Literature DB >> 28336739

Disparities between research attention and burden in liver diseases: implications on uneven advances in pharmacological therapies in Europe and the USA.

Nambi Ndugga1, Teisha G Lightbourne2, Kavon Javaherian2, Joaquin Cabezas1, Neha Verma2, A Sidney Barritt1, Ramon Bataller1.   

Abstract

OBJECTIVES: Effective oral therapies for hepatitis B and C have recently been developed, while there are no approved pharmacological therapies for alcoholic and non-alcoholic fatty liver diseases (ALD and NAFLD). We hypothesise that fewer advances in fatty liver diseases could be related to disparities in research attention.
METHODS: We developed the Attention-to-Burden Index (ABI) that compares the research activities during 2010-2014, and an estimate of disease burden of these 4 major liver diseases. The resulting ratio reflects either overattention (positive value) or inadequate attention (negative value) compared with disease burden. The mean research attention and disease burden were calculated from 5 and 6 different parameters, respectively. The efficacy rate of current pharmacological therapies was assessed from published clinical trials.
FINDINGS: The mean research attention for hepatitis B and C was 31% and 47%, respectively, while NAFLD and ALD received 17% and 5%. The overall burden was 5% and 28% for hepatitis B and C, and 17% and 50% for NAFLD and ALD. The calculated ABI for hepatitis B and C revealed a +6.7-fold and +1.7-fold overattention, respectively. NAFLD received an appropriate attention compared with its burden, while ALD received marked inadequate attention of -9.7-fold. The efficacy rate of current pharmacological agents was 72% for hepatitis B, 89% for hepatitis C, 25% for non-alcoholic steatohepatitis and 13% for alcoholic hepatitis. Importantly, we found a positive correlation between the mean attention and the efficacy rate of current therapies in these 4 major liver diseases.
INTERPRETATION: There are important disparities between research attention and disease burden among the major liver diseases. While viral hepatitis has received considerable attention, there is a marked inadequate attention to ALD. There is a critical need to increase awareness of ALD in the liver research community. Published by the BMJ Publishing Group Limited. For permission to use (where not already granted under a licence) please go to http://www.bmj.com/company/products-services/rights-and-licensing/.

Entities:  

Keywords:  Hepatitis B virus; Hepatitis C virus; Non-alcoholic fatty liver disease; PUBLIC HEALTH; alcoholic liver disease

Mesh:

Year:  2017        PMID: 28336739      PMCID: PMC5372160          DOI: 10.1136/bmjopen-2016-013620

Source DB:  PubMed          Journal:  BMJ Open        ISSN: 2044-6055            Impact factor:   2.692


This is the first comprehensive systematic study assessing the relative attention to the major liver diseases. This study develops a novel tool to estimate the ratio between the research attention and burden of major liver disease (ie, the Attention-to-Burden Index or ABI). We found a strong correlation between the efficacy of current pharmacological therapies and the degree of research attention devoted to each major liver disease, which strongly suggests the need to reallocate more research resources to alcoholic liver disease. The global burden of the major liver disease is largely unknown and we used an array of different variables. The efficacy of pharmacological therapies for viral hepatitis can be easily calculated based on viral parameters, while the parameters to evaluate the resolution of fatty liver diseases are not well established.

Introduction

Liver diseases are a major cause of morbidity and mortality.1 The main causes include chronic viral hepatitis B (HBV) and C (HCV), as well as alcoholic and non-alcoholic fatty liver diseases (ALD and NAFLD, respectively). The role of these causes on the burden of liver disease depends on disease severity and on geographical factors. In global north countries such as France, fatty liver diseases (NAFLD, ALD or its combination) account for most cases of liver fibrosis while HBV is highly prevalent in Asian countries.2 3 Regarding advanced liver disease, ALD is the main cause of cirrhosis worldwide, accounting for 50% of the cases.4 In Europe and the USA, stark increases in morbidity due to alcohol-associated liver disease have been observed in the past 15 years.5 6 Importantly, the role of NAFLD as a cause of advanced liver disease and hepatocellular carcinoma has markedly increased in many countries due to the epidemics of diabetes and obesity.7 Major advances have been made in the management of viral hepatitis, such as vaccines and oral therapies for HBV, and oral regimes for HCV.8 9 In the past decade, there has been an increased focus on NAFLD, with studies identifying targeted therapies and subsequent clinical trials.10 11 In comparison to the advances, ALD has been afforded scant attention, with few advances in its management.12 Patients with ALD are mostly identified at late stages of the disease, and programmes for early detection are scarce. Moreover, the genetic and environmental factors are largely unknown. We hypothesised that differences in advancement between viral hepatitis and fatty liver diseases, in particular ALD, are related to varying allocations of research resources. There are no systematic studies assessing the relative research on different aetiologies of liver disease, or how commensurate research attention is with disease burden. The current study was undertaken to fill this gap.

Methods

General design

For this systematic analysis, data on the research attention were obtained at multiple levels for the four main liver disease aetiologies, carried out during the years 2010–2014, and analysed during 2015. The aetiologies categorised were HCV, HBV, NAFLD and ALD, while data on less prevalent liver diseases were considered but not included in the final analysis. A quantitative scoring system was used to define and subsequently measure research attention to liver disease aetiology. When a single cause of liver disease was identified in a presentation, grant, clinical trial or scientific publication, full points (1.0 point) were allocated to the disease. When two causes of liver disease were identified, points were equally shared (0.5 point each). When the focus of a study could be attributed to more than two causes of liver disease or the study investigated a common mechanism (eg, hepatocellular apoptosis) and/or consequence of liver diseases (eg, ascites), the finding was excluded. Basic science studies that investigated common mechanisms of liver disease were also excluded.

