Aspirin Use Is Associated with a Reduced Incidence of Hepatocellular Carcinoma: A Systematic Review and Meta-analysis.

Hepatocellular carcinoma (HCC) is the third-leading cause of cancer-related death worldwide, with a growing incidence and poor prognosis. While some recent studies suggest an inverse association between aspirin use and reduced HCC incidence, other data are conflicting. To date, the precise magnitude of risk reduction-and whether there are dose-dependent and duration-dependent associations-remains unclear. To provide an updated and comprehensive assessment of the association between aspirin use and incident HCC risk, we conducted a systematic review and meta-analysis of all observational studies published through September 2020. Using random-effects meta-analysis, we calculated the pooled relative risks (RRs) and 95% confidence intervals (CIs) for the association between aspirin use and incident HCC risk. Where data were available, we evaluated HCC risk according to the defined daily dose of aspirin use. Among 2,389,019 participants, and 20,479 cases of incident HCC, aspirin use was associated with significantly lower HCC risk (adjusted RR, 0.61; 95% CI, 0.51-0.73; P ≤ 0.001; I2 = 90.4%). In subgroup analyses, the magnitude of benefit associated with aspirin was significantly stronger in studies that adjusted for concurrent statin and/or metformin use (RR, 0.45; 95% CI, 0.28-0.64) versus those that did not (P heterogeneity = 0.02), studies that accounted for cirrhosis (RR, 0.49; 95% CI, 0.45-0.52) versus those that did not (P heterogeneity = 0.02), and studies that confirmed HCC through imaging/biopsy (RR, 0.30; 95% CI, 0.15-0.58) compared with billing codes (P heterogeneity < 0.001). In four studies, each defined daily dose was associated with significantly lower HCC risk (RR, 0.98; 95% CI, 0.97-0.98), corresponding to an 8.4% risk reduction per year of aspirin use.
Conclusion: In this comprehensive systematic review and meta-analysis, aspirin use was associated with a significant reduction in HCC risk. These benefits appeared to increase with increasing dose and duration of aspirin use.

body mass index

confidence intervals

defined daily dose

diabetes mellitus

hepatitis B virus

Hepatocellular carcinoma

hepatitis C virus

nonalcoholic fatty liver disease

National Health Insurance Research Database

randomized control trial

relative risk

Despite the decline in overall cancer‐related mortality over the past decade, hepatocellular carcinoma (HCC) incidence and mortality continue to increase in the United States and worldwide.( ) Among those who develop HCC, the prognosis remains grim, with limited treatment options and 5‐year survival of 12%,( , ) underscoring the need for effective primary prevention strategies.

While the benefits of aspirin for the prevention of colorectal cancer are well‐established,( ) a growing body of recent evidence suggests that aspirin may also help to prevent other cancers,( , , , ) including HCC, through diverse potential mechanisms including the inhibition of cyclooxygenase enzymes, or through pleiotropic effects on inflammatory lipids, platelets, and the gut microbiome.( , , ) However, to date, observational studies focused on aspirin use and HCC risk have yielded conflicting results, with some demonstrating an inverse association between aspirin use and HCC risk, and others finding null associations.( , , , ) Furthermore, inconsistencies in study design, and variability in definitions of aspirin exposure, outcomes or comorbidities, have rendered it difficult to compare effect sizes across studies. As a result, prior meta‐analyses on this topic have included only a fraction of published studies,( , , , ) which can result in biased estimates of effect with limited generalizability.

Thus, to provide the most comprehensive and updated estimates for the potential association between aspirin use and incident HCC risk, we performed a systematic review and meta‐analysis of all observational studies, to evaluate aspirin use—including dose and duration of use—in relation to the risk of developing HCC.

Methods

Search Strategy

A medical librarian (L.P.) undertook a systematic literature search of PubMed, Embase, and Web of Science (inception through September 1, 2020), to identify all existing studies that evaluated aspirin use in relation to HCC incidence. The full PubMed search strategy is available in Supporting Table S1. The title and abstract of all identified studies were screened by two independent reviewers (Z.M. and A.A.), and studies that did not address the research question were excluded. All remaining articles were subsequently reviewed in full against the selection criteria. References were also examined to identify additional studies of relevance. Any discrepancies were resolved by consensus between the two reviewers, or with the input of a third reviewer (T.S.).

