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. Author manuscript; available in PMC: 2011 Feb 15.
Published in final edited form as: Cancer. 2010 Feb 15;116(4):974–982. doi: 10.1002/cncr.24810

Knowledge of Hepatitis C Virus Screening in Long-Term Pediatric Cancer Survivors: A Report from the Childhood Cancer Survivor Study

Meagan Lansdale 1, Sharon Castellino 2, Neyssa Marina 1, Pamela Goodman 3, Melissa M Hudson 4, Ann C Mertens 5, Stephanie M Smith 6, Wendy Leisenring 3, Leslie L Robison 4, Kevin C Oeffinger 6
PMCID: PMC2819650  NIHMSID: NIHMS156710  PMID: 20041485

Abstract

Background

Pediatric cancer survivors who were treated before routine hepatitis C virus (HCV) screening of blood donors in 1992 have an elevated risk of transfusion-acquired HCV.

Methods

To assess long-term pediatric cancer survivors’ knowledge of HCV testing and blood transfusion history, a questionnaire was administered to 9,242 participants in the Childhood Cancer Survivor Study (CCSS) who are at risk for transfusion-acquired HCV following cancer therapy from 1970–1986.

Results

More than 70% of survivors reported either no prior HCV testing (41%) or uncertainty about testing (31%), with only 29% reporting prior testing. One-half recalled having a treatment-related blood transfusion; those who recalled a transfusion were more likely to report HCV testing (39%) than those who did not (18%) or were unsure (20%). In multivariate models, survivors who reported no prior HCV testing were more likely to be older (odds ratio [OR] per five-year increase, 1.1; 95% confidence interval [95% CI], 1.0–1.1) and to report no care at a cancer center within the past two years (OR, 1.2; 95% CI, 1.0–1.4), no cancer treatment summary (OR, 1.3; 95% CI, 1.2–1.5), and no transfusions (OR, 2.6; 95% CI, 2.3–3.0) or uncertainty about transfusions (OR, 2.2; 95% CI, 1.9–2.6), and less likely to be racial/ethnic minorities (OR, 0.9; 95% CI, 0.8–1.0) or survivors of acute myeloid leukemia (OR, 0.7; 95% CI, 0.5–1.0).

Conclusions

Many pediatric cancer survivors at risk for transfusion-acquired HCV are unaware of their transfusion history and prior testing for HCV and would benefit from programs to increase HCV knowledge and screening.

Keywords: cancer screening, late effects, survivorship, adverse treatment effects, chronic disease

INTRODUCTION

Hepatitis C virus (HCV) is the primary cause of chronic liver disease and liver transplantation in the United States.1 Based upon the 1999–2002 National Health and Nutrition Examination Survey (NHANES), at least 4.1 million Americans have been infected with HCV, of whom 3.2 million are chronically infected.2 Though many patients with chronic HCV are initially asymptomatic, the infection progressively impairs liver function and causes 10,000–12,000 deaths annually.1, 3 Two to three decades after first infection, 15–35% of patients develop cirrhosis, which increases the risk of hepatocellular carcinoma to 1–4% per year.3, 4 As the population ages, the burden of HCV-related morbidity and mortality is projected to grow substantially.57

Before the first blood donor screening regulations were adopted in the mid-1980s, an estimated 40% of HCV transmission resulted from blood transfusions.8 Pediatric cancer patients frequently require blood and blood products during therapy; thus, those who were treated before the current HCV blood donor screening methods were initiated in 1992 have an elevated risk of transfusion-acquired HCV. As in the general population, chronic HCV infection in pediatric cancer survivors is associated with liver fibrosis, cirrhosis, hepatocellular carcinoma, extra-hepatic manifestations, and impaired quality of life.915 In cancer survivors, these effects may be compounded by exposure to immunosuppressive and hepatotoxic chemotherapy.9, 12, 13, 15

Since the natural history of HCV infection may be modified by lifestyle choices (i.e. avoidance of alcohol) and clinical care (i.e. availability of antiviral therapy, liver function monitoring), patient knowledge of HCV status is of critical importance. Recognizing that some survivors are unsure of whether or not they received a transfusion or blood product during therapy, the Children’s Oncology Group recommends that all survivors who were treated prior to 1993 be screened for HCV.16 Importantly, survivors’ awareness of screening and their HCV status is largely unknown. This study aimed to assess survivors' knowledge of blood transfusion history and prior testing for HCV in a large and diverse population of childhood cancer survivors at risk for transfusion-acquired HCV.