Quantification of research attention

The relative level of attention to each liver disease was calculated at five different levels: primary research presented at major scientific liver meetings, drugs in development, research opportunities, clinical trials and publications. The mean research attention was calculated by averaging the relative level of attention devoted to each liver disease in each of the five categories.

Major scientific liver meetings

The scoring system for the two major global liver scientific meetings (American Association Study of Liver Diseases (AASLD) and European Association for the Study of the Liver (EASL)) was designed to reflect the quantity of presentations as well as the level of presentation. The scores were allocated as follows: 5 points, title of a large symposium (eg, postgraduate course); 4 points, title of small courses or joint workshops; 3 points, scientific presentations at an oral general meeting or plenary session, presidential lectures or state-of-the-art lectures and titles of parallel session; 2 points, scientific presentations at a parallel session, early morning workshops, meet-the-professor luncheon or grand rounds and titles from sections of the poster presentations; and 1 point, scientific presentation as a poster. The number of abstracts in each category was multiplied by the allocated score to provide an overall weighted research attention. Only clinical and translational studies including human samples were included. Scores for attention are reported as a percentage or total N.

Drugs in development

A systematic online search of the 38 major pharmaceutical companies was made to determine the amount of pharmacological therapies in development for the four major liver diseases. Drugs in development that were specifically indicated for one of the four liver diseases were included in the analysis.

Research opportunities

The National Institutes of Health (NIH) Research Portfolio Reporting Tools (RePORTER) was accessed to identify public funding opportunities in the USA. The following Boolean searches were performed using these terms: ‘alcoholic liver disease’ excluding ‘non-alcoholic fatty liver disease’, ‘hepatitis C virus’, ‘hepatitis B virus’, ‘nonalcoholic fatty liver disease’ excluding ‘alcoholic liver disease’. To identify public grant opportunities for the European Union (EU), the Community Research and Development Information Service (CORDIS) advanced search database was used, and the ‘Only Projects’ tab was selected and the same search items were entered. The number of corresponding grants was recorded by disease category.

Clinical trials and scientific publications

The same search terms used for the research opportunities section were entered into Clinicaltrials.gov and PubMed to identify ongoing clinical trials and publications, respectively. Observational and interventional ongoing studies for the four major liver diseases were identified. Trials and/or publications on unspecific liver diseases (ie, cirrhosis) were excluded.

Estimation of disease burden

We estimated the burden of each of the four main liver diseases by combining parameters indicative of early and advanced liver disease as well as hospitalisation costs. The following parameters were used to estimate the relative burden of each of the major four liver diseases: (1) liver-related mortality in the USA;13 (2) causes of liver fibrosis estimated by non-invasive tests;14 (3) causes of liver cirrhosis;15 (4) cause of liver transplantation in the USA and the EU. The causes of liver transplantation in Europe were identified from the European Liver Transplantation Registry. To account for patients with concurrent aetiologies (eg, HCV/ALD), we divided the number of patients with HCV/ALD and assigned half of them to HCV and half of them to ALD.16 17 (5) Inpatient hospitalisation costs of patients with liver disease in the USA.18 (6) Hospital admissions and discharges: the data were obtained from the total number of patient discharges for each of the four main liver diseases.18

Estimation of rate of efficacy of current pharmacological therapies

We conducted a systematic review of the main controlled clinical trials testing targeted therapies for viral hepatitis and fatty liver diseases. Studies published during the period 2010–2014 in the most cited journals were included and reviewed. For HBV, the cure rate was determined by DNA clearance or persistent reduction of Hepatitis B Surface Antigen (HBsAg). For HCV, we considered the sustained viral response (SVR) at 12 weeks to help determine drug efficacies. In patients with biopsy-proven non-alcoholic steatohepatitis (NASH), we defined drug efficacy as histological improvement of patients in the NAFLD Activity Score (NAS) score and/or fibrosis. Regarding ALD, in the absence of consistent studies in patients with early disease, rates of efficacy were based on 28-day survival in patients with alcoholic hepatitis (AH).

Development of the Attention-to-Burden Index

The Attention-to-Burden Index (ABI) was developed to compare the research activities during 2010–2014, and an estimate of disease burden of the four major liver diseases. The ABI for each liver disease was calculated as the mean research attention divided by the mean disease burden for each liver disease. A resulting ratio close to 1 reflects an appropriate attention compared with the burden. In contrast, ABI reflects either overattention (positive value) or inadequate attention (negative value) compared with the burden.

Statistical analysis

Descriptive data are reported for liver meeting attention, drug development attention, published article attention, clinical trial attention, research grant attention and burden of disease as either N or per cent where appropriate. Ratios were created comparing the proportion of disease attention and proportion of disease burden. SPSS software (Chapel Hill, North Carolina, USA) was used to determine the Pearson's correlation between drug efficacy and research attention to the four main liver diseases. An analysis of variance test was also carried out to determine the level of significance of the correlation between research attention and pharmaceutical drug efficacy.