Eligibility Criteria

The systematic review and meta‐analysis were performed according to the Preferred Reporting Items for Systematic Reviews and Meta‐analyses (PRISMA) guidelines.( ) We included all human clinical studies written in English that evaluated aspirin exposure and incident HCC risk, and that reported effect estimates (i.e., relative risks [RRs], odds ratios [ORs], or hazard ratios [HRs]) for the association between aspirin use and HCC incidence, or provided sufficient data for their calculation. This also included studies focused primarily on alternative medication exposures, but nevertheless included an effect estimate for aspirin use or data for its calculation. After the initial records were screened by title and abstract, we reviewed 62 full‐text articles and excluded 43 papers for the following reasons: (1) incorrect study design (n = 24; preclinical study, review without original research, or letter to editor or commentary); (2) abstract only (n = 12); (3) wrong patient population (n = 3; patients with established liver cancer), or (4) overlapping study populations (n = 4). For the studies with overlapping populations, we chose to include the study with the largest sample size, as outlined in detail in the Supporting Appendix. After these exclusions, 19 studies were included in the meta‐analysis. Supporting Fig. S1 summarizes the study selection process.

Data Abstraction

Two independent reviewers (Z.M. and A.A.) conducted critical appraisal and extracted data according to a prespecified data collection form. Specifically, the following data were extracted from each study: first author, publication year, study period, study design, geographic region, number of aspirin‐exposed subjects, number of unexposed subjects, method of defining aspirin exposure, dose and/or duration of aspirin use (if reported), method of ascertaining HCC, etiology of underlying liver disease (if known), proportion with cirrhosis (if reported), number of incident HCC cases among aspirin user and nonuser groups, concomitant use of nonsteroidal anti‐inflammatory drugs, metformin or statin medications (if reported), other covariates included in multivariable models or propensity‐score matching, HRs/RRs/ORs and 95% confidence intervals (CIs) before and after adjustment for confounders, and the database used to obtain patient information. Among studies reporting dose and/or duration of aspirin use, we extracted data regarding the defined daily dose (DDD) of aspirin; or if the DDD was not reported, then we calculated the DDD based on the dosage and number of filled 30‐day prescriptions or the duration of daily aspirin use.

Statistical Analysis

We used the established random effects model described by DerSimonian and Laird to calculate pooled RR and 95% CIs. ( ) Wherever possible, we used adjusted risk estimates from the included studies to account for confounding variables. Between‐study heterogeneity was calculated using Cochran’s Q test and I2 statistic. All P values were two‐tailed, and P < 0.05 was considered statistically significant for all analyses except for tests of heterogeneity and publication bias. We considered heterogeneity to be statistically significant with P < 0.10 and an I2 statistic >50%. A P value of <0.10 was used as a conservative threshold to test for heterogeneity, given that some sample sizes were relatively small and certain subgroups contained a small number of studies, as recommended by prior publications,( , ) including the Cochrane handbook.( ) To identify potential sources of heterogeneity, we performed subgroup analyses according to strata defined by study design, geographic region, definition of aspirin exposure, minimum required duration of aspirin exposure, HCC ascertainment, cohort versus case‐control studies, studies including patients with viral hepatitis, studies including patients with cirrhosis, and studies that simultaneously accounted for statins and metformin. In additional sensitivity analyses, we evaluated whether study region or study design accounted for the observed heterogeneity of results. Publication bias was assessed using a funnel plot and Egger’s test. Qualitative inspection of funnel plots was completed by evaluating the logarithmic odds ratio versus the standard errors.( ) Finally, using a range of assumed control risks for incident HCC, we calculated the number needed to treat (NNT), to prevent one case of incident HCC from an established algorithm.( ) The hazard difference was assumed to represent a valid approximation of the risk difference, given the rarity of incident HCC diagnoses (i.e., event rates <5% per year).( ) All analyses were performed using STATA software 15.1 (StataCorp 2017, College Station, TX).

