NR | 5859 (52%) | NR | Not stated | Not stated | |
12 months | 8644 | 5160 (60%) | ||||||
18 months | 6467 | 4110 (64%) | ||||||
24 months | 4485 | 3201 (71%) |
aClinical monitoring using WHO clinical staging except mentioned otherwise
In four studies that reported the proportion of patients who received VL monitoring in both centralized and decentralized models of care, two studies reported a higher proportion of monitoring of patients attending centralized care (vs decentralized care): 99% (1774/1958) versus 91% (676/681) [16] and 29% (38/133) versus 14% (22/154) [15], while another two studies reported a similar or higher proportion of patients with access to VL monitoring with decentralized care (vs centralized care): 92% versus 90% [13] and 61% (296/482) versus 14% (41/289) [17]. In the two latter studies, both conducted in SA, the difference in service coverage between models of care was not discussed; however, one study [13] reported results of a 30 month randomized trial aimed to assess the effects of an outreach training program provided to nurses for ART initiation and prescribing at primary care clinics while the other [17] reported outcomes of a community-based, decentralized HIV services delivery program supported by Medecins Sans Frontieres (MSF).
Overall, studies conducted in urban settings reported a higher uptake of VL monitoring services: three studies conducted in urban HIV clinic settings in SA [16, 18, 19] reported more than 80% of patients had VL data available after 6–24 months on treatment while three other studies in rural settings (two in South Africa [20, 21] and one in Rwanda [22]) reported 30–43% of patients had access to this service at 12 months follow-up although almost all (five of six) studies stated that VL (and CD4) was planned to be measured 6 monthly for all patients on ART. The ability of nursing staff to establish virological failure for timely referral and regimen switch was a concern as only 59% of patients who demonstrated persistently elevated VL in two consecutive VL monitoring tests were referred for further treatment intervention [18]. None of the included studies reported on-site VL or CD4 testing.
Among 12 studies that included data regarding virological assessment, only three studies reported the platform used for viral load testing (two studies with Nucli-Scens EasyQ HIV-1 and one study with a generic HIV VL platform-Biocentric) and none of these three studies discussed the blood sample used for VL testing (plasma or dried blood spot). None of the other nine studies reported how and where virological and/or immunological monitoring for patients on treatment was conducted.
Clinical and immunological monitoring
The majority (15 of 20) of included studies reported the use of WHO clinical staging to assess and monitor patients’ responses to treatment (Table 2). Only three studies specifically provided data regarding the proportion of patients who received clinical monitoring through decentralized HIV treatment programs. The other 12 studies did not provide sufficient data for calculation of the coverage of clinical monitoring at decentralized settings.
One study [18] conducted in urban SA assessed the adherence of nursing staff at a primary health care clinic to national guidelines regarding monitoring and follow-up of HIV patients on ART. In this retrospective, cross-sectional study the authors randomly selected and assessed medical records of 488 patients attending the clinic from June 2011 to June 2012 and reported 84% (412/488) and 78% (381/488) patients with clinical monitoring data available by June 2011 and June 2012 respectively.
Another study [14] aimed to evaluate clinical outcomes of patients enrolled in a community-based HIV care program delivered by PLWHs (intervention group) as compared to patients receiving standard, clinic-based care (control group). The reported proportions of patients monitored clinically at 12 months follow-up were identical for both groups, 85% (74/87) for the control group and 85.3% (87/102) for the intervention group. One study [23] reported a lower level of clinical monitoring coverage with 1250 (58%) and 1199 (56%) out of 2145 patients initiated on ART receiving clinical assessments at 6 and 12 months follow-up, respectively.
Among 11 studies with patient follow-up periods from 6 to 24 months, the reported proportion of patients with a CD4 count measurement with data recorded at 6–12 month intervals ranged from 6 to 100%. One study [19] with follow-up data of up to five years reported that 67% (127/191) to 85% (3823/4512) of patients had their CD4 count measured, and 78% (148/191) to 87% (3932/4512) of patients having their VL measured, at 12 month intervals. Data from this study showed that the proportion of patients receiving immunological and virological monitoring decreased over time, although the total number of patients in care also reduced by 96% after 5 years on treatment (from 4512 after 12 months to 191 after 5 years follow-up).