METHODS

Study Population

The Childhood Cancer Survivor Study (CCSS) is a multi-institutional longitudinal cohort study tracking the health outcomes of long-term (≥5-year) cancer survivors who were diagnosed with leukemia, Hodgkin lymphoma, non-Hodgkin lymphoma, neuroblastoma, CNS tumor, kidney (Wilms) tumor, bone tumor, or soft tissue sarcoma before 21 years of age. All participants were diagnosed between 1970 and 1986 and treated at one of 26 participating institutions in the United States and Canada. The CCSS recruitment methodology and cohort characteristics have been described in detail previously.1719 All participants provided written informed consent prior to study initiation.

This analysis is limited to participants who completed the CCSS 2003 Follow-up Survey. At the time of the CCSS 2003 Follow-up Survey, there were 11,465 survivors who were alive and eligible for medical records abstraction. Of the 11,465 survivors, 1751 (15%) were passive or active non-respondents, 406 (3.5%) could not be located, and 66 (0.06%) did not respond to the HCV questions. Participants did not differ from non-participants by diagnosis, original cancer treatment, or age at diagnosis. However, participants were slightly more likely to be female (49% female in the participants vs. 43% in the nonparticipants, p <0.001) and slightly younger at the first contact (mean age at baseline contact 23.7 years vs. 24.3 years, p <0.001).

Cancer Treatment Information

Information regarding original cancer diagnoses was obtained for eligible cases from treating institutions. For all CCSS participants returning signed medical releases, information regarding primary cancer therapies was collected, including initial treatment, treatment for relapse, and (where applicable) preparatory regimens for bone marrow transplantation. Qualitative information was abstracted from medical records for 42 specific chemotherapeutic agents, for which quantitative dose information was abstracted on 22. Copies of radiation therapy records were obtained and centrally reviewed, including doses of cranial and craniospinal radiotherapy and total body irradiation. Importantly, during the era in which these patients were diagnosed and treated, blood transfusions were often administered in hospitals or settings outside of the treating institution. Thus, transfusion history was not included in the abstraction process. The treatment abstraction forms employed in data collection are available at www.stjude.org/ccss.

Main Outcome Measures

The primary outcomes of interest were survivors’ knowledge of prior testing for HCV and treatment-related blood transfusion history. The following three questions were asked: “Has a doctor or health care professional ever tested you for hepatitis C?”; “Did you receive a blood transfusion (red cells, platelets, fresh/frozen plasma) during your treatment for cancer?”; and “Have you received a blood transfusion for another reason either before your cancer was diagnosed or since you finished treatment?” Participants responded to all questions with “yes”, “no”, or “not sure” and provided their age at time of interest (test or transfusion). A small number of participants (N=74) who reported no treatment-related transfusions but recalled having a transfusion for another reason after 1993 (based on reported age) were excluded from some analyses since their recall of testing and transfusions may differ systematically from those at highest risk for transfusion-acquired HCV (treated/transfused before 1993). For exploratory purposes, though it was not a main outcome of the analysis, participants who reported a prior test for HCV were also asked to report the result of that test: “positive for hepatitis C (means that you are or have been infected)”, “negative for hepatitis C”, or “not sure”.

Independent Variables

Demographic and cancer-related information (age, gender, race/ethnicity, diagnosis, age at diagnosis) was collected previously through the CCSS. The CCSS 2003 Follow-up survey assessed socioeconomic status (health insurance, household income, and education) and health care practices during the previous two years. Participants were asked whether, during that two-year time period, they received care at a cancer center or clinic (yes vs no) or discussed HCV with a physician (yes vs no), and whether they currently had a written summary of their previous cancer treatment (yes vs no/not sure). The 2003 Follow-up questionnaire is available for download at www.stjude.org/ccss.

