Vertical transmission has become the most common mode of transmission of hepatitis C virus (HCV) in children. The rate of perinatal transmission from an HCV-infected mother to her child ranges from 2% to 5% and the prevalence of HCV in children in developed countries ranges between 0.1% and 0.4%. Spontaneous viral clearance seems to be dependent on the genotype and has been reported between 2.4%-25%. For chronically infected patients, treatment with recombinant polyethylene glycol (PEG)-interferon α-2b and daily ribavirin has now been approved as standard treatment for children 2-17 years of age. In five large prospective studies, a total of 318 children and adolescents aged 3-17 years were treated either with subcutaneous PEG-interferon α-2b at a dose of 1-1.5 μg/kg or 60 μg/m² once a week in combination with oral ribavirin (15 mg/kg per day) or PEG-interferon α-2a with ribavirin. Subjects with genotype 1 and 4 received the medication for 48 wk and individuals with genotype 2 and 3 mainly for 24 wk. Overall sustained viral response (SVR) was achieved in 193/318 (60.7%) of treated patients. Stratified for genotype; 120/234 (51%) with genotype 1, 68/73 (93%) with genotype 2/3, and 6/11 (55%) with genotype 4 showed SVR. Relapse rate was between 7.7% and 17%. Overall, treatment was well tolerated; however, notable side effects were present in approximately 20%. According to recent experiences in the treatment of chronic hepatitis C in children and adolescents, a combination of PEG-interferon α with ribavirin has been found to be well tolerated and highly efficacious, particularly in individuals with genotype 2/3. Thus, this treatment can be recommended as standard of care until more effective treatment options will become available for genotype 1 patients.

Combination therapy of polyethylene glycol (PEG)-in-terferon α-2a or α-2b with ribavirin is standard of care for adults with chronic hepatitis C. Clear benefits in terms of sustained viral response (SVR) and side effect profile have been documented with PEG-interferon α compared with recombinant interferon α with and without ribavirin. An additional advantage of the pegylated form of interferon is the extended serum half-life, which allows a once-weekly administration regimen. Until recently, only recombinant interferon α-2b in combination with ribavirin had been approved by the Food and Drug Administration (FDA) and European Medicines Agency (EMA) for use in children and adolescents. Since December 2008 and September 2009, respectively, the FDA and EMA approved PEG-interferon α-2b in combination with ribavirin in the United States and Europe for children aged 3 years and older[1]. Although most experts believe treatment is beneficial, due to several factors associated with treating young patients with chronic hepatitis C, this topic remains controversial[2-4]. However, there is no doubt that chronic hepatitis C remains an epidemiologically important health care issue in children and adolescents. Associated costs in the United States are estimated between $17 and $40 million annually[5]. Effective treatment of chronic hepatitis C virus (HCV) at an early age would help to prevent the long-term sequelae of chronic infection, improve the prognosis of patients, and reduce health care expenditure.

The prevalence of HCV in children in developed countries ranges between 0.1% and 0.4% but may even exceed 10% in some regions of Saudi Arabia and Africa[6-8]. The rate of perinatal HCV transmission from an infected mother to her child ranges from 2% to 5%. Clinically most relevant are genotypes 1, 2 and 3; considerably less spread is genotype 4[2]. It is estimated that there are 1 million individuals aged less than 18 years infected with chronic hepatitis C worldwide[9].

Since the early 1990s, transmission of HCV infection has occurred predominantly by parenteral transfusion of blood products or by non-use of disposable syringes. However, transfusion-associated hepatitis C has now become extremely rare in countries with adequate hygienic facilities. Subjects who were particularly at risk such as premature infants, hemophiliacs, patients with thalassemia, and children with malignant diseases or organ transplantations have now reached adulthood and vertical transmission from HCV-infected mothers to their offspring has become the most common cause of chronic hepatitis C in children. Importantly, in the case of vertical infection, the chronicity rate is very high[10].

Children chronically infected with HCV may be at risk for social disintegration and impaired quality of life. A possible psychological burden may be present and some physical impairment has been described. To date, only two rather small studies have been published reporting significantly lower physical and psychosocial scores and worse cognitive functioning compared with non-infected controls[11,12].