Results

Analysis of research attention to major liver diseases (2010–2014)

We first performed a systematic analysis of the research attention paid to the four main liver diseases during the period 2010–2014 at five different levels. EASL meetings had a research attention of 55% and 25% for HCV and HBV, respectively, while NAFLD and ALD received 13% and 7%, respectively. AASLD meetings provided similar research focus to HCV and HBV (attentions of 49% and 32%, respectively) while NAFLD and ALD received 14% and 4% (figure 1A, table 1 and online supplementary table S1).
Figure 1

Parameters of research attention to the four major liver diseases. The relative level of attention devoted to each liver disease from different parameters: (A) detailed analysis of all presentations at the two major annual scientific liver meetings (AASLD and EASL); (B) research opportunities offered by public agencies in the USA and in the EU; (C) ongoing registered clinical trials (ClinicalTrials.gov); (D) scientific publications (PubMed). AASLD, American Association Study of Liver Diseases; AH, alcoholic hepatitis; ALD, alcoholic liver disease; EASL, European Association for the Study of the Liver; EU, European Union; HBV, hepatitis B virus; HCV, hepatitis C virus; NAFLD, non-alcoholic fatty liver disease; NASH, non-alcoholic steatohepatitis; NIH, National Institutes of Health.

Table 1

Weighted research attention to main liver diseases in the two most attended international liver conferences, 2010–2014

Weighted values2010–2014HCV
HBV
NAFLD
ALD
International Liver ConferenceEASLAASLDEASLAASLDEASLAASLDEASLAASLD
Symposia*277.547.592.549.535102515
Titles of sessions†144278100164501104244
Oral—general presentations‡7843.52113.527633
Oral—parallel presentations§3354263913201116
Poster presentation¶945.51708423.51135231475.598.5135
Total weighted points147821316631401356621.5179.5213

*Incidence multiplied by 5 research points. It includes courses, joint workshops and industry-supported satellite symposia.

†Incidence multiplied by 4 research points. It includes titles of entire oral parallel session and poster categories.

‡Incidence multiplied by 3 research points. It includes plenary sessions, presidential lectures, state-of-the-art lectures and European Liver Patients Association (ELPA) workshops.

§Incidence multiplied by 2 research points. It includes early morning workshops, meet-the-professor luncheons and grand rounds.

¶Incidence multiplied by 1 research point.

AASLD, American Association for the Study of the Liver; ALD, alcoholic liver disease; EASL, European Association for the Study of Liver Diseases; HBV, hepatitis B virus; HCV, hepatitis C virus; NAFLD, non-alcoholic fatty liver disease.

Weighted research attention to main liver diseases in the two most attended international liver conferences, 2010–2014 *Incidence multiplied by 5 research points. It includes courses, joint workshops and industry-supported satellite symposia. †Incidence multiplied by 4 research points. It includes titles of entire oral parallel session and poster categories. ‡Incidence multiplied by 3 research points. It includes plenary sessions, presidential lectures, state-of-the-art lectures and European Liver Patients Association (ELPA) workshops. §Incidence multiplied by 2 research points. It includes early morning workshops, meet-the-professor luncheons and grand rounds. ¶Incidence multiplied by 1 research point. AASLD, American Association for the Study of the Liver; ALD, alcoholic liver disease; EASL, European Association for the Study of Liver Diseases; HBV, hepatitis B virus; HCV, hepatitis C virus; NAFLD, non-alcoholic fatty liver disease. Parameters of research attention to the four major liver diseases. The relative level of attention devoted to each liver disease from different parameters: (A) detailed analysis of all presentations at the two major annual scientific liver meetings (AASLD and EASL); (B) research opportunities offered by public agencies in the USA and in the EU; (C) ongoing registered clinical trials (ClinicalTrials.gov); (D) scientific publications (PubMed). AASLD, American Association Study of Liver Diseases; AH, alcoholic hepatitis; ALD, alcoholic liver disease; EASL, European Association for the Study of the Liver; EU, European Union; HBV, hepatitis B virus; HCV, hepatitis C virus; NAFLD, non-alcoholic fatty liver disease; NASH, non-alcoholic steatohepatitis; NIH, National Institutes of Health. In the analysis of drugs in the pipeline from the main 38 drug companies, we found 74 drugs specifically indicated to treat these four major liver diseases. Eighty-two per cent of such drugs were for HCV, mainly oral-acting interferon-free regimes. A smaller proportion of drugs were devoted to HBV (12%), while only 6% of the drugs in development were focused on treating either NAFLD (3%) or ALD (3%; see online supplementary table S2). Next, research opportunities were assessed in public agencies in the USA and the EU (see online supplementary table S3). In the USA and the EU, it was found that the majority of funding opportunities were devoted to HCV (48% and 61%, respectively), followed by HBV (21% and 30%; figure 1B). In contrast, NAFLD received less attention (20% in the USA and 7% in the EU) while ALD received minimal funding opportunities (3% in the USA and 0% in the EU). Next, registered clinical trials were analysed to determine the proportion of focus devoted to the four main liver diseases. A total of 1273 clinical trials were found, and most studies were devoted to test anti-HCV and HBV drugs (32% and 36%, respectively; figure 1C). The proportion of ongoing trials for NAFLD was 5%, while 18% of ongoing trials were specifically devoted to ALD (table 2). These differences were similar when the clinical trials were divided between interventional and observational trials (data not shown). Finally, the relative number of scientific publications devoted to different types of liver diseases was analysed for the period 2010–2014. A total of 39 093 publications were found on the four main liver diseases included in our study. Published studies for HCV and HBV accounted for 46% and 32%, respectively (figure 1D). The publications for NAFLD were lower at 17%, and for ALD, even more so at 5%. Overall, the mean research attention afforded to the four main liver diseases was greater for HCV and HBV at 47% and 31%, respectively, than it was for NAFLD and ALD at 17% and 5%, respectively (figure 2).
Table 2

