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Hepatitis C Screening: Barriers to Linkage to Care

  • Sammy Saab*,1,2,
  • Youssef P. Challita1,
  • Lisa M. Najarian1,
  • Rong Guo3,
  • Satvir S. Saggi1 and
  • Gina Choi1,2
 Author information
Journal of Clinical and Translational Hepatology 2019;7(3):226-231

DOI: 10.14218/JCTH.2018.00063

Abstract

Background and Aims: Hepatitis C (HCV) is a medical and public health concern. Once infected individuals are identified, management includes not only education but also the use of antiviral therapy. Although screening for HCV is readily available, barriers exist which prevent assessment and treatment in individuals potentially infected with HCV.

Methods: This is a retrospective study of patients screened for HCV within the University of California, Los Angeles Health Care System between February 22 and July 9, 2018. We defined linkage to care as: 1) confirmatory HCV RNA test after screening HCV antibody test found a positive result; and 2) follow-up appointment for treatment was established with a specialist. Demographic and baseline laboratory values were collected. Factors potentially associated with prohibiting linkage of care were evaluated.

Results: During the study period, 17,512 individuals were screened for HCV. A total of 238 (1.35%) were found to have detectable HCV antibodies. Of the individuals with detectable HCV antibodies, 48 (20%) did not undergo confirmatory testing with viral levels. Of the 190 individuals who underwent further testing, 70 patients were noted to be viremic. Among them, 17 of the 70 (24%) were not linked to a specialist for further care. Younger patients (p = 0.02) and people who inject drugs (p = 0.02) were less likely to be referred for specialty care.

Conclusions: The results of our study highlight that younger patients and people who inject drugs are less likely to be referred to specialty care for HCV treatment. Efforts are needed to engage these populations.

Keywords

Hepatitis C, Screening, Linkage

Introduction

Hepatitis C is a viral infection with significant hepatic and extra-hepatic manifestations.1 Not only is hepatitis C a common cause of cirrhosis, it is a major risk factor for hepatocellular carcinoma and one of the leading indications for liver transplantation.2 Moreover, its extra-hepatic manifestations include varied expressions of glomerulonephritis, cryoglobulinemia, and lymphoma.3–5

The largest cohort of individuals infected with hepatitis C virus (HCV) are the baby-boomers, people born between the years 1945 and 1965.6 Although there are multiple risk factors for this blood-borne infection, many individuals may have been infected through blood transfusions before HCV was identified and blood products were screened for the virus.7 Thus, a significant number of infected individuals are unaware of their infection status.8 The treatment of HCV has evolved from therapies that were associated with significant adverse effects to the development of all-oral direct acting therapies that are highly effective, safe, and tolerable.9 Consequently, major health care societies recommend screening patients for HCV based on their age, in addition to risk factors and recommended therapy to all infected individuals regardless of severity of fibrosis as long as their prognosis is at least 1 year.10 Identifying those infected is the first step toward the elimination of HCV.11,12

There is a cascade of events that begin with identifying HCV infected individuals and continue toward treatment. The biggest limitation appears to be identifying those infected.13 Screening for HCV relies on testing for antibodies of the virus and then confirming the presence of infection by measuring the viral load. After HCV infection is confirmed, patients should be linked to care with a provider experienced in treating HCV.10 However, there are a number of limitations that can exist in every stage of care. The hypothesis of our study is that most barriers to HCV treatment are modifiable. We reviewed the cascade of events following screening for HCV in order to identify barriers for linking patients infected with HCV to care.

Methods

Screening

All patients found to have detectable HCV antibodies for hepatitis C at the University of California, Los Angeles Healthcare System during the study period between February and July 2018 were identified using an administrative database.14 Ordering providers were alerted of the results by the laboratory. We also contacted providers of patients with positive enzyme-linked immunosorbent assay results. Our coordinator recommended additional laboratory testing in the form of an HCV RNA quantitative PCR with reference to genotype and offered to facilitate a clinic appointment with a Hepatologist.