Two studies provided data that compared coverage of immunological monitoring between decentralized and centralized HIV care sites and both studies reported a higher uptake of services in the decentralized model. One study [17] reported 72% (348/482) of patients attending rural primary health care clinics versus 28% (81/289) attending a hospital had their CD4 count determined after 12 months of treatment. The authors reported that ART services provided at primary clinics were supported by Médecins Sans Frontières (MSF) with involvement of peer support groups to track defaulters, provide adherence support, advocate for better drug supply and monitoring of HIV program whereas no such supports were provided to patients receiving care at hospital. The second study [16] reported 95% of down-referred (decentralized) patients (n = 693) versus 81% of centralized patients (n = 2079) had a CD4 count (and VL) available at 12 months but the information on treatment monitoring procedure (platform used for VL testing, type of blood sample used and place where VL testing performed) was not presented.
One study [23] aimed to assess the coverage of immunological monitoring between HIV patients living in a semi-urban district in Zimbabwe and reported only 21 and 8% of urban (n = 1545), and 2 and 1% of rural patients (n = 600) had received CD4 testing at 6 and 12 months follow-up, respectively. The authors reported that CD4 testing at rural health centers was usually restricted to the day of outreach visits when outreach staff collected blood samples in Ethylenediaminetetraacetic Acid (EDTA) tubes and brought the blood back to the district hospital for testing within 24 h. Limited capacity for specimen transportation within local health systems was noted as the main reason for the differences in access to CD4 testing between rural and urban patients.
Toxicity monitoring
No study reported the proportion of patients receiving laboratory monitoring for ARV drug toxicity at scheduled monitoring visits in program settings. The proportion of patients who changed their initial regimen (drug substitution, not considered as switching to second line ART) due to drug toxicity was reported as ranging from 5% (161/3029) [13] to 29% (304/1040) [22]. One retrospective cohort study [24] reported 83.4% of all patients were screened for side-effects at all visits but the frequency of visits was not stated. A randomized controlled trial [25] reported 17% (68/404) and 16% (66/408) toxicity failure in patient groups managed by a nurse and by a doctor at primary care settings, respectively.
Secondary outcomes
Three studies reported the proportion of patients with virological failure and four studies reported the proportion of patients who switched from 1st to 2nd line ART. The reported proportion of patients with treatment failure ranged from 14% (n = 4512) [19] to 49% (n = 488) [18] and the proportion of patients starting 2nd line treatment was from 0.5% (n = 1040) [22] during 24 months follow-up to 12.2% (n = 4512) [19] at 60 months on treatment. One study assessed the outcomes of routine VL monitoring of ART programs through a decentralized network of 22 primary care clinics and three reference facilities in Zimbabwe. These investigators reported 17% (551/3242) of VL tests had detectable HIV (>1000 copies/µL) and among 288 patients with an initial detectable VL result, 78 patients (27%) did not receive adherence counseling, 86 (30%) patients had no follow-up VL, and 15 patients (5.2%) patients were switched to 2nd line treatment, among whom four patients were switched based on a single detectable VL result [26].
Factors that influence the implementation and feasibility of decentralization
Data from included studies suggest that patients were supportive of decentralization of HIV treatment and care as it could help to improve their access to care (Table 3). One study [27] reported 96% (29/31) of patients interviewed were ‘very satisfied’ or ‘satisfied’ with HIV treatment services provided by nurses, and the main reasons for this included reduced cost, receiving services near home and shorter queue, and being treated better by staff. Health professionals also reported positive responses: nurses were comfortable, motivated, enthusiastic about the opportunity to be directly involved in providing life-saving treatment; physicians supported decentralization and nurse-led ART initiation as it could help increase ART coverage, but expressed uncertainty about the ability of nurses to manage and refer complicated cases [28].