Research attention from clinical trials, public agencies and PubMed

HCV (n, %)HBVNAFLDALD
Drugs in development61 (82)9 (12)2 (3)2 (3)
EASL1478 (55)663 (25)356 (13)179.5 (7)
AASLD2131 (49)1401 (32)621.5 (14)135 (5)
PubMed15 438 (39)10 724 (27)5518 (14)1728 (4)
NIH grants738 (48)328 (21)300 (20)47 (3)
EU grants52.5 (61)25.5 (30)6 (7)0 (0)
Clinical trials407 (32)461 (36)66 (5)235 (18)
Mean research attention47%31%17%5%

Percentages in parentheses calculated from a combination of HCV, HBV, NAFLD and ALD.

AASLD, American Association for the Study of the Liver; ALD, alcoholic liver disease; EASL, European Association for the Study of Liver Diseases; EU, European Union; HBV, hepatitis B virus; HCV, hepatitis C virus; NAFLD, non-alcoholic fatty liver disease; NIH, National Institutes of Health.

Figure 2

Calculation of mean research attention to the four major liver diseases. The mean research attention to the four main liver diseases (HBV, HCV, NAFLD and ALD) was calculated from five parameters: scientific publications (PubMed); research opportunities offered by public agencies in the USA and the EU; ongoing registered clinical trials (ClinicalTrials.gov); detailed analysis of all presentations at the two major annual scientific liver meetings (AASLD and EASL); and number of drugs in development in the pipeline of 38 major pharmaceutical companies. AASLD, American Association Study of Liver Diseases; ALD, alcoholic liver disease; EASL, European Association for the Study of the Liver; EU, European Union; HBV, hepatitis B virus; HCV, hepatitis C virus; NAFLD, non-alcoholic fatty liver disease.

Research attention from clinical trials, public agencies and PubMed Percentages in parentheses calculated from a combination of HCV, HBV, NAFLD and ALD. AASLD, American Association for the Study of the Liver; ALD, alcoholic liver disease; EASL, European Association for the Study of Liver Diseases; EU, European Union; HBV, hepatitis B virus; HCV, hepatitis C virus; NAFLD, non-alcoholic fatty liver disease; NIH, National Institutes of Health. Calculation of mean research attention to the four major liver diseases. The mean research attention to the four main liver diseases (HBV, HCV, NAFLD and ALD) was calculated from five parameters: scientific publications (PubMed); research opportunities offered by public agencies in the USA and the EU; ongoing registered clinical trials (ClinicalTrials.gov); detailed analysis of all presentations at the two major annual scientific liver meetings (AASLD and EASL); and number of drugs in development in the pipeline of 38 major pharmaceutical companies. AASLD, American Association Study of Liver Diseases; ALD, alcoholic liver disease; EASL, European Association for the Study of the Liver; EU, European Union; HBV, hepatitis B virus; HCV, hepatitis C virus; NAFLD, non-alcoholic fatty liver disease.

Estimation of disease burden for the major liver diseases

In the absence of systematic studies assessing the burden of the major liver disease worldwide, we next estimated the overall burden of the four major liver diseases by combining data from six different parameters (see methods). The relative numbers of mortality caused by liver disease in the USA can be attributed to 23% HCV, 0.54% to HBV, 3% to NAFLD and 50% to ALD.13 The indications of liver fibrosis in the USA were 10% to HCV, 7% to HBV, 48% to NAFLD and 35% to ALD.14 The causes of liver cirrhosis in the USA were 47% to HCV, 3% to HBV, 27% to NAFLD and 25% to ALD.15 The main indications of liver transplantation in the EU and the USA were attributed as 28% and 40% to HCV, 11% HBV (EU), in the USA there were no data on HBV due to its low indication rate for transplantation, 10% and 16% to NAFLD, and 39% and 23% to ALD.16 17 HCV and HBV contributed to $167 785 million (15%) and $52 062 (5%) of hospitalisation costs, while NAFLD and ALD contributed to $45 755 (4%) and $848 189 (76%), respectively, in the USA.18 The relative number of hospital admissions and discharges were obtained from Peery et al's18 calculation of the burden of gastrointestinal disease in the USA in 2012, and were attributed to the four aetiologies of liver disease: at 14 749 (17%) and 4568 (5%) to HCV and HBV, and at 2858 (3%) and 64 752 (74%) to NAFLD and ALD (see online supplementary table S4). Taking into account all these parameters, the mean disease burden was calculated at 28% and 5% for HCV and HBV, respectively, and 17% and 50% for NAFLD and ALD (figure 3).
Figure 3

Estimation of mean disease burden to four main liver diseases. The mean disease burden to the four main liver diseases (HBV, HCV, NAFLD and ALD) was calculated from seven parameters: total number of US hospitals discharged, US hospitalisation costs, OLTY-EU, OLTY-US, cirrhosis-US, fibrosis and US mortality. ALD, alcoholic liver disease; HBV, hepatitis B virus; HCV, hepatitis C virus; NAFLD, non-alcoholic fatty liver disease.