Statistical Analysis

The proportion of participants who self-reported prior testing for HCV (yes, no, not sure) or recalled having a treatment-related blood transfusion (yes, no, not sure) was described according to demographic characteristics, socioeconomic status, cancer-related factors, and health care practices. Within each blood transfusion response category, participants were further characterized by the proportion who reported a prior test for HCV. Associations between participant characteristics and reporting no prior HCV testing or uncertainty about testing (vs. prior testing) were assessed by univariate and multivariate logistic regression. All factors that were significant at the univariate level were included in the multivariate model and sequentially removed according to the Likelihood Ratio Test and a two-sided significance level of 0.05. All analyses were conducted with SAS version 9.1 (SAS Institute Inc., Cary, NC).

RESULTS

The most common cancer diagnosis in the study cohort was leukemia and the median age of participants was 6 years (range, 0–20) at diagnosis and 31 years (range, 17–54) at time of study. Most were non-Hispanic white (86%), were educated beyond high school (79%), had health insurance or were Canadian (88%), and had an annual household income greater than $20,000 (68%). Complete participant characteristics are provided in Table 1.

Table 1.

Characteristics of survivors according to self-reported history of prior test for Hepatitis C virus (HCV)

Self-Report of Prior Test for HCV
Characteristics Total Yes No Not sure
N N % N % N %
All Survivors 9242 2652 29 3758 41 2832 31
Diagnosis
  Acute lymphoblastic leukemia 2717 920 34 995 37 802 30
  Acute myeloid leukemia 233 103 44 58 25 72 31
  Other leukemias 184 61 33 58 32 65 35
  CNS tumor 1168 224 19 624 53 320 27
  Kidney (Wilms) 862 240 28 364 42 258 30
  Neuroblastoma 626 160 26 269 43 197 31
  Soft tissue sarcoma 815 231 28 344 42 240 29
  Bone cancer 759 225 30 298 39 236 31
  Non-Hodgkin lymphoma 699 193 28 268 38 238 34
  Hodgkin lymphoma 1177 295 25 479 41 403 34
Gender
  Female 4559 1339 29 1791 39 1429 31
  Male 4682 1313 28 1966 42 1403 30
Race/Ethnicity
  White, non-Hispanic 7917 2238 28 3204 40 2475 31
  Other 1325 414 31 554 42 357 27
Health Insurance
  No 1104 309 28 462 42 333 30
  Yes or Canadian 8064 2330 29 3256 40 2478 31
Household Income
  < $20,000 2914 843 29 1191 41 880 30
  ≥ $20,000 6066 1742 29 2456 40 1868 31
Education
  High school or less 1920 512 27 850 44 558 29
  Post-high school education 7202 2112 29 2858 40 2232 31
Age at Diagnosis (years)
  0–4 3756 1079 29 1566 42 1111 30
  5–9 2060 628 30 801 39 631 31
  10–14 1855 548 30 751 40 556 30
  15–20 1570 397 25 639 41 534 34
Age at Interview (years)
  15–24 2063 613 30 832 40 618 30
  25–34 4082 1234 30 1625 40 1223 30
  ≥ 35 3096 805 26 1300 42 991 32
Care at Cancer Center ≤ 2 y ago
  No 7943 2191 28 3359 42 2393 30
  Yes 1298 461 36 399 31 438 34
Physician Discussed HCV ≤ 2 y ago
  No 7830 1998 26 3285 42 2547 33
  Yes 519 444 86 44 8.5 31 6.0
Cancer Treatment Summary
  No 5758 1582 27 2471 43 1705 30
  Yes 2286 820 36 815 36 651 28
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Note: Total sample size for each variable may be less than 9242 due to missing values.

Of the 9,242 survivors in this analysis, 29% reported prior HCV testing, while 41% reported no testing and 31% were unsure (Table 1). Notably, even among those who received care at a cancer center within the previous two years, the proportion reporting prior HCV testing was little more than one-third (36%). Participants who reported having a recent discussion with their physician about HCV were much more likely to report testing (86%) than those who had no such discussion (26%).