Results

Search Results

Among the 12,536 unique studies identified through our search strategy, 19 observational studies met the criteria for inclusion. These included two prospective cohort studies, 12 retrospective cohort studies and five case‐control studies, with a total of 2,389,019 total participants and 20,479 incident cases of HCC. Eight studies were removed after initial search, as they were exact duplicates (identified through multiple search engines), and four studies were excluded from the primary meta‐analysis due to overlapping populations.( , , , ) Supporting Fig. S1 shows the flow diagram adapted from PRISMA( ) for study selection.

Study Characteristics

Table 1 outlines the characteristics of included studies. Among the 2,389,019 subjects, 29% (701,297) were exposed to aspirin. Most studies accounted for sex (15 of 19) and age (14 of 19), while a smaller proportion of studies adjusted for other medications (10 of 19), body mass index (BMI) (4 of 19), alcohol use (6 of 19), smoking status (5 of 19), and other comorbidities (7 of 19), and 11 of 19 studies accounted for cirrhosis (with 4 of 19 adjusting for cirrhosis in multivariable models). Most studies from the United States and Europe included subjects with hepatitis C virus (HCV) infection, nonalcoholic fatty liver disease or unknown causes of underlying liver disease, while most studies conducted in Asia included subjects with hepatitis B virus (HBV) infection. The median Newcastle‐Ottawa scale (NOS) score was 7, and 16 of 19 studies were considered high‐quality (NOS > 7) (Supporting Table S2).

TABLE 1

Baseline Characteristics of Observational Studies Included in the Meta‐analysis

Study (Author, Year)	Region	Study Design	Mean Age	HCC Cases (n) #	Aspirin Group (n)	Total Number	Aspirin Assessment	HCC Assessment ‡	Covariates ||	Accounted for Cirrhosis	Exposure Group Balance
Lee, T, 2020	Taiwan	Retrospective cohort	63.2	436	2,478	7,434	Prospective/prescription	ICD‐9 code 155	1, 2, 5, 11‐13, 17, 23, 28	Y	PS
Shen, 2020	USA	Case control	NR	673	676	1,839	Retrospective/self‐reported	US State Cancer Registry ¶	1, 2, 10, 25, 26, 27	Y	NR
Shin, 2020	Korea	Retrospective cohort	64.6	133	224	949	Prospective/prescription	Imaging or biopsy	1, 2,11, 15, 17	Y	PS
Simon, 2020	Sweden	Retrospective cohort	45	1,612	14,205	50,275	Prospective/prescription	ICD code	2, 3, 5, 6, 8, 12‐14, 29	Y	IPTW
Du, 2019	China	Retrospective cohort	45	41	59	264	Prospective/prescription	AFP and imaging or biopsy	NR	Y	NR
Lee, T, 2019	Korea	Retrospective cohort	58.8	697	2,123	10, 615	Prospective/prescription	ICD‐9 M code 155	1, 2, 3, 5, 12‐14	Y	PS
Tsoi, 2019	Hong Kong	Retrospective cohort	67.5	9,370	204,170	612,509	Prospective/prescription	ICD‐9 M code 155	1, 2, 12	N	IPTW
Hwang, 2018	Korea	Retrospective cohort	50	2,336	64,782	460,755	Prospective/prescription	ICD‐10 code C22.0 §	1, 2, 4, 7‐ 9, 12, 13, 17‐19	Y	PS
Lin, 2018	Taiwan	Retrospective cohort	NR	110	3,576	18,243	Prospective/prescription	ICD‐9 M code 155	1, 2, 12, 13, 21	N	NR
Tseng, 2018	Taiwan	Retrospective cohort	NR	1,750	23,112	43,800	Prospective/prescription	ICD‐9 M code 155	1, 2, 3, 6, 13, 22	Y	NR
Lee, M, 2017	Korea	Retrospective cohort	55.2	63	343	14,392	Prospective/prescription	AFP and imaging or biopsy	1‐3, 5, 11‐12, 15, 16, 17	Y	PS
Lee, T, 2017	Taiwan	Retrospective cohort	52.69	NR	5,602	18,080	Prospective/prescription	ICD‐9 M code 155	1‐3, 12‐13, 17	N	NR
Kim, 2017	Korea	Case control	NR	229	390	1,374	Prospective/prescription	ICD‐10 code C22.0 §	1, 2, 3, 12	Y	NR
Yang, 2016	UK	Case control	67	1,195	1,670	5,835	Prospective/prescription*	Read code	3, 4, 6, 8, 9, 12, 13	Y	NR
Petrick, 2015	USA	Prospective cohort	NR	346	258,179	803,248	Prospective/self‐reported*	ICD‐0‐3 histology codes 8170‐8175	1‐4, 8‐10, 29	N	NR
Sahasrabuddhe, 2012	USA	Prospective cohort	62.8	250	89,585	300,504	Prospective/self‐reported*	ICD‐9 and ICD‐10 code	1‐4, 9, 8‐10	N	NR
Chiu, 2011	Taiwan	Case control	66.1	1,166	162	2,332	Retrospective/prescription*	ICD‐9 M code 155	NR	N	NR
Friis, 2003	Denmark	Retrospective cohort	70	21	29,470	29,470 †	Prospective/prescription	ICD‐7 code	NR	N	NR
Coogan, 2000	USA	Case control	NR	51	491	7,101	Retrospective/self‐reported*	AFP and imaging or biopsy	1, 2, 8, 9, 10, 30‐33	N	NR