Estimation of mean disease burden to four main liver diseases. The mean disease burden to the four main liver diseases (HBV, HCV, NAFLD and ALD) was calculated from seven parameters: total number of US hospitals discharged, US hospitalisation costs, OLTY-EU, OLTY-US, cirrhosis-US, fibrosis and US mortality. ALD, alcoholic liver disease; HBV, hepatitis B virus; HCV, hepatitis C virus; NAFLD, non-alcoholic fatty liver disease.

Relative research attention compared with disease burden (ABI)

In order to critically analyse if there are disparities between the attention that the liver research community pays to the major liver disease and their burden, we generated ABI (if the relative attention equals the relative burden of a given liver disease, the ratio should be 1). The calculated ABI for hepatitis B and C revealed a +6.7-fold and +1.7-fold overattention, respectively. NAFLD received an ABI of −1.2-fold, reflecting its recent rise in attention within the field of hepatology, while ALD received a marked inadequate attention of −9.7-fold (figure 4 and table 3). The ABI indicates that while viral hepatitis has been extensively studied during the past years, ALD is being markedly overlooked.
Figure 4

ABI for the four major liver diseases. ABI was calculated using the ratio of mean research attention (comprising different parameters shown in figure 1) to mean disease burden (comprising the parameters shown in figure 2) of the four main liver diseases. A value >1 reflects overattention compared with the disease burden, while a value <1 reflects inadequate attention. ABI, Attention-to-Burden Index ALD, alcoholic liver disease; HBV, hepatitis B virus; HCV, hepatitis C virus; NAFLD, non-alcoholic fatty liver disease.

Table 3

Attention to Burden Index

HBVHCVNAFLDALD
Mean research attention29%51%15%5%
Mean disease burden5%28%17%50%
Ratio6.711.670.930.10
Fold-over ratio6.711.67−1.08−9.68
Attention-to-Burden Score6.711.7−1.1−9.7

The Attention-to-Burden score is bolded to highlight it. It is the final score that was calculated that informed the Attention Burden Index. ALD, alcoholic liver disease; HBV, hepatitis B virus; HCV, hepatitis C virus; NAFLD, non-alcoholic fatty liver disease.

Attention to Burden Index The Attention-to-Burden score is bolded to highlight it. It is the final score that was calculated that informed the Attention Burden Index. ALD, alcoholic liver disease; HBV, hepatitis B virus; HCV, hepatitis C virus; NAFLD, non-alcoholic fatty liver disease. ABI for the four major liver diseases. ABI was calculated using the ratio of mean research attention (comprising different parameters shown in figure 1) to mean disease burden (comprising the parameters shown in figure 2) of the four main liver diseases. A value >1 reflects overattention compared with the disease burden, while a value <1 reflects inadequate attention. ABI, Attention-to-Burden Index ALD, alcoholic liver disease; HBV, hepatitis B virus; HCV, hepatitis C virus; NAFLD, non-alcoholic fatty liver disease.

Efficacy rate of current therapies: correlation with the degree of research attention

Finally, we hypothesised that there is a relationship between the degree of research attention to each major liver disease and the therapeutic advances. In order to address this question, we conducted a systematic review of the main controlled clinical trials testing targeted therapies for viral hepatitis and fatty liver diseases. For HBV and HCV, we determined the efficacy in terms of sustained viral response. In patients with biopsy-proven NASH, we defined drug efficacy as histological improvement of patients in the NAS and/or fibrosis. Regarding ALD, there are no consistent clinical trials to test targeted therapies in patients with early/compensated forms. Therefore, we focus on the efficacy of drugs in improving short-term survival in patients with AH. Following these criteria, the efficacy rate of current pharmacological agents was 72% for HBV, 89% for HCV, 25% for NASH and 13% for AH (figure 5A and see online supplementary table S5). Importantly, there was a positive relationship between the mean attention to each major liver disease and the success rate of pharmacological therapies (figure 5B). This figure strongly suggests that the greater the concentration of research on one liver disease, the more likely to develop efficacious drugs.18–46
Figure 5

Correlation between the efficacy of current drug therapies for hepatitis and the mean research attention. (A) Current mean rate of efficacy for therapeutic drugs; (B) correlation between the efficacy of current drug therapies for hepatitis and the mean research attention. The efficacy of current drug therapies to treat chronic hepatitis (HCV), chronic hepatitis B (HBV), NASH and AH was calculated based on large published clinical trials (see Methods section). Definition criteria of drug efficacy for each of the four type of hepatitis were: HCV: sustained viral response at 12 weeks; HBV: achievement of end points suppressing viral replication; NASH: reduction in NAS or fibrosis score; AH: effect on short-term mortality rate. AH, alcoholic hepatitis; HBV, hepatitis B virus; HCV, hepatitis C virus; NAS, NAFLD Activity Score; NASH, non-alcoholic steatohepatitis.

Correlation between the efficacy of current drug therapies for hepatitis and the mean research attention. (A) Current mean rate of efficacy for therapeutic drugs; (B) correlation between the efficacy of current drug therapies for hepatitis and the mean research attention. The efficacy of current drug therapies to treat chronic hepatitis (HCV), chronic hepatitis B (HBV), NASH and AH was calculated based on large published clinical trials (see Methods section). Definition criteria of drug efficacy for each of the four type of hepatitis were: HCV: sustained viral response at 12 weeks; HBV: achievement of end points suppressing viral replication; NASH: reduction in NAS or fibrosis score; AH: effect on short-term mortality rate. AH, alcoholic hepatitis; HBV, hepatitis B virus; HCV, hepatitis C virus; NAS, NAFLD Activity Score; NASH, non-alcoholic steatohepatitis.