Table 2 presents the proportion of survivors reporting prior testing for HCV according to self-reported history of treatment-related blood transfusions. One-half of survivors recalled having a treatment-related transfusion, and of those who recalled a transfusion, 39% reported prior testing for HCV, compared to 18% of those who recalled no transfusion and 20% of those who were unsure of their transfusion history. As expected given diagnosis-specific treatment protocols, there was wide variation in the proportion recalling a treatment-related transfusion among survivors of different cancer types, ranging from 31% of CNS tumor survivors to 84% of acute myeloid leukemia (AML) survivors. Although the proportion reporting HCV testing varied by diagnosis even among those who recalled a transfusion, it was never more than one-half (range, 31% to 46%), indicating substantial gaps in survivors’ knowledge of HCV. Of those who reported prior testing, 89% were unsure of the test result and 10% reported HCV positivity (data not shown).

Table 2.

Percent reporting prior testing for HCV, by self-reported history of blood transfusion or other blood product

Self-Report of Blood Transfusion History
Characteristics Total
(N=9168)		 Transfusion
(N=4573)		 No Transfusion
(N=3081)		 Unsure
(N=1514)
N % of total % tested % of total % tested % of total % tested
All Survivors* 9168 50 39 34 18 17 20
Diagnosis
  Acute lymphoblastic leukemia 2691 69 41 19 18 12 21
  Acute myeloid leukemia 231 84 46 8.2 47 7.4 18
  Other leukemias 184 68 42 18 12 14 19
  CNS tumor 1154 31 31 47 13 21 15
  Kidney (Wilms) 858 42 39 32 19 26 21
  Neuroblastoma 620 38 37 36 16 25 21
  Soft tissue sarcoma 812 40 39 41 20 19 22
  Bone cancer 756 56 38 31 20 13 19
  Non-Hodgkin lymphoma 691 47 36 38 19 15 22
  Hodgkin lymphoma 1170 31 40 56 19 13 16
Gender
  Female 4522 54 39 33 19 14 19
  Male 4645 46 39 35 17 19 20
Race/Ethnicity
  White, non-Hispanic 7857 50 39 34 17 17 19
  Other 1311 52 40 33 21 16 23
Health Insurance
  No 1093 49 35 29 18 22 25
  Yes or Canadian 8002 50 40 34 18 16 19
Household Income
  < $20,000 2889 50 38 32 19 18 20
  ≥ $20,000 6020 50 39 34 18 16 19
Education
  High school or less 1906 49 37 33 16 19 20
  Post-high school education 7142 50 40 34 18 16 20
Age at Diagnosis (years)
  0–4 3722 50 39 29 18 21 21
  5–9 2033 52 40 30 19 17 20
  10–14 1849 51 39 38 18 11 21
  15–20 1563 46 37 43 17 11 12
Age at Interview (years)
  15–24 2041 54 40 28 17 18 20
  25–34 4045 51 41 32 19 17 21
  ≥ 35 3081 46 36 39 18 15 17
Care at Cancer Center ≤ 2 y ago
  No 7875 48 37 34 18 18 20
  Yes 1292 60 48 31 18 8.9 12
Physician Discussed HCV ≤ 2 y ago
  No 7770 48 34 35 17 16 18
  Yes 515 81 90 11 66 7.8 72
Cancer Treatment Summary
  No 5713 48 37 36 18 16 20
  Yes 2269 57 46 30 19 13 27
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Includes only blood transfusions due to cancer treatment

*

Total (N=9168) excludes survivors who had a transfusion after 1993 for a non-cancer cause (n=74); subtotals within each category may be less than 9168 due to missing values