Table 3.
First author, year | Reported implementing issues/barriers for ART services under decentralized care from system perspective | Acceptability and reported quality of decentralized care from service provider and patient perspectives |
---|---|---|
Assefa, 2012 [30] | Policy: lack of regulation framework enabling nurse to perform tasks such as ARV prescription, monitoring of patients on ART Finance: high cost associated with training and monitoring quality of services Human resource: additional workload for nurse without increased remuneration/compensation; Community health workers were not permanent employee/formal health system |
Patient’s perspective: Nurse led ART services was well accepted, help to reduce waiting time; provide appropriate counseling; combat stigma and discrimination in society and can help to provide opportunity for employment |
Georgeu, 2012 [28] | Workload, including paperwork increased significantly for nurses and other team members through broader human resource shortage and lack of capacity (e.g. data capturers performed basic nurse duties when nurse too busy, nurse dispensed when pharmacist not available) Increased number of patients on treatment further strained scare/inadequate human and physical resources of health system: insufficiently staff and resources; fragmented information, poor patient transport/referral system; unreliable drug supplies due to poor communication, transport between pharmacy/central dispensing unit and clinics |
Nurses were comfortable, motivated, enthusiastic about opportunity to be directly involve in providing life-saving ART treatment Physicians reported mix attitude: majority support decentralization and nurse initiated ART but significant minority reported uncertainty about the ability of nurses to manage and refer complicate cases Patients were supportive of decentralization as it improved access to care, reduced travel time/cost but some wanting ART to remain a separate services and expressed preference toward physician services because of higher clinical status and only doctor can medically certify social grant—key source of income for people living with HIV/AIDS in South Africa |
Humphreys, 2010 [27] | Among patients interviewed in intervention group (received nurse led/primary care based ART services) 81% (25/31) were very satisfied 13% (4/31) were satisfied 3% (1/31) dissatisfied and 3% (1/31) very dissatisfied as compared to services at main hospital Reasons for satisfaction includes: reduced cost, services provided nearer to home, shorter queue and being treated better by staff. Reasons for dissatisfaction were lack of doctor and delay of service because team from hospital arrive late |
|
Labhardt, 2012 [29] | CD4, VL and biochemistry were not available on site at decentralized settings Hemoglobin was available in 2/5 and 2/7 health centers of two studied districts |
A number of system factors that could hinder the implementation and scale-up of decentralization in low-resource settings were identified and discussed. These factors include: (i) Limited resources available for treatment monitoring services (ii) Lack of a policy framework which allows non-physician staff (nurses) to initiate HIV treatment; (iii) increased workload (clinical and administrative) for nurses without commensurate remuneration; (iv) unreliable antiretroviral drug supplies due to poor communication, inadequate transport between pharmacy/central dispensing unit and clinics; and (v) high costs associated with health worker training and monitoring of service quality [29, 30].
Discussion
Why treatment monitoring is important to achieve the 90-90-90 goal
Monitoring of patients on antiretroviral treatment (ART), especially in the context of rapid scale up of ART coverage in high HIV burden and low-resource settings through different models of services delivery including decentralization, is one of the most important elements to ensure effectiveness and sustainability of any HIV treatment and care program. The “90-90-90” goal aims at having 90% of HIV positive people knowing their infection status; 90% of those people receiving ART, and 90% of those on ART with virologic suppression, and is considered a universal target needed to effectively control and ultimately end the global HIV epidemic. There are two key milestones that need to be achieved to make the last “90” target a reality. First, the majority (>90%) of patients on ART must have access to appropriate and timely ART monitoring: 12-monthly VL assessment or 6-monthly clinical assessment and CD4 count if VL is not available. Second, effective treatment and well-functioning patient support systems including adherence coaching must be in place to achieve a majority (>90%) of patients on ART with sustained viral suppression.