Discussion

In the past decade, major advances have been achieved in the field of viral hepatitis, with the development of highly active oral antiviral therapies. In clear contrast, there are no approved therapies for NAFLD and ALD and interventions for AH are largely unchanged over the past 40+ years. We hypothesised that these discrepant advances are related to unequal allocation of research resources. Our systematic study found marked disparities between research attention and disease burden among the aetiologies of liver disease. We compared multiple modalities of hepatology research attention (eg, scientific meeting presentations, research funding, drugs under development, funding opportunities and publications) with measures of liver disease burden (prevalence, fibrosis and healthcare costs). We found a lack of correlation between research attention and disease burden. Overall, viral hepatitis received a 5–7-fold overattention, while alcoholic liver disease received a 10-fold underattention. There are a few similar studies in other fields of medicine that have investigated research attention and disease burden.47 Using a similar methodology to ours, these studies used clinicaltrials.gov, while others compared NIH funding to disease burden. Unfortunately, the discrepancy between funding and burden has become a common theme. The finding of attention–burden discordance is most likely multifactorial. HBV and HCV are causes of cirrhosis and hepatocellular carcinoma, and are important public health issues in their own right.1 2 Therapeutic targets for viral hepatitis are better defined than those for fatty liver diseases (eg, proteins regulating viral replication), and there is a significant interest to develop antiviral agents. It is important to recognise that the nature of these diseases also plays an important role in the development of drug therapies. The pathways of viral hepatitis (HBV and HCV) diseases have a significant positive effect on the advancement of effective drug therapies compared with that of fatty liver diseases. HBV and HCV have clear aetiologies, with transmission of the virus occurring in determined pathways which provide scientific researchers with clear targets for the development of pharmacotherapies. In contrast, fatty liver diseases (NAFLD and ALD) have multiple causes and are linked to other health conditions, their complex aetiologies, which necessitate the development of therapies that address multiple targets, and may contribute to the lack of drugs targeted to NAFLD or ALD. It is observed that increases in attention become self-perpetuating, with scientific advances (ie, drug development efforts, research allotment, etc) influencing greater research attention (more presentations, drugs, funding opportunities and publications) and vice versa. The inadequate attention especially to ALD is complex and includes the social stigma surrounding alcoholism, poorly defined targets for therapy, a lack of good animal models, few non-invasive markers of severity and poor general awareness of the diseases. Additionally, there is a lack of large-scale early detection efforts, and thus patients are often identified at very late stages of the disease. These challenges alongside patient identification, research and therapy result in a high burden of disease. Our findings should be viewed as a comparative assessment of relative attention and burden among the major liver diseases. While we completed an extensive search, which expanded over a 5-year period and involved multiple areas within both the public and private sectors, our estimates were derived from pre-existing databases with their own respective inclusion and exclusion criteria. Thus, limitations of this study include the possibility of incomplete estimates. Other limitations include the inability to complete a systematic review of the global burden of the major liver diseases due to the limited number of articles that focus on fatty liver disease burdens. The limited and heterogeneous resources used for burden estimates reflect the need for further research. Consequences of this large discrepancy among hepatitis and fatty liver diseases include extraordinary advances in the therapy of HCV and HBV prevention, while little advancements in early detection and treatment of ALD and NAFLD have been made. It is unknown if these differences impact mortality. The next decade could benefit from greater research attention being allocated to NAFLD and ALD. Translational studies identifying targets for therapy for fatty liver disease will certainly encourage pharmaceutical companies to invest in clinical trials. Ultimately, efforts by public funding agencies and the scientific community to address the diseases with the greatest public health burden will result in improved health outcomes for the greatest number of people. A striking finding of our study is the minimal attention that both public and private sources pay to ALD, which is the main cause of cirrhosis globally.4 In recent years, a concurrent increase in addiction behaviour and the prevalence of resulting illnesses such as ALD has been observed in the USA and Europe.5 6 Accompanying the sharp rise in ALD cases is the increasing burden of patients with liver disease on national health systems, identifying them as the main group expenditures in patient hospitalisation costs.18 In spite of its significant health and socioeconomic burden, few major advances have been made in the management of patients with ALD. The pharmacological therapies used today have not changed since 1971 (ie, prednisolone for AH), and no widespread early detection programmes have been developed.48 Our study should increase awareness in the public health agencies and academic institutions, especially in Europe, to devote more resources to face this prevalent and devastating liver disease. The development of a European Agency for Alcohol Studies, similar to the National Institute for Alcohol and Alcoholism (NIAAA) in the USA, seems a timely initiative.
  47 in total

1.  Evolution of indications and results of liver transplantation in Europe. A report from the European Liver Transplant Registry (ELTR).

Authors:  René Adam; Vincent Karam; Valérie Delvart; John O'Grady; Darius Mirza; Jurgen Klempnauer; Denis Castaing; Peter Neuhaus; Neville Jamieson; Mauro Salizzoni; Stephen Pollard; Jan Lerut; Andreas Paul; Juan Carlos Garcia-Valdecasas; Fernando San Juan Rodríguez; Andrew Burroughs
Journal:  J Hepatol       Date:  2012-05-16       Impact factor: 25.083

Review 2.  Hepatitis B virus infection.