Included both aspirin and nonsteroidal anti‐inflammatory drugs.

Aspirin users were compared with the population in North Jutland County, Denmark (total number was not reported).

ICD code did not specify morphology (M) or histology unless otherwise specified.

Authors with C22 codes did not specify topography versus morphology (M) codes.

Variables adjusted for with either multivariable regression analysis, PS, or IPTW: 1, age; 2, sex; 3, diabetes mellitus; 4, BMI; 5, cirrhosis; 6, hepatitis B/C; 7, physical activity; 8, alcohol; 9, smoking; 10, race; 11, MELD; 12, other medications (i.e., statins and/or metformin); 13, comorbidities; 14, nucleoside analogues; 15, CTP score; 16, hep level; 17, lab tests such as cholesterol, plasma glucose, AST/ALT, albumin, PLT; 18, socioeconomic status; 19, Charlson comorbidity index score; 20, diet; 21, urbanization; 22, occupation; 23, HCV diagnosis year; 24, number of years of aspirin use; 25, education; 26, household income; 27, marital status; 28, index date to start of follow‐up; 29, cohort; 30, religion; 31, education; 32, family history of digestive cancer; and 33, interview year.

NJ, NYC, and CT State Cancer Registry.

Due to no specification of HCC case number from Lee T (2017), the HCC case numbers are slightly less than the true total cohort number for each subgroup in Table 2.

Abbreviations: AFP, alpha‐fetoprotein; ALT, alanine aminotransferase; AST, aspartate aminotransferase; CTP, Child‐Turcotte‐Pugh; hep level, hepatitis B or C viral load; IPTW, inverse probability of treatment weighting; M code, morphology code; MELD, Model for End‐Stage Liver Disease; NR, not reported; NYC, New York City; PLT, platelet.