VL monitoring
WHO has recommended VL testing as the preferred method for monitoring the responses of patients on ART [8] and it has been suggested that in order to achieve the “90-90-90” goal, viral load monitoring should and can become the standard of care in LMICs with high HIV prevalence [31]. There is ample evidence showing that routine VL monitoring can provide an early and more accurate diagnosis of treatment failure when compared to clinical and immunological monitoring [32, 33], but evidence regarding the value of VL monitoring as compared to immunological monitoring in reducing mortality among patients on ART has been mixed [34–38]. Availability of, and access to, VL testing is still limited due to the requirements of expensive laboratory equipment, complex sample collection and processing, and the need for highly trained personnel [39]. A recent WHO survey on availability and use of HIV diagnostics in LMICs found that the overall coverage of VL testing among patients on ART from 94 countries was 23% [40]. In our review, a wide range of VL monitoring coverage was observed. Although we found a median VL monitoring coverage of 86% at 12 months follow-up, this level of coverage may not well reflect regular VL monitoring practice under decentralized HIV care models in LMICs. Among eight studies which reported VL monitoring rate of greater than 50% among patients on ART, five studies reported results of decentralized HIV programs supported by external donors such as MSF [17, 19, 26], Absolute Return for Kids [41], U.S. Agency for International Development (USAID) [14], and two studies reported results of randomized trials in which VL testing was part of the funded studies in well-resourced settings [13, 14]. In addition, existing evidence suggests that the longer a patient is on ART the lower the rate of receiving regular VL test. Only three studies evaluated the long-term (more than 24 months) follow-up of VL coverage [15, 19, 41]. Thus, further research is needed to examine patient retention and treatment monitoring practices with long-term follow-up, particularly in rural settings.
Clinical and immunological monitoring
At decentralized primary care levels in LMICs, clinical and CD4 count monitoring remains a viable option to monitor treatment responses in settings where VL testing is not available. In our review, limited data were available to assess the feasibility and coverage of clinical and immunological monitoring in a decentralized model of HIV care, as only two studies provided data on the actual proportion of patients who received both clinical and CD4 monitoring. Of note, these are the two studies designed to assess treatment monitoring practice in two different settings, providing a contrasting picture of the coverage of treatment monitoring services. Differences in treatment monitoring coverage between these ART programs could be explained by study settings and service delivery models; one in an urban, well staffed HIV clinics with clinical staff on call and easy access to laboratory testing [18] while the other was in rural areas with ART service provided by outreach teams and with long distances for sample delivery from clinics to a laboratory facility located at a district hospital [23]. This finding highlights an important potential gap in existing knowledge. It has implications related to the implementation of treatment monitoring in future decentralized ART programs, particularly in rural, resource-constraint settings, as when only a minority of patients is engaged in an ART program where they receive regular monitoring, an increase in treatment failure and drug resistance can be foreseen.
Drug toxicity monitoring
Limited data were available to assess the feasibility of drug toxicity monitoring for patients on ART in decentralized settings. None of the included studies reported the proportion of patients on ART who received laboratory-based drug toxicity monitoring, but one RCT showed that the proportion of patients reporting toxic drug effects (defined as adverse events that required treatment interruption for >42 days) during the study period was higher than the total virological failure rate among patients on ART [25]. This finding is in line with results from other studies suggesting that drug toxicity is the most common reason for changing initial treatment regimen [42, 43]. The WHO guidelines emphasize that laboratory monitoring is not required for treatment initiation. However, there are major toxicities associated with ARV drugs that should be monitored in all patients on treatment. The basic monitoring for potential toxicity of drugs such as tenofovir, zidovudine and nevirapine require laboratory assessment of renal function, hemoglobin, and liver enzymes, respectively. Without the availability of, and access to, these basic tests, monitoring for ART toxicity cannot be performed, and could compromise the long-term effectiveness and sustainability of the ART program. Researches have showed that HIV patients on ART who have regimen substitution due to drug toxicity/drug related adverse reactions were at higher risk of loss to follow-up [44, 45] which may partly explain the significant reduction in number of patients in care after five years of follow-up reported from study included in this review [19].