Univariate and multivariate comparisons of survivors who reported no prior HCV testing (or uncertainty about testing) versus a prior test for HCV are shown in Table 3. Nearly all participants who reported no prior HCV testing also reported not having a recent discussion with their physician about HCV (99%); thus, this variable was excluded from the multivariate analysis to identify other associations with the outcome of interest. In multivariate models, survivors who recalled not having a treatment-related blood transfusion or uncertainty about their transfusion history were two times more likely to report no prior testing for HCV (no transfusion: OR, 2.6; 95% CI, 2.3–3.0; uncertain: OR, 2.2; 95% CI, 1.9–2.6). Additional factors that were associated with reporting no prior HCV testing included: older age at study (per five-year increase, OR, 1.1; 95% CI, 1.0–1.1), no recent care at a cancer center (OR, 1.2; 95% CI, 1.0–1.4), and no cancer treatment summary (OR, 1.3; 95% CI, 1.2–1.5). Compared to Hodgkin lymphoma survivors, CNS tumor survivors were more likely to report no prior testing (OR, 1.5; 95% CI, 1.2–1.8) and AML survivors were less likely to report no prior testing (OR, 0.7; 95% CI, 0.5–1.0). Racial/ethnic minorities were also slightly less likely than non-Hispanic whites to report no prior testing (OR, 0.9; 95% CI, 0.8–1.0).

Table 3.

Comparison of 9168 survivors reporting no prior HCV testing versus those reporting a prior test for HCV

Univariate Model* Multivariate Model*
Characteristics OR 95% CI P-value OR 95% CI P-value
Diagnosis
  Acute lymphoblastic leukemia 0.7 0.6 – 0.8 <0.001 1.0 0.8 – 1.2 0.715
  Acute myeloid leukemia 0.4 0.3 – 0.6 <0.001 0.7 0.5 – 1.0 0.041
  Other leukemias 0.7 0.5 – 1.0 0.021 1.0 0.7 – 1.4 0.808
  CNS tumor 1.4 1.2 – 1.7 0.001 1.5 1.2 – 1.8 <0.001
  Kidney (Wilms) 0.9 0.7 – 1.1 0.159 1.0 0.8 – 1.3 0.884
  Neuroblastoma 1.0 0.8 – 1.2 0.818 1.1 0.9 – 1.5 0.372
  Soft tissue sarcoma 0.9 0.7 – 1.0 0.103 0.9 0.7 – 1.1 0.378
  Bone cancer 0.8 0.7 – 1.0 0.027 1.0 0.8 – 1.2 0.656
  Non-Hodgkin lymphoma 0.9 0.7 – 1.1 0.224 1.0 0.8 – 1.3 0.830
  Hodgkin lymphoma (referent) 1.0 1.0
Gender
  Female (referent) 1.0
  Male 1.1 1.0 – 1.2 0.159
Race/Ethnicity
  White, non-Hispanic (referent) 1.0 1.0
  Other 0.9 0.8 – 1.0 0.027 0.9 0.8 – 1.0 0.041
Health Insurance
  No 1.1 0.9 – 1.2 0.534
  Yes or Canadian (referent) 1.0
Household Income
  < $20,000 1.0 0.9 – 1.1 0.836
  ≥ $20,000 (referent) 1.0
Education
  High school or less 1.1 1.0 – 1.3 0.022
  Post-high school education (referent) 1.0
Age at Diagnosis (years)
  0–4 0.8 0.7 – 1.0 0.011
  5–9 0.8 0.7 – 0.9 0.001
  10–14 0.8 0.7 – 0.9 0.006
  15–20 (referent) 1.0
Age at Interview (years)
  Per 5-year increase 1.1 1.0 – 1.1 <0.001 1.1 1.0 – 1.1 0.006
Care at Cancer Center ≤ 2 y ago
  No 1.5 1.3 – 1.6 <0.001 1.2 1.0 – 1.4 0.012
  Yes (referent) 1.0
Cancer Treatment Summary
  No 1.5 1.3 – 1.6 <0.001 1.3 1.2 – 1.5 <0.001
  Yes (referent) 1.0 1.0
Transfusion History
  No transfusion 2.9 2.6 – 3.3 <0.001 2.6 2.3 – 3.0 <0.001
  Responded unsure 2.6 2.3 – 3.0 <0.001 2.2 1.9 – 2.6 <0.001
  Transfusion for cancer (referent) 1.0 1.0
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Total (N=9168) excludes survivors who had a transfusion after 1993 for a non-cancer cause (n=74); “No prior testing” includes survivors who were uncertain about prior testing