Authors:  Christian Trépo; Henry L Y Chan; Anna Lok
Journal:  Lancet       Date:  2014-06-18       Impact factor: 79.321

3.  Pentoxifylline improves nonalcoholic steatohepatitis: a randomized placebo-controlled trial.

Authors:  Claudia O Zein; Lisa M Yerian; Prema Gogate; Rocio Lopez; John P Kirwan; Ariel E Feldstein; Arthur J McCullough
Journal:  Hepatology       Date:  2011-08-24       Impact factor: 17.425

4.  Pentoxifylline improves short-term survival in severe acute alcoholic hepatitis: a double-blind, placebo-controlled trial.

Authors:  E Akriviadis; R Botla; W Briggs; S Han; T Reynolds; O Shakil
Journal:  Gastroenterology       Date:  2000-12       Impact factor: 22.682

5.  Nonalcoholic steatohepatitis is the second leading etiology of liver disease among adults awaiting liver transplantation in the United States.

Authors:  Robert J Wong; Maria Aguilar; Ramsey Cheung; Ryan B Perumpail; Stephen A Harrison; Zobair M Younossi; Aijaz Ahmed
Journal:  Gastroenterology       Date:  2014-11-25       Impact factor: 22.682

6.  Simeprevir plus sofosbuvir, with or without ribavirin, to treat chronic infection with hepatitis C virus genotype 1 in non-responders to pegylated interferon and ribavirin and treatment-naive patients: the COSMOS randomised study.

Authors:  Eric Lawitz; Mark S Sulkowski; Reem Ghalib; Maribel Rodriguez-Torres; Zobair M Younossi; Ana Corregidor; Edwin DeJesus; Brian Pearlman; Mordechai Rabinovitz; Norman Gitlin; Joseph K Lim; Paul J Pockros; John D Scott; Bart Fevery; Tom Lambrecht; Sivi Ouwerkerk-Mahadevan; Katleen Callewaert; William T Symonds; Gaston Picchio; Karen L Lindsay; Maria Beumont; Ira M Jacobson
Journal:  Lancet       Date:  2014-07-28       Impact factor: 79.321

7.  Prednisolone or pentoxifylline for alcoholic hepatitis.

Authors:  Mark R Thursz; Paul Richardson; Michael Allison; Andrew Austin; Megan Bowers; Christopher P Day; Nichola Downs; Dermot Gleeson; Alastair MacGilchrist; Allister Grant; Steven Hood; Steven Masson; Anne McCune; Jane Mellor; John O'Grady; David Patch; Ian Ratcliffe; Paul Roderick; Louise Stanton; Nikhil Vergis; Mark Wright; Stephen Ryder; Ewan H Forrest
Journal:  N Engl J Med       Date:  2015-04-23       Impact factor: 91.245

Review 8.  Hepatitis C virus treatment in the real world: optimising treatment and access to therapies.

Authors:  Fabien Zoulim; T Jake Liang; Alexander L Gerbes; Alessio Aghemo; Sylvie Deuffic-Burban; Geoffrey Dusheiko; Michael W Fried; Stanislas Pol; Jürgen Kurt Rockstroh; Norah A Terrault; Stefan Wiktor
Journal:  Gut       Date:  2015-11       Impact factor: 23.059

9.  Phase 2b trial of interferon-free therapy for hepatitis C virus genotype 1.

Authors:  Kris V Kowdley; Eric Lawitz; Fred Poordad; Daniel E Cohen; David R Nelson; Stefan Zeuzem; Gregory T Everson; Paul Kwo; Graham R Foster; Mark S Sulkowski; Wangang Xie; Tami Pilot-Matias; George Liossis; Lois Larsen; Amit Khatri; Thomas Podsadecki; Barry Bernstein
Journal:  N Engl J Med       Date:  2014-01-16       Impact factor: 91.245

10.  Liver cirrhosis mortality in 187 countries between 1980 and 2010: a systematic analysis.

Authors:  Ali A Mokdad; Alan D Lopez; Saied Shahraz; Rafael Lozano; Ali H Mokdad; Jeff Stanaway; Christopher J L Murray; Mohsen Naghavi
Journal:  BMC Med       Date:  2014-09-18       Impact factor: 8.775
View more
  11 in total

1.  Charges for Alcoholic Cirrhosis Exceed All Other Etiologies of Cirrhosis Combined: A National and State Inpatient Survey Analysis.

Authors:  A Sidney Barritt; Yue Jiang; Monica Schmidt; Paul H Hayashi; Ramon Bataller
Journal:  Dig Dis Sci       Date:  2019-01-23       Impact factor: 3.199

2.  Colder Weather and Fewer Sunlight Hours Increase Alcohol Consumption and Alcoholic Cirrhosis Worldwide.

Authors:  Meritxell Ventura-Cots; Ariel E Watts; Monica Cruz-Lemini; Neil D Shah; Nambi Ndugga; Peter McCann; A S Barritt; Anant Jain; Samhita Ravi; Carlos Fernandez-Carrillo; Juan G Abraldes; Jose Altamirano; Ramon Bataller
Journal:  Hepatology       Date:  2019-02-27       Impact factor: 17.425

3.  Alcohol-Related Liver Disease Is Rarely Detected at Early Stages Compared With Liver Diseases of Other Etiologies Worldwide.