Barriers related to treatment monitoring and evaluation of treatment monitoring under decentralization
Technological constraints
From a technology perspective, in the absence of point of care (POC) testing, access to laboratory monitoring for patients on ART under a decentralized model of care in low-resource settings will likely be limited. For VL monitoring; until the arrival of a true point of care VL test, the feasibility of VL monitoring for patients received ART at the primary clinic level will depend on system capacity to collect and process a blood sample, transport the sample to a central laboratory for testing and return the result in a timely manner. For immunological monitoring, there are CD4 POC technologies available that can be operated in decentralized settings and produce reliable results for treatment monitoring [46]; their use has been shown to improve access to this alternative monitoring method and increases patient retention along the HIV treatment cascade compared to conventional laboratory testing [47].
Human resource constraints
A lack of trained medical doctors for initiation and management of patients on ART has been identified as a major barrier for scaling up of ART programs [48, 49]. Task-shifting of HIV services from physician to non-physician carers has been introduced to overcome this challenge [4, 13]. From a treatment monitoring perspective, however, task-shifting does not come without challenges. Findings from our review suggest that increased clinical and administrative responsibilities associated with provision of nurse-led ART services could further burden the already-limited personnel at primary health care level. Primary health care staff reported their reluctance to put more PLWHA on treatment because of concern over their capacity to manage the burden of an increasing number of patients on ART. The quality of treatment monitoring could also be a concern as nursing staff were unable to identify and refer all cases of treatment failure at decentralized settings for regimen change, even with the availability of two consecutive VL monitoring results indicating virological failure. The lower than expected rate of patients initiated on second line ART may represent an appropriate strategy to optimize adherence before switching therapy but it may also indicate clinicians’ lack of confidence regarding interpretation of VL results and second line treatment. The introduction of any new assay into a clinical setting requires education of the clinician in its interpretation; this is especially the case with a complicated tool such as a VL test. On the other hand, early switching to second line ART after a single detectable VL test without appropriately addressing non-adherence issues would potentially result in the unnecessary initiation of second line ART and, without addressing poor adherence would lead to suboptimal second-line outcomes [50, 51]. This is an important issue of concern particularly in settings where treatment options are limited and second and third-line regimens are costly.
Recommendations
In LMICs the challenge of limited coverage of, and access to, treatment monitoring services that is associated with decentralization of HIV treatment and care often lies within the health care system; therefore a comprehensive strategy to improve the practice of treatment monitoring should be considered from a health system strengthening perspective (Fig. 2).
In terms of service delivery, treatment and treatment monitoring services should ideally be delivered close to where the patient lives, with appropriate diagnostic technology and human resource availability at the primary health care level. The development and implementation of POC technologies to provide immunological and virological monitoring are critically important to ensure appropriate treatment monitoring, particularly with further scale up of HIV treatment services in decentralized settings.
The impact of future studies towards improving the implementation of decentralized care would benefit from the inclusion of some standardized targets and outcomes in published reports. In the absence of clearly defined indicators and targets, the assessment and appraisal of coverage and quality of treatment monitoring services continues to be a challenge. Given the momentum in scaling up ART and towards achieving the 90-90-90 target, there is a need for standardized measures that can be used in many upcoming researches reporting global progress towards this ambitious goal. The development and adoption of a specific set of processes and target indicators regarding treatment monitoring could help to align the reporting system within different levels of health services provision, improve the timeliness of reporting results, and ensure that appropriate action is taken when results support particular interventions (e.g. adherence counseling).