Spontaneous viral clearance in vertically infected children seems to be dependent on genotype and was found to range from 2.4%-25%[13,14]. It may be higher in parenterally infected individuals and was reported to reach 35%-45% by adolescence[15,16]. Children infected with genotype 3 have a higher spontaneous clearance rate than those infected with genotype 1. Beyond the age of 4 years, spontaneous viral clearance seems to become rather unlikely[13]. Patients who do not clear the virus within the first years of life will develop chronic hepatitis C. Overall, the cumulative probability of progression to chronicity is approximately 80%[17,18]. Most children are clinically asymptomatic or show only mild unspecific symptoms. In roughly 10% of patients, hepatomegaly may be present[17]. During the chronic course, alanine aminotransferase (ALT) levels may be normal or intermittently elevated. Only few patients show persistent markedly elevated ALT levels. Inflammatory activity in liver tissue is usually mild and the risk of severe complications is low. However, despite the favourable prognosis during the first and second decade of life, approximately 4%-6% of children will develop evidence of advanced liver fibrosis or cirrhosis[19,20]. A recently published study in pediatric patients with chronic hepatitis C cured of malignancy reported liver cirrhosis in 5% after three decades of observation[21]. Progression of fibrosis depends on age and additional risk factors such as obesity and alcohol consumption. Thus, progression usually starts beyond the second life decade and there is evidence that it seems to proceed more rapidly in patients with genotype 3[22]. Large liver transplantation units have reported on children who needed liver transplantation due to progressive HCV infection[23].

Many years ago, treatment started in adults with the use of interferons, yielding SVR rates in the 10%-15% range. According to the use of different treatment regimens and small numbers of treated children, it was difficult to compare the response rates in children to those in adults. Overall, SVR seemed to be better in children. Nineteen studies using recombinant α-interferon were published between 1992 and 2003[24]. A meta-analysis of trials with interferon-α monotherapy revealed a wide range (0%-76%, mean 27%) of SVR. Subjects infected with genotype 2 and 3 clearly responded better than patients harbouring genotype 1. Based on an increasing number of randomized controlled trials in adults, ribavirin was added to interferon-α in treatment trials for children. Between 2000 and 2005, six studies were published all demonstrating an SVR from 27% to 64%[25]. The stratification according to genotypes showed a very good response (> 80%) in patients with genotype 2 and 3 and an SVR of approximately 36%-53% in those with genotype 1. Results of an extensive trial in children published by Gonzalez-Peralta led to the approval of recombinant interferon α-2b in combination with ribavirin[26].

However, when PEG-interferon in combination with ribavirin became the standard of care for adults with chronic hepatitis C, trials in children promptly started. Some advantages were present such as a reduced injection frequency to once per week, better SVR, and better interferon tolerance. Interestingly, the sole controlled randomized trial, comparing a pegylated interferon α (PEG-interferon α-2a) with and without additional ribavirin, was only published in 2011. It clearly demonstrated that in the pediatric age group, the addition of ribavirin was necessary to obtain significantly better treatment results[27]. Specifically, in genotype 1 patients, SVR rate was 17% with PEG-interferon monotherapy compared with 47% in individuals with combination treatment. The difference was also striking in subjects infected with genotype 2 and 3 (36% vs 80%).

Up to now, results of seven trials using PEG-interferon α in combination with ribavirin have been reported[27-32]. SVR rates in patients with genotype 1 from 5 trials with more than 30 patients ranged from 44% to 59%. Achieving SVR in children with genotype 2 and 3 was very successful and yielded rates of more than 90%. The relapse rate was between 7.7% and 17%. Four trials used PEG-interferon α-2b and two used PEG-interferon α-2a in combination with ribavirin. An additional report presented the retrospective data in 33 treated Japanese children and young adults[33]. SVR rate in these patients was approximately 82%. Unfortunately, no information regarding genotypes was provided. Table 1 and Figure 1 summarize the characteristics of the five prospective studies. Peg-interferon α-2b and ribavirin were approved for patients aged 3 to 17 years of age by the FDA in December 2008 and the EMA in September 2009.

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Figure 1 Distribution of genotypes in the five representative prospective trials using polyethylene glycol-interferon α-2b and polyethylene glycol-interferon α-2a in combination with ribavirin, published between 2005 and 2011.

Baseline viral load

Two studies stratified the results in genotype 1 patients according to the viral load before treatment. In the first study, the cut-off level was 600  000 IU/mL: 32% of children with genotype 1 and high viral load (> 600  000 IU/mL) and 73% with low viral load (< 600  000 IU/mL) achieved SVR[32]. In the second trial, the cut-off value was 500  000 IU/mL: 45% of children with genotype 1 and > 500  000 IU/mL and 62% with < 500  000 IU/mL achieved SVR[30].

Figure 2 summarizes the SVR in relevant pediatric trials using PEG-interferon in combination with ribavirin.