We collected data on patients’ age, gender, health insurance type, health care setting of antibody screening, home zip code, homeless status, injection drug usage and laboratory test results. The zip code was used to estimate the patients’ socioeconomic status.15 We also recorded the time between antibody and RNA testing, and the number of emails sent to the primary providers until a response was obtained. The health care setting was stratified according to whether testing occurred during hospitalization, emergency department visit, or clinic visit. Clinics were further stratified if there were single specialty (by Primary Care Providers) or multispecialty (not including Gastroenterology or Hepatology physicians).

Successful linkage to care was assessed in two separate ways: 1) if the patient underwent testing for RNA (testing linkage); and 2) if the patient was referred to a hepatitis C specialist if they were viremic (specialty linkage). Patients were given 3 weeks from their positive antibody result to undergo HCV RNA testing. Patients who tested for HCV viremia within the 3-week period met the criteria for successful testing linkage to care. Barriers to linkage of care were recorded for both assessments.

Statistics

Outcomes at both the testing linkage and specialty linkage levels were assessed. Standard descriptive analyses, median (interquartile range [IQR]), n (%), and univariate analysis were conducted using Microsoft Excel 15.2 (Microsoft, Seattle, WA, USA) by testing linkage or specialty linkage. Further analysis was conducted in the form of chi-squared, Fischer’s exact tests, and multivariate logistic regression using the Statistical Analysis Software version 9.4 (SAS Institute Inc., Cary, NC, USA).

Results

A total of 17,512 patients were screened during the study period, among whom 238 were found to have detectable HCV antibodies (Fig. 1). The median (IQR) age of patients found to be HCV antibody positive was 59 (47–66) years (Table 1). Most of the patients were male and had commercial insurance. Most of the patients were tested in primary or multispecialty clinics, and lived within 10 miles of the site of testing. Few patients were homeless or people who inject drugs (PWID). Median (IQR) liver-associated factors and platelet test results are shown in Table 2. The median (IQR) aspartate aminotransferase to platelet ratio index was 0.3 (0.2–0.5).

Cascade of care.
Fig. 1.  Cascade of care.
Table 1.

Overall demographics and hepatitis C viral load assessment

Variable not testedTotal, n = 238HCV RNA tested, n = 190HCV RNA, n = 48
Median age (IQR), years59 (47–66)59 (46–66)61 (51–67)
Gender – M/F, %150/88 (63/37%)118/72 (62/38%)32/16 (67/33%)
Insurance type
 Private97 (40%)81(43%)16 (33.3%)
 Medicare59 (25%)45 (24%)14 (29.2%)
 HMO59 (25%)45 (24%)14 (29.2%)
 Medi-Cal19 (8%)16 (8%)3 (6.3%)
 No insurance4 (2%)3 (1%)1 (2%)
Health care setting
 Hospital84 (35%)69 (36%)15 (31%)
 ER17 (7%)14 (7%)3 (6%)
Clinic
 Single specialty65 (27%)51 (27%)14 (29%)
 Multispecialty72 (30%)56 (30%)16 (33%)
Median distance (IQR), miles†9.0 (3.6–24.3)9.3 (3.6–22.8)7.4 (3.6–30.8)
Median household income (IQR), thousand$72 (53k-86)$72 (51k-86)$71 (55k-90)
Homeless34 (14%)26 (14%)8 (17%)
PWID33 (14%)27 (14%)6 (13%)
Table 2.

Median laboratory values of hepatitis C antibody-positive patients

VariableTotal, n = 238HCV RNA tested, n = 190HCV RNA not tested, n = 48
Platelet count (IQR),1/L221 (182–279)218 (178–279)228 (194–278)
AST (IQR), U/L28 (19–44)28 (19–45)28 (20–37)
ALT (IQR), U/L25 (17–49)25 (16–50)32 (18–43)
Total bilirubin (IQR), mg/dL0.4 (0.3–0.7)0.4 (0.3–0.7)0.6 (0.3–0.7)
APRI (IQR)0.3 (0.2–0.5)0.3 (0.2–0.6)0.3 (0.2–0.4)