TABLE 2

Subgroup Analysis to Identify Sources of Heterogeneity

Subgroup Analysis	No. of Studies	No. of HCC Cases	Total No. of Subjects	RR (95% CI)	Tests of Heterogeneity		Heterogeneity Between Groups (P)
					I2	P
Region
European/U.S.	7	4,148	1,198,272	0.70 (0.54‐0.90)	82.8%	<0.001	P = 0.43
Asian	12	16,331	1,190,747	0.55 (0.42‐0.71)	92.6%	<0.001
HCC ascertainment
Not confirmed (diagnostic code)	13	19,172	1,561,226	0.74 (0.62‐0.87)	89.2%	<0.001	P < 0.001
Confirmed (imaging/pathology)	6	1,307	827,793	0.30 (0.15‐0.58)	51.0%	<0.001
Minimum required duration of aspirin use
>4 weeks	15	18,488	1,837,235	0.60 (0.49‐0.74)	92.0%	<0.001	P = 0.65
No minimum duration	4	1,991	1,107,458	0.66 (0.47‐0.93)	71.2%	0.015
Aspirin ascertainment
Prospective	16	18,569	2,377,747	0.61 (0.50‐0.74)	91.0%	<0.001	P = 0.77
Retrospective	3	1,890	11,272	0.67 (0.31‐1.46)	89.9%	<0.001
Cohort vs. case control
Cohort study	14	17,165	2,370,538	0.59 (0.49‐0.72)	52.4%	<0.001	P = 0.67
Case control	5	3,314	18,481	0.68 (0.39‐1.18)	89.3%	<0.001
Definition of aspirin exposure
Prescription data	15	19,159	1,276,327	0.63 (0.51‐0.77)	91.8%	<0.001	P = 0.54
Self‐reported data	4	1,320	1,112,692	0.55 (0.38‐0.80)	75.4%	0.007
Accounted for viral hepatitis
Yes	10	9,032	596,583	0.69 (0.58‐0.83)	84.8%	<0.001	P = 0.54
No/unspecified	9	11,447	1,792,436	0.54 (0.39‐0.75)	86.9%	<0.001
Accounted for cirrhosis †
Cirrhosis	11	9,165	597,532	0.49 (0.45‐0.52)	21.2%	<0.001	P = 0.02
No cirrhosis/unspecified	8	11,314	1,791,487	0.68 (0.51‐0.82)	90.8%	0.002
Accounted for hepatoprotective medications *
Yes	10	16,048	1,199,512	0.45 (0.28‐0.64)	50.7%	<0.001	P = 0.02
No	9	4,431	1,189,507	0.71 (0.60‐0.86)	89.3%	<0.001
Exposure group balance
PS or IPTW	7	14,647	1,156,929	0.56 (0.43‐0.72)	94.9%	<0.001	P = 0.29
None	12	5,832	1,232,090	0.67 (0.51‐0.88)	78.6%	<0.001

Statins and/or metformin.

Studies could account for cirrhosis by including cirrhosis as a covariate in the multivariable model, or by including cirrhosis as a matching variable to balance exposure groups, or by including a cirrhosis‐only population for analysis.

Abbreviation: IPTW, inverse probability weighting.

Aspirin Use and HCC Risk

Overall, random‐effects meta‐analysis demonstrated that aspirin users had a 39% lower risk of developing incident HCC, compared with nonusers, after accounting for confounding variables (pooled adjusted RR, 0.61; 95% CI, 0.51‐0.73; P ≤ 0.001), with considerable heterogeneity (Cochran’s Q test P ≤ 0.001; I2 = 90.4%) (Fig. 1). We identified no evidence of publication bias through visual inspection of the funnel plot (Supporting Fig. S2) or through quantitative testing, using Egger’s test (P = 0.78).

FIG. 1

Forest plot of aspirin use and risk of HCC development among 19 observational studies, including 2,389,019 participants and overall relative risks with respective weightings. The pooled results of included studies illustrate a significant relative reduction in risk of HCC in participants who used aspirin (RR, 0.61; 95% CI, 0.51‐0.73).

Subgroup and Sensitivity Analyses

We performed subgroup analyses to evaluate potential sources of heterogeneity (Table 2). Among studies that accounted for concurrent statin and/or metformin use (n = 10), aspirin was associated with a significant, 55% lower risk of incident HCC (RR, 0.45; 95% CI, 0.28‐0.64), with moderate heterogeneity (I2 = 50.7%). In contrast, among studies that did not account for those other hepatoprotective medications (n = 9), the RR for aspirin use was 0.71 (95% CI, 0.60‐0.86), with substantial heterogeneity (I2 = 89.3%). Among studies that accounted for underlying cirrhosis (n = 11), aspirin use was associated with a significant, 51% lower HCC risk (RR, 0.49; 95% CI, 0.45‐0.52), with minimal heterogeneity (I2 = 21.2%); however, among the eight studies that did not account for underlying cirrhosis, the observed RR was 0.68 (95% CI, 0.51‐0.82), with substantial heterogeneity (I2 = 90.8%). Furthermore, among studies that simultaneously accounted for both cirrhosis and use of statins and/or metformin (n = 7),( , , , , , , ) aspirin use was associated with a significant, 45% reduced risk of HCC (RR, 0.55; 95% CI, 0.49‐0.60), with minimal heterogeneity (I2 = 8.7%), suggesting that, together, those two factors might explain the significant heterogeneity in our primary analysis.