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Figure 2 Sustained viral response in five large prospective trials with polyethylene glycol-interferon α-2b¹/α-2a² and ribavirin stratified for genotype and viral load[27,28,30-32]. G: Genotype; HVL: High viral load, > 600  000 U/mL, (Wirth et al[32]), > 500  000 U/mL (Sokal et al[30]); LVL: Low viral load, < 600  000 U/mL (Wirth et al[32]), < 500  000 U/mL (Sokal et al[30]).

The majority of treated children and adolescents will tolerate PEG-interferon and ribavirin well. Nevertheless, almost all patients will experience at least one side effect. The clinical significance of adverse events is summarized in Table 2. Most adverse events are mild to moderate, such as flu-like symptoms including fever, anorexia, fatigue, dry skin and moderate hair loss. In some patients, dose reduction of PEG-interferon may be necessary due to decreased white blood cell counts. Severe anemia is very rare; hence, the need for dose reduction of ribavirin is extremely infrequent. The rates of discontinuation of treatment due to adverse events were low in all trials published. Severe psychiatric side effects were rare in pre-pubertal individuals, but may be of significance in affected individuals. Appearance of thyroid autoantibodies and thyroid dysfunction during long-term treatment (> 24 wk) has to be considered and carefully monitored. Up to 20% of treated patients, particularly with genotype 1, may have abnormal thyroid stimulating hormone levels or other signs of thyroid dysfunction[31,35]. Another notable side effect is transient growth impairment. Inhibited growth can be observed in 50%-70% with decrease of growth velocity below the 3rd percentile. Shortly after the end of treatment, catch-up growth usually starts with an increased growth velocity followed by achievement of previous growth velocity levels, which can be observed during the follow-up period. Nevertheless, if possible, treatment during pubertal growth spurt should be avoided[36]. In addition, weight loss is very common during the treatment phase; however, most patients experience compensatory weight gain after treatment ends[32]. Regarding quality of life, and behavioral, emotional and cognitive outcomes during and after treatment, no significant impairment has been detected in the PEDS-C trial[37]. More follow-up studies are in progress to evaluate long-term sequelae.

There is no doubt that treatment response in patients with genotype 1 is not entirely satisfactory and improved treatment regimens are desirable. A number of directly acting antiviral agents, designed to target viral encoded proteins essential to the HCV life cycle, are currently under development. Phase III trials in adults have been completed for two protease inhibitors (telaprevir and boceprevir) and have shown a significantly increased viral elimination rate in combination with PEG-interferon and ribavirin[38-40]. Brand new data indicate that in a considerable number of patients with rapid response, exposure to PEG-interferon and ribavirin may be shortened and response-guided therapy will become the treatment of choice[41]. Approval of telaprevir and boceprevir has been sanctioned by the FDA and EMA in 2011, and pediatric trials will follow in the near future. In adults, genotype 1 non-responders have also demonstrated SVR rates ranging between 59% and 66%, depending on the duration of boceprevir treatment, compared to 20% with standard of care[42]. Given that efficacy data could be extrapolated from adults to children, an approved triple therapy regimen should be expected for non-responders. Nevertheless, they should definitely be included in future pediatric trials[36].

In children and adolescents, PEG-interferon treatment in combination with ribavirin for 48 wk produces a sustained viral response rate in approximately 50% of adequately treated individuals. Thus, this option can be offered to all patients irrespective of the level of aminotransferases or mode of infection. There is evidence that subjects with low viral load may respond better than patients with high viral load. In patients infected with genotype 2 or 3, a 90% or even better SVR rate can be achieved. Thus, treatment for 24 wk should be administered in all patients with genotype 2 and 3. According to the approval of the drugs, treatment start is possible beyond three years of age. However, because spontaneous viral elimination may occur within the first 4-5 years of life in vertically infected individuals, watchful waiting for up to five years of age is a justified alternative to an early treatment start. Additionally, different individual and family variables may influence the appropriate time to initiate therapy. An experienced pediatric gastroenterologist should supervise the management of treating these patients. Mid-childhood age before pubertal growth spurt is preferable. Table 3 summarizes pros and cons to indicate or possibly to defer treatment. Adverse events are usually well tolerated, but severe side effects may occur in a small number of patients making dose adjustment necessary. Overall, the encouraging results, particularly in patients with relatively low viral load and/or favourable genotypes and in line with an appropriate consideration of early stopping rules, endorse application of treatment in eligible patients. Re-treatment in non-responding genotype 1 patients should be deferred until a combination of standard care with direct acting antivirals has become available.