A total of 190 (79%) out of the 238 patients with detectable HCV antibodies were further assessed for HCV viremia, of which 70 (37%) had detectable viral levels. Forty-eight patients with detectable HCV antibodies did not undergo viral load testing. Of the 48 patients who did not undergo HCV RNA testing, the test was not ordered by the provider for 27 patients. For the remaining 21 of the 48 patients, the test was ordered but not completed by the patient. Demographic comparison of the patients who were and were not checked for HCV viremia is shown in Table 1, and laboratory results in Table 2. There were no statistically significant differences in the demographics and lab results between these two groups.

A total of 53 out of the 70 (75%) patients with HCV viremia were referred to specialty care for further treatment. Demographics and laboratory values of patients who were and were not referred for specialty care are shown in Tables 3 and 4. Patients who were not referred for specialty care were younger (median age of 48 vs 60, p = 0.02), and more likely to be PWID (8/17, 47% vs 9/53 17%, p = 0.02). In a multivariate logistic regression analysis including age and PWID as independent variables, the adjusted odds ratio for PWID was 0.31 (p = 0.07, 95% confidence interval [CI]: 0.09–1.09) and the adjusted odds ratio for age was 1.03 (p = 0.09, 95% CI: 1.00–1.07). In addition, we examined the interaction between age and PWID; the interaction effect was not significant and thus excluded from the model (p = 0.50). The reasons provided by laboratory ordering providers for not referring are listed in Table 5. The most common reason for lack of specialty care was that the patient did not attend the appointment.

Table 3.

Demographics of patients referred and not referred to specialty care

VariableReferred, n = 53Not referred, n = 17
Median age (IQR)60 yrs (49–67)48 yrs (30–58)
Gender – M/F (%)33/20 (62%/38%)11/6 (65%/35%)
Insurance type
 Private24 (45%)6 (35%)
 Medicare13 (25%)2 (12%)
 HMO9 (17%)7 (41%)
 Medi-Cal7 (13%)2 (12%)
 No insurance00
Medical setting
 Hospital23 (43%)8 (46%)
 ER3 (6%)4 (24%)
Clinic
 Single specialty13 (25%)1 (6%)
 Multispecialty14 (26%)4 (24%)
Distance from home to clinic (IQR), miles3.6 (3.4–15.9)8.9 (3.5–18.0)
Median household income (IQR), thousand$72 (51–82)$57 (56–73)
Homeless8 (15%)6 (35%)
PWID9 (17%)8 (47%)
Table 4.

Median laboratory values according to specialty referral in hepatitis C viremic patients

VariableReferred, n = 53Not referred, n = 17
Platelet count (IQR), 1/L204 (175–259)256 (183–270)
AST (IQR), U/L38 (29–53)35 (26–63)
ALT (IQR), U/L40 (22–61)39 (24–75)
Total bilirubin (IQR), mg/dL0.5 (0.3–0.8)0.5 (0.3–0.8)
APRI (IQR)0.4 (0.3–0.6)0.3 (0.2–0.5)
Table 5.

Failures in Linkage to care by specialty linkage definition, n = 17

Unsuccessful linkage reasonsn
Physician deferred treatment6
 Upcoming kidney transplant1
 Primary care physician will proceed with treatment1
 Physician states patient will not follow through with treatment3
 Patient fled facility1
Physician did not respond to linkage request via email4
Patient noncompliant to referral7

Discussion

The results of this study highlight the disparity between HCV screening and linkage of care. In our study, approximately 27% of patients who were found to have detectable HCV antibodies were not linked to either further testing or specialty care. We identified barriers to care and offering suggestions to mitigate these limitations. The definition of linkage to care varies across studies. Studies have defined linkage as confirmatory HCV RNA testing in patients found to have HCV antibodies,16–19 referral to specialty clinics among viremic patients,8,20–29 or both.30–35 Two studies defined linkage to care as receiving HCV RNA testing, referral to specialty care and attending the first appointment with the specialist.36,37 Several studies defined linkage to care as attending the first appointment with a provider and starting viral treatment,38–40 whereas two studies defined linkage to care as being seen by a specialist.41–43 In our study we defined linkage separately so we can better understand the limitations of care.