Several additional factors contributed to the observed heterogeneity. First, among the six studies in which HCC was confirmed by imaging and/or biopsy,( , , , , , ) aspirin use was associated with a 70% reduced HCC risk (95% CI, 0.15‐0.58), with moderate heterogeneity (I2 = 51.0%). In contrast, among the 13 studies that defined HCC using diagnostic codes,( , ) aspirin users had a 26% lower risk of HCC (95% CI, 0.62‐0.87), with substantial heterogeneity (I2 = 89.2%). Second, among cohort studies (n = 14), aspirin use was significantly associated with reduced HCC risk (RR, 0.59; 95% CI, 0.49‐0.72), with moderate heterogeneity (I2 = 52.4%), whereas substantial heterogeneity was found among the five case control studies (RR, 0.68; 95% CI, 0.39‐1.18; I2 = 89.3%). Finally, when we restricted the analyses exclusively to populations with established cirrhosis (n = 6 studies), aspirin use was associated with 31% lower HCC risk, with no heterogeneity (RR, 0.69; 95% CI, 0.62‐0.75; I2 = 0%). In contrast, no significant differences were found in subgroups defined by geographic region, assessment of viral hepatitis, required duration of aspirin usage (i.e., >4 weeks vs. no minimum), method of aspirin ascertainment (i.e., prospective vs. retrospective), or the definition of aspirin exposure (i.e., self‐report vs. prescription) (all P heterogeneity > 0.10; Table 2).

To assess whether any individual study might exert a disproportionate influence on the overall summary RR, we compared our findings after excluding each individual study in turn; no single study was found to substantially affect the main summary estimate (Supporting Fig. S3).

Exploratory Dose‐Response and Duration‐Response Analysis

Four studies( , , , ) reported risk of incident HCC according to dose and/or duration of aspirin use, from which we calculated continuous aspirin DDD exposures, as outlined in the Supporting Appendix. Meta‐analysis of these eligible studies revealed a significant, dose‐dependent and duration‐dependent inverse association between increasing aspirin DDD and reduced HCC risk. Specifically, each additional aspirin DDD contributed to a significant 0.02% reduction in HCC risk (adjusted RR, 0.98; 95% CI, 0.97‐0.98), which corresponds to an 8.4% risk reduction per year of daily aspirin use. The results showed substantial heterogeneity (Cochran’s Q2 test = 8.57; P = 0.036; I2 = 65.0%). There was no evidence of publication bias either quantitatively (P = 0.78) or qualitatively (Supporting Fig. S2). Given the small number of eligible studies, further subgroup analyses were not undertaken.

Number Needed to Treat

Due to substantial between‐study heterogeneity, it was not possible to calculate a single pooled estimate of the NNT with aspirin to prevent one case of incident HCC. Nevertheless, if we assume an HCC incidence rate of 0.6 per 100 person‐years among adults with noncirrhotic chronic HBV infection,( , ) and assume a 39% lower observed HCC risk with aspirin use, then an estimated 427 adults with noncirrhotic chronic HBV infection would need to be treated with aspirin for 1 year to prevent one case of incident HCC. Alternatively, if we restricted the population to higher‐risk patients with cirrhosis (in whom the annual HCC incidence rate is between 2% and 4%), then even if we assumed a conservative annual HCC incidence rate of 2% per year, only 128 adults with cirrhosis would need to be treated with aspirin for 1 year, to prevent one case of HCC.