Authors:  Neil D Shah; Meritxell Ventura-Cots; Juan G Abraldes; Mohamed Alboraie; Ahmad Alfadhli; Josepmaria Argemi; Ester Badia-Aranda; Enrique Arús-Soler; A Sidney Barritt; Fernando Bessone; Marina Biryukova; Flair J Carrilho; Marlen Castellanos Fernández; Zaily Dorta Guiridi; Mohamed El Kassas; Teo Eng-Kiong; Alberto Queiroz Farias; Jacob George; Wenfang Gui; Prem H Thurairajah; John Chen Hsiang; Azra Husić-Selimovic; Vasily Isakov; Mercy Karoney; Won Kim; Johannes Kluwe; Rakesh Kochhar; Narendra Dhaka; Pedro Marques Costa; Mariana A Nabeshima Pharm; Suzane K Ono; Daniela Reis; Agustina Rodil; Caridad Ruenes Domech; Federico Sáez-Royuela; Christoph Scheurich; Way Siow; Nadja Sivac-Burina; Edna Solange Dos Santos Traquino; Fatma Some; Sanjin Spreckic; Shiyun Tan; Julio Vorobioff; Andrew Wandera; Pengbo Wu; Mohamed Yacoub; Ling Yang; Yuanjie Yu; Nerma Zahiragic; Chaoqun Zhang; Helena Cortez-Pinto; Ramon Bataller
Journal:  Clin Gastroenterol Hepatol       Date:  2019-01-29       Impact factor: 11.382

4.  ACG Clinical Guideline: Alcoholic Liver Disease.

Authors:  Ashwani K Singal; Ramon Bataller; Joseph Ahn; Patrick S Kamath; Vijay H Shah
Journal:  Am J Gastroenterol       Date:  2018-01-16       Impact factor: 10.864

Review 5.  The Role of Myeloid-Derived Cells in the Progression of Liver Disease.

Authors:  Chris John Weston; Henning Wolfgang Zimmermann; David H Adams
Journal:  Front Immunol       Date:  2019-04-24       Impact factor: 7.561

6.  Propranolol Is Associated with Lower Risk of Incidence of Hepatocellular Carcinoma in Patients with Alcoholic Cirrhosis: A Tertiary-Center Study and Indirect Comparison with Meta-Analysis.

Authors:  Tzu-Hao Li; Yu-Lien Tsai; Chien-Fu Hsu; Chih-Wei Liu; Chia-Chang Huang; Ying-Ying Yang; Hung-Cheng Tsai; Shiang-Fen Huang; Yun-Cheng Hsieh; Hsuan-Miao Liu; Tzung-Yan Lee; Ming-Chih Hou; Chang-Youh Tsai; Han-Chieh Lin
Journal:  Gastroenterol Res Pract       Date:  2020-04-09       Impact factor: 2.260

Review 7.  Public health policies and alcohol-related liver disease.

Authors:  Meritxell Ventura-Cots; Maria Pilar Ballester-Ferré; Samhita Ravi; Ramon Bataller
Journal:  JHEP Rep       Date:  2019-08-08

8.  Gender-related disparities in the frequencies of PD-1 and PD-L1 positive peripheral blood T and B lymphocytes in patients with alcohol-related liver disease: a single center pilot study.

Authors:  Beata Kasztelan-Szczerbinska; Katarzyna Adamczyk; Agata Surdacka; Jacek Rolinski; Agata Michalak; Agnieszka Bojarska-Junak; Mariusz Szczerbinski; Halina Cichoz-Lach
Journal:  PeerJ       Date:  2021-01-20       Impact factor: 2.984

9.  Bile acid-receptor TGR5 deficiency worsens liver injury in alcohol-fed mice by inducing intestinal microbiota dysbiosis.

Authors:  Madeleine Spatz; Dragos Ciocan; Gregory Merlen; Dominique Rainteau; Lydie Humbert; Neuza Gomes-Rochette; Cindy Hugot; Nicolas Trainel; Françoise Mercier-Nomé; Séverine Domenichini; Virginie Puchois; Laura Wrzosek; Gladys Ferrere; Thierry Tordjmann; Gabriel Perlemuter; Anne-Marie Cassard
Journal:  JHEP Rep       Date:  2021-01-19

10.  An Experimental DUAL Model of Advanced Liver Damage.

Authors:  Raquel Benedé-Ubieto; Olga Estévez-Vázquez; Feifei Guo; Chaobo Chen; Youvika Singh; Helder I Nakaya; Manuel Gómez Del Moral; Arantza Lamas-Paz; Laura Morán; Nuria López-Alcántara; Johanna Reissing; Tony Bruns; Matías A Avila; Eva Santamaría; Marina S Mazariegos; Marius Maximilian Woitok; Ute Haas; Kang Zheng; Ignacio Juárez; José Manuel Martín-Villa; Iris Asensio; Javier Vaquero; Maria Isabel Peligros; Josepmaria Argemi; Ramón Bataller; Javier Ampuero; Manuel Romero Gómez; Christian Trautwein; Christian Liedtke; Rafael Bañares; Francisco Javier Cubero; Yulia A Nevzorova
Journal:  Hepatol Commun       Date:  2021-03-11
View more

北京卡尤迪生物科技股份有限公司 © 2022-2023.