Aethlon Medical Inc (AEMD)

[ANESRI]

The high comorbidity burden of the hepatitis C virus infected population in the United States

http://www.biomedcentral.com/1471-2334/12/86


Discussion

To our knowledge, this is the first study to systematically profile non-selected comorbidities in an HCV population. Nearly every HCV patient in our study had at least one comorbidity, and in general, these comorbidities were more common in the overall HCV infected case patients compared to the uninfected controls. In addition, comorbidities covered a wide range of diseases and symptoms affecting a number of body systems. Our findings substantiate that HCV is a systemic disease with many extra-hepatic features which highlight the urgency to treat these extra-hepatic conditions regardless of the liver disease itself. Individualized anti-viral treatment decisions for HCV infection should weigh the potential risks and benefits of both hepatic and extra-hepatic manifestations to increase the likelihood of treatment success.

Our insured study population reported a 47% current treatment rate, which is comparable to treatment rates (10-51%) in other US medical claims database studies [20-22]. There are multiple reasons why HCV patients may not be treated which include disease stage, patient choice and lack of access to liver specialists [23]. Non-liver specialists may decide that the patient is ineligible for treatment based on a list of contraindications, whereas liver specialists may otherwise safely treat the patient with relative contraindications (i.e. patients with cirrhosis and moderate thrombocytopenia) since most treatment regimens are individualized to achieve maximal sustained virological response. Treatment rates appear to be declining in the US, and it is estimated that from 2002-2030, only 14.5% of liver-related deaths caused by HCV will be prevented [24]; therefore, it is urgent to understand what barriers may exist that are preventing treatment uptake as the burden of HCV morbidity and mortality increases.

Up to one-third of our HCV population had a comorbidity that could potentially make them ineligible for antiviral HCV treatment. This indicates that a high proportion of the HCV population could potentially receive effective treatment if their comorbid conditions could be managed. A recent review has reported that the benefits of treatment can potentially reach a wider HCV population by including targeted groups such as active drug users and persons those with psychiatric illnesses [25]. These patients were able to complete antiviral therapy, achieve a sustained virological response, and did not develop adverse events that would require discontinuation of treatment. However, it was recommended that individualized management of these patients could be integrated within addiction and treatment services [26]. These studies suggest that some comorbidities can be effectively managed, increasing access to HCV treatment with successful outcomes.

Our findings confirm previous studies as we consistently observed the known comorbidities associated with HCV antiviral treatment and disease among our top ranked list, highlighting that our systematic evaluation supports how common these conditions are among the HCV infected population. However, three conditions, benign neoplasms, genitourinary symptoms, and viral infections, were identified in our ranked list and have not been previously reported to be associated with treatment or disease progression. The prevalence of benign neoplasms were mainly of the large bowel and skin (trunk and unspecified sites), which could possibly be explained by metastasis to these sites among HCV patients with HCC but its pathophysiology is unclear and warrants further study [27,15]. In our study, the prevalence of HCC was low, but we cannot exclude the possibility that this may be an underestimation if patients were diagnosed prior to the study period. HCV patients with genitourinary symptoms were mainly of hematuria and proteinuria [28] which could be clinical manifestations of glomerular kidney disease that is known to be associated with cryoglobulinemia and membranoproliferative glomerulonephritis [29]. For the unexpected finding of viral infections, the significance is difficult to interpret given the lack of specificity as almost half the cases were coded as non-specific viral infections.

Our HCV infected population was more likely to report comorbidities than the uninfected controls. This may be explained in part by the higher-risk or unhealthy behavior (e.g., alcohol and drug users) of those infected with HCV, making them more vulnerable to acquire new morbidities than the uninfected population. Indeed, prevalence of alcohol use and drug-use were much higher among the HCV infected compared to the uninfected population (alcohol; 7% vs. < 1%; drug use 15% vs. 3%, respectively). In addition, HCV-infected patients with health insurance may have closer follow-up care and higher rates of screening for other diseases than the uninfected, hence increasing the reporting of conditions. HCV-infected patients may also have more comorbidities because of the illness itself, which may place them at higher risk for other conditions. However, we identified disorders of lipid metabolism to be significantly lower among the HCV population compared to the uninfected population. This finding is not clearly understood since HCV infection is associated with enhanced lipogenesis that may lead to the pathological development of steatosis and metabolic syndromes such as insulin resistance, obesity, and HCC [18].