Discussion

In this systematic review and meta‐analysis of more than 19,000 incident HCC cases recorded in over 2.3 million participants across seven different countries, aspirin use was associated with a significant, 39% lower risk of developing incident HCC. The HCC risk reduction associated with aspirin was similar in both Asian and Western populations, and in patients with and without viral hepatitis. Subgroup analyses further demonstrated that the apparent benefits of aspirin were most homogenous in well‐phenotyped populations that simultaneously accounted for cirrhosis and for concurrent use of other hepatoprotective medications. Additionally, our secondary dose‐response meta‐analysis of more than 1.3 million adults and over 4,294 incident HCC cases demonstrated that the inverse association between aspirin use and HCC incidence was highly dose‐dependent and duration‐dependent, such that 1 year of daily aspirin use contributed to a significant, 8.4% reduction in HCC risk. Importantly, the likelihood of significant selection or publication bias was very small. Overall, these findings provide further rationale for the design of randomized control trials (RCTs) to evaluate the safety and efficacy of aspirin therapy in at‐risk patients with chronic liver disease.

Although two recent meta‐analyses have addressed the association between aspirin use and HCC risk,( , ) those previous meta‐analyses each included fewer than 50% of published observational studies.( , , , , , , , , ) Furthermore, neither of those previous meta‐analyses addressed key HCC risk factors, including viral hepatitis, cirrhosis, concurrent use of statins or metformin, or the methods by which aspirin use was ascertained or HCC cases were confirmed. This is important, because failing to account for those factors could yield biased and imprecise risk estimates, with limited generalizability. In contrast, by incorporating 11 additional studies that were not part of the most recent published meta‐analysis, ( ) and by conducting detailed subgroup and stratified analyses, the current study is able to provide a more comprehensive assessment of aspirin use in relation to HCC risk.

The association between aspirin use and HCC risk was most homogenous in studies that simultaneously accounted for underlying cirrhosis and concurrent use of other hepatoprotective medications, as well as in studies that confirmed HCC diagnoses with appropriate imaging or pathology. It is well‐established that HCC risk is dependent on the severity of underlying liver disease; thus, accounting for underlying cirrhosis could address potential selection bias. Reliance on administrative diagnostic codes to define HCC may also introduce misclassification, which in turn could substantially attenuate risk estimates. Finally, it has been hypothesized that the combined use of aspirin together with either statins or metformin could act synergistically to prevent hepatocarcinogenesis.( , ) Indeed, in vitro studies of HCC cell lines have demonstrated that co‐administration of simvastatin and a cyclooxygenase‐2 inhibitor, NS398, act synergistically to activate apoptosis and inhibit proliferation.( )

The apparent benefits of aspirin were similar in both Asian and Western populations, and in patients with and without established viral hepatitis. Although this could suggest that the chemopreventive effects of aspirin might be broadly generalizable, caution must be stressed. In Asia, HBV infection represents the dominant HCC risk factor, whereas in the United States and Europe, the dominant risk factors include chronic HCV infection, alcohol use, and nonalcoholic fatty liver disease (NAFLD). Prior studies have found that aspirin may exert unique, HBV‐specific hepatoprotective and chemopreventive benefits, by reducing hepatic infiltration of CD8+ T cells and other pro‐inflammatory cells.( ) Furthermore, among published studies in Western populations, all but one( ) have lacked comprehensive data regarding underlying HBV or HCV infection, cirrhosis, or the relative contribution of prescription aspirin versus over‐the‐counter (OTC) aspirin. As the United States and parts of Europe have widely available OTC aspirin, it is possible that studies relying on prescription claims or medical record data in those regions may introduce exposure misclassification, by missing a proportion of aspirin users. Finally, it has been suggested that aspirin use and prescribing patterns may differ in Asia, compared with Western countries( ); thus, without careful accounting for both selection and indication bias, it is possible that aspirin users included in previous studies were at inherently lower risk of developing HCC, compared with nonusers.( , )

The association between aspirin use and HCC risk was modestly attenuated but remained statistically significant in analyses restricted only to patients with cirrhosis. It has been previously suggested that aspirin might exert its hepatoprotective effects early in the course of chronic liver disease, by preventing or delaying the development of liver fibrosis.( ) However, physicians are also less likely to prescribe aspirin to patients with cirrhosis, out of concern for bleeding; this raises the important possibility that selection bias or confounding by indication could have affected our results. Although the apparent benefits of aspirin were similar in studies that used propensity‐score approaches to balance treatment groups,( , , , , , , ) it is nevertheless impossible to exclude these potential biases. This in turn highlights the known limitations of observational studies and underscores the need for well‐designed RCTs to test the safety and efficacy of aspirin therapy across the full spectrum of chronic liver disease.