*

Models do not include “physician discussed HCV ≤ 2 y ago” because the strong association with “no prior testing” outcome may mask other associations

DISCUSSION

In this large cohort of pediatric cancer survivors at risk for transfusion-acquired HCV, less than 30% reported prior HCV testing. Fifty percent of survivors recalled having a blood transfusion during cancer therapy. For perspective, at St. Jude Children's Research Hospital, which maintained a record of blood transfusions administered during this time period, the following percent of survivors had a record of a blood transfusion: all patients, 58%; AML, 95%; ALL, 83%; Wilms tumor, 63%; osteosarcoma, 53%; neuroblastoma, 51%; Non-Hodgkin lymphoma, 48%; soft tissue sarcoma, 39%; Ewing's sarcoma, 34%; CNS tumor, 32%; Hodgkin lymphoma, 12%. Even among the 50% of CCSS survivors in our study who reported having a blood transfusion, only 39% reported a prior test for HCV. Awareness of HCV testing is essential for obtaining appropriate follow-up care and minimizing the effects of infection; thus, these gaps in knowledge constitute a serious public health problem that warrants attention.

Survivors who did not recall a therapy-related transfusion or were uncertain about transfusions were twice as likely as those who recalled having a transfusion to report no prior HCV testing. This suggests that health care providers may be more likely to test patients who know they were transfused, as recommended by the Centers for Disease Control and Prevention (CDC) and National Institutes of Health (NIH), rather than test all pediatric cancer survivors who were treated before 1993, as recommended by the COG.1, 3, 16 The 1993 cutoff date may vary for survivors treated outside North America, based on the timing of donor screening for HCV with the second generation ELISA in other regions. Since standard therapy for AML requires transfusion of blood or blood products, it is appropriate to assume that all AML survivors in this cohort had a transfusion. Notably, 84% of AML survivors recalled having a blood transfusion, but only 44% reported prior HCV testing (46% of those who recalled a transfusion). While awareness of transfusion history is certainly important, it does not seem to be sufficient to ensure HCV testing.

Knowledge of HCV testing and infection status is necessary for optimal patient care, particularly because the severity of disease may be minimized by careful clinical follow-up and pharmacological and lifestyle interventions. Evidence suggests that combination therapy with interferon-α and ribavirin is effective against chronic HCV in pediatric cancer survivors, with 44–67% achieving a sustained virological response.9, 20, 21 Changes in diet and physical activity may also modify the disease course, as obesity has been linked with more severe liver steatosis among pediatric cancer survivors with transfusion-acquired chronic HCV.9 Although alcohol is a well-known risk factor for more severe HCV-associated liver disease, recent data indicates that individuals with HCV report greater alcohol consumption than those without the disease, highlighting the importance of behavioral counseling in caring for patients with chronic HCV.2

Despite the availability of these strategies to minimize the burden of disease, several lines of research from the CCSS suggest that long-term survivors of pediatric cancer may be at particular risk of morbidity from transfusion-acquired chronic HCV, especially as they age. By 25 years after therapy, two-thirds of survivors in the CCSS reported at least one chronic condition and 38.5% reported two or more.22 In the same cohort, older age has been associated with greater risk of moderate to extreme adverse general health, functional impairment, activity limitations, and pain.23 The effect of these comorbidities on the clinical course of HCV is unknown, but may contribute to liver damage and declining health status and quality of life. In light of this, it is concerning that only 18% of more than 8,500 CCSS participants reported recent survivor-focused medical care with risk-based counseling or tests to screen for late effects.24 Older participants were less likely to report risk-based counseling and screening, just as older participants in this analysis were less likely to report prior testing for HCV. Together, these findings suggest that long-term pediatric cancer survivors at risk of transfusion-acquired HCV may be less likely to obtain appropriate clinical follow-up and HCV screening as they age, despite the increased risk of comorbidities and clinical manifestations of HCV attributable to a longer interval of time since cancer therapy and possible HCV exposure.