Lastly, from governance and financing perspectives, it is obvious that if the ambitious “90-90-90” goal is to be achieved in 2020, the importance of treatment monitoring must be emphasized equally with the importance of treatment coverage. Substantial resources are required to ensure appropriate treatment monitoring for all people on ART. Critical to success is the assessment of system capacity, particularly human resources and health technology in delivering treatment monitoring. This must be conducted as an integrated component of the decision-making process in order to identify the optimal strategy to increase high quality coverage of HIV treatment and care services in any given specific setting. Expansion of ART coverage without considering system capacity for the provision of appropriate treatment monitoring to all patients will inevitably lead to more treatment failures and increased development of drug resistance, with resulting public health costs to address these problems. Therefore, the recommendation of WHO that lack of access to, or availability of, laboratory monitoring should not be a barrier in initiating patients on treatment may need to be revisited, as the closer we get to the second “90” goal of having 90% people diagnosed with HIV on treatment, the higher the importance of assuring that those patients who are on treatment are also appropriately monitored, such that the last “90” goal of having 90% people on treatment with viral suppression can be achieved.
Limitation
This review has some limitations that should be taken into account when interpreting the findings. Here, we identified only two studies that aimed to assess the monitoring and management of HIV patients. This paucity of data results in challenges regarding data interpretation and meant that we were unable to analyze and discuss differences in coverage of treatment monitoring services as well as quality of the services. Lack of information and data from unpublished government and program reports and studies published in non-English language may contribute to limited data availability. Moreover, limited data from studies conducted in SSA countries has made it difficult to generalize the findings outside the sub-Saharan African context.
Conclusions
The findings of this review suggest that there are potential major gaps in coverage and quality of treatment monitoring services for HIV patients on ART. Further studies particularly from non-SSA countries with longer-term of follow up are in need to assess the feasibility of treatment monitoring in the context of decentralization HIV treatment and care in LMICs. Significant investment in POC testing and, improving quality of and training for nursing staff to effectively manage patients on ART is required to improve quality of HIV treatment and care services. The development of a set of target program indicators for treatment monitoring is necessary to reinforce the importance of treatment monitoring in the HIV continuum of care toward achievement of the 90-90-90 goal by the year 2020.
Authors’ contributions
MP, SL, DA, SC developed review protocol. LR, MP performed literature search. MP, BP performed data extraction and drafted the manuscript. LR, BP, DA, SC, SL reviewed and commented on initial and final drafts of the manuscript. All authors read and approved the final manuscript.
Acknowledgements
The authors gratefully acknowledge the contribution to this work of the Victorian Operational Infrastructure Support Program received by the Burnet Institute. We thank Peter Higgs at the Burnet Institute for his valuable comments on the draft of the manuscript.
Competing interests
The authors declare that they have no competing interests.
Availability of data and materials
All data generated or analysed during this study are included in this published article.
Funding
Funding was provided by the National Health and Medical Research Council of Australia (NHMRC) (Project Grant GNT 1063725; Career Development Fellowship to S. Luchters, Principal Research Fellowship to S. Crowe, and Infrastructure for Research Institutes Support Scheme Grant). Minh Pham received support via an International Postgraduate Research Scholarship (IPRS) from the Commonwealth of Australia and the Victorian International Research Scholarship (VIRS) from State Government of Victoria, Australia.
Abbreviations
- ART
antiretroviral therapy
- PLWH
people living with HIV/AIDS
- LMICs
low and middle income countries
- SSA
sub-Saharan Africa
- SA
South Africa
- VL
viral load
- RCT
randomized control trial
- POC
point of care
Additional file
Contributor Information
Minh D. Pham, Email: minh.pham@burnet.edu.au
Lorena Romero, Email: L.Romeo@alfred.org.au.
Bruce Parnell, Email: bruce.parnell@burnet.edu.au.
David A. Anderson, Email: anderson@burnet.edu.au
Suzanne M. Crowe, Email: crowe@burnet.edu.au
Stanley Luchters, Phone: +61 0423 066185, Email: stanley.luchters@burnet.edu.au.
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Associated Data
This section collects any data citations, data availability statements, or supplementary materials included in this article.
Data Availability Statement
All data generated or analysed during this study are included in this published article.