Due to its potent antiplatelet effects, the bleeding risks associated with aspirin represent an important consideration in patients with chronic liver disease. Previous RCTs have demonstrated that aspirin therapy for the primary prevention of cardiovascular disease increases the risk of major gastrointestinal and extracranial bleeding (0.10% vs. 0.07% per year in nonusers; P < 0.0001)( ); however, those trials excluded patients with cirrhosis. At present, data regarding the potential aspirin‐related bleeding risks in patients with liver disease are limited. In this meta‐analysis, only four retrospective cohort studies, three of which conducted in patients with chronic viral hepatitis and one conducted in patients with alcoholic cirrhosis,( ) specifically evaluated bleeding events associated with aspirin use.( , , , ) All four studies found a null association between daily aspirin use and excess bleeding risk, including a single exploratory comparison of patients with and without cirrhosis. However, given the small sample sizes and exploratory nature of those analyses, further research is needed to fully characterize the potential risks of aspirin in patients with liver disease of varying degrees of severity.

To our knowledge, this represents the most comprehensive meta‐analysis to date that is focused on aspirin use in relation to incident HCC risk. It is strengthened by the inclusion of over 2.3 million participants from seven countries, which increases generalizability and permits calculation of more precise risk estimates. Furthermore, by demonstrating a significant dose‐response and duration‐response relationship, we provide additional support for a causal association between aspirin use and reduced HCC incidence.

We acknowledge several limitations. First, our findings are based exclusively on observational studies; thus, we cannot exclude the possibility of residual confounding and bias related to immortal time, selection, or the underlying indications for aspirin use. However, among the few previous studies that were conducted in unselected, population‐based cohorts with careful accounting for those factors, the estimates were similar. Second, we acknowledge that there was substantial heterogeneity among the 19 included studies; however, this was no longer present among studies that carefully accounted for both underlying cirrhosis and concurrent use of other hepatoprotective medications. Nevertheless, there remain other important potential sources of heterogeneity that should be assessed in future studies, including individual major HCC risk factors (e.g., HBV, HCV, alcohol use, NAFLD or nonalcoholic steatohepatitis [NASH]), modifiers of HCC risk (e.g., fibrosis severity, adequacy of viral suppression in HBV, HCV eradication), or environmental and lifestyle factors (e.g., BMI, diabetes, smoking, diet). Third, the 19 included studies varied widely in the covariates used for multivariable models, and most (9 of 19) did not adjust for concomitant use of statins or metformin, two medications that have been independently associated with HCC risk reduction. Moreover, very few studies ascertained data regarding adherence to HCC screening recommendations. Fourth, we did not contact investigators to request unpublished data. Finally, although we conducted subgroup analyses in patients with cirrhosis, we lacked sufficient data to examine aspirin use across individual fibrosis stages, and only one study specifically evaluated aspirin use and HCC risk among patients with established NAFLD or NASH. Thus, future prospective studies are needed in well‐phenotyped populations with NAFLD/NASH, to assess whether aspirin might offer unique benefits in that growing patient population.

In conclusion, this systematic review and meta‐analysis demonstrates that aspirin use is associated with a significant dose‐dependent and duration‐dependent reduction in the risk of developing incident HCC. The apparent benefits of aspirin were similar in Asian and Western populations, and in patients with and without established viral hepatitis. Although HCC risk reduction was modestly attenuated in patients with cirrhosis, significant benefit nevertheless persisted. Well‐designed, prospective studies are needed to evaluate the safety of aspirin therapy across the complete spectrum of chronic liver disease, and to characterize the optimal dose, duration of use, and timing of aspirin initiation or discontinuation, to achieve maximal benefit while incurring minimal risks. Our findings support the planning of RCTs to confirm these observations.

Supplementary Material

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