It is important to acknowledge that the risk of transfusion-acquired HCV has declined markedly over the past two to three decades, following the implementation of more stringent blood donor screening regulations.25 The second-generation HCV antibody screening test that has been used in North America since 1992 has lowered the estimated risk of infection to 0.001% per unit of blood, compared to 0.03% per unit with the first-generation antibody (1990–1991), 0.19% per unit with surrogate markers (1986–1990), and 0.45% per unit with HIV, syphilis, and HBV screening only (1985–1986).3, 25, 26 Most survivors in this study cohort were treated for cancer and exposed to blood or blood products prior to these regulations (1970–1980), when 10–12% of patients who received blood transfusions were infected with HCV.27, 28 Therefore, for many long-term pediatric cancer survivors alive today, the risk of transfusion-acquired HCV is not trivial.

Although we did not have access to blood samples to objectively measure the prevalence of HCV infection in this study cohort, we did ask participants who recalled prior HCV testing if they were or had ever been infected with HCV. Comparable to other U.S. cohorts that reported transfusion-acquired HCV infection rates of 6–12% in pediatric cancer survivors, approximately 10% of survivors in this study who recalled HCV testing also reported HCV infection.9, 13, 15 Of concern, 89% were unsure of their HCV status, indicating a widespread breakdown in knowledge and awareness.

In interpreting these study findings, several limitations warrant consideration. The primary outcomes, HCV testing and therapy-related transfusion history, were obtained by participant self-report and not verified by medical records or other sources. Of note, participants who were younger at the time of their cancer diagnosis (ie, less than 10 years of age), may have needed to rely upon the recall of their parents for whether or not they had a blood transfusion. Self-reported methods cannot provide objective measures of fact, but are well suited for characterizing subjective outcomes like knowledge and awareness, which was the primary focus of this analysis. Similarly, although the cohort was not biochemically tested for HCV, participant self-report of HCV status still provides important information about knowledge, which may influence health behaviors. Since this study was cross-sectional in nature, temporality of associations cannot be inferred, so that we cannot know, for example, whether HCV testing preceded or followed a recent physician’s discussion about HCV or a survivor’s recall of blood transfusion history.

The relatively low level of awareness about HCV testing and transfusion history that is documented in this study constitutes a serious public health problem. As survivors age, the impact of undetected chronic HCV on health and quality of life is likely to worsen, given the progressive nature of the infection. The importance of knowing one’s HCV status is underscored by the availability of clinical and behavioral strategies that can alter the disease course and minimize morbidity and mortality. Given the lack of understanding even among this relatively health conscious cohort of CCSS participants, there is an urgent need for interventions to educate and screen pediatric cancer survivors who may have undetected HCV following previous therapy-related blood transfusions. In conclusion, many pediatric cancer survivors at risk for transfusion-acquired HCV lack knowledge of their transfusion history and prior testing for HCV, and would benefit from public health programs to educate survivors and screen for this disease.

ACKNOWLEDGMENT

The Childhood Cancer Survivor Study (CCSS) is a collaborative, multi-institutional project, funded as a resource by the National Cancer Institute, of individuals who survived five or more years after diagnosis of childhood cancer. CCSS is a retrospectively ascertained cohort of 20,346 childhood cancer survivors diagnosed before age 21 between 1970 and 1986 and approximately 4,000 siblings of survivors, who serve as a control group. The cohort was assembled through the efforts of 26 participating clinical research centers in the United States and Canada. The study is currently funded by a U24 resource grant (NCI grant # U24 CA55727) awarded to St. Jude Children’s Research Hospital. Currently, we are in the process of expanding the cohort to include an additional 14,000 childhood cancer survivors diagnosed before age 21 between 1987 and 1999. For information on how to access and utilize the CCSS resource, visit www.stjude.org/ccss

Funding: This work was supported by Grant U24-CA-55727 (L.L. Robison, Principal Investigator) from the Department of Health and Human Services, funding to the University of Minnesota from the Children's Cancer Research Fund, and funding to St. Jude Children’s Research Hospital from the American Lebanese Syrian Associated Charities (ALSAC).

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