HCV infection possesses a number of characteristics that make elimination feasible, including the lack of a non-human reservoir, easy diagnosis, and effective curative treatment.11 Indeed, the World Health Organization proposes that viral infection can be eliminated within the next two decades provided that the diagnosis rate is 90%, the treatment rate is 80%, and the curative rate is 90%.44,45 However, the results of our study highlight barriers to HCV elimination. Not only are there significant deficiencies in screening in the USA46 but a major gap exists between the diagnosis and treatment. The results of our study, as well as of others, suggest that the biggest obstacle to curing infected patients is linkage of care. Concentrated efforts are essential to bridge the gap.

This study demonstrated the important predictors of lack of linkage to specialty care for hepatitis C were being a young adult and a PWID. The odds of receiving specialty care decrease by 70% for PWID (odds ratio = 0.31, 95% CI: 0.087–1.099, p = 0.07). Similarly, for every unit decrease in age (years) the odds of being linked to specialty care decreases by 3% (odds ratio = 1.032, 95% CI: 0.996–1.072, p = 0.09). This finding is of particular concern as PWIDs likely represent one of the fastest growing cohorts of HCV infection in the USA. In fact, in over a dozen states in this country, the HCV prevalence among young individuals is as high or higher than among baby-boomers.47 If HCV elimination is truly a goal, we must better engage this population. Several proposals to include HCV linkage to care among PWID include utilization of a multidisciplinary approach, fostering better communication, and increasing awareness of the implications of HCV infection.22,23,48

There are several limitations to our study. The most important is its retrospective nature. For many of our patients who were not linked to care, the reasons could only be projected. Nevertheless, thorough review of the medical record and discussions with the primary providers important insights were provided. Another important limitation is that we could not exclude selective screening in our cohort. The current practice for screening involves an opt–in approach, whereby a provider is alerted that their patient is a baby-boomer and should be considered for HCV screening, according to the Center for Disease Control guidelines.7 Moreover, providers also screened patients based on risk factors for viral hepatitis C. Nonetheless, our entire cohort of patients screened consisted of almost 18,000 patients. Another limitation is that our study cohort may not reflect the general population of patients with HCV. For instance, the viremic rate in patients with detectable HCV antibodies was 37%, which is substantially lower than described by others in the literature. One possible reason is that patients with HCV antibodies, but undetectable HCV RNA viral levels, may have been previously treated. We do not think this accounts for a substantial number of our aviremic patients since in that situation there would be no medical indication for screening. Moreover, there has been a trend noted in the literature of lower viremic rates in screening programs.34 Another limitation to our study is that patients were not directly contacted for reasons for not following up with viral load testing or appointment for treatments. Prospective studies may help clarify additional patient level barriers than what we described in our retrospective study.

The results of our study highlight that deficiencies exist in extending HCV-related care in the fastest growing infected cohort in the USA, particularly for the young and PWID. For HCV elimination policy to be effective, these cohorts must be engaged.

Abbreviations

CI: 

confidence interval

HCV: 

hepatitis C virus

IQR: 

interquartile range

PWID: 

people who inject drugs

Declarations

Acknowledgement

The research described was supported by NIH/National Center for Advancing Translational Science (NCATS) UCLA CTSI Grant Number UL1TR001881.

Conflict of interest

The authors have no conflict of interests related to this publication.

Authors’ contributions

Contributed to study concept and design (SS), acquisition of data (YPC, LMH, SSS), analysis and interpretation of data (SS, YPC, LMN, GC), drafting of the manuscript (SS, YPC), critical revision of the manuscript for important intellectual content (SS, YPC, GC), statistical analysis (RG, YPC), administrative, technical, or material support (SS), study supervision (SS, GC), and guarantor of the article (SS). All authors approved the final version of the manuscript.

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