Serum glucose and risk of cancer: a meta-analysis

Diabetes mellitus is a risk factor for many chronic diseases including cardiovascular disease and cancer. People with diabetes are 2-fold more likely to die from cancer than those without [1]. Therefore, it is thought that pre-diagnostic elevated blood glucose levels are associated with risk of cancer [2‐4]. Several epidemiological studies have investigated this association. The largest being a Korean cohort study of over one million men and women found a hazard ratio for all solid cancers of 1.22 (95% CI: 1.16-1.27) for men in the fifth quintile compared to the first quintile [5].

Despite the growing evidence for an association between diabetes and carcinogenesis [6], the mechanism by which raised glucose contributes to risk of cancer is not fully established [7]. The insulin – insulin growth factor (IGF)-1 axis is a commonly suggested pathway. It is thought that insulin resistance, which impairs the action of insulin and occurs in individuals with type 2 diabetes or metabolic syndrome, leads to prolonged hyperinsulinaemia. This decreases the production of IGF-binding proteins, which consequently results in raised IGF-1 levels and cellular changes leading to carcinogenesis via increased mitosis and reduced apoptosis [8]. It is, however, important to note that hyperinsulinemia during the early stages of diabetes may play a role in carcinogenesis independent of IGF-1 [9].

Another suggested pathway between glucose and risk of cancer is the reduced hepatic production of sex hormone binding globulin (SHBG) following prolonged hyperinsulinaemia [8]. This leads to an increase of available sex hormones, such as oestrogen and testosterone, which can drive carcinogenesis in hormonal sensitive cancers like postmenopausal breast or prostate cancers [8].

Elevated glucose can result in a state of chronic inflammation which changes the cytokine micro-environment and leads to an increase of cytokines such as interleukin 6 (IL-6) [10], tissue necrosis factor alpha (TNF-α) [11, 12] and vascular endothelial growth factor (VEGF) [13]. These changes can lead to an increase in tumour cell motility, invasion and even tumour metastasis [14, 15].

Finally, glucose may have a direct role in cancer development as it is a key nutrient. It is needed for proliferating cells and several types of tumour cells have been shown to have up-regulated glucose transporters [16].

Given the above-suggested pathways and the increasing prevalence of diabetes and cancer, this meta-analysis aims to summarize and quantify the existing evidence for a link between raised serum glucose and risk of all solid cancers. Using data from epidemiological studies on adult participants whose serum glucose levels and cancer diagnoses were assessed, this study aims to answer the question whether there is a higher risk of solid cancer in those with raised glucose levels, compared to those with normal levels.

This meta-analysis was conducted following the PRISMA statement for completing systematic reviews and meta-analyses [17].

The Pubmed search resulted in a total of 1,473 studies, 45 of which were deemed as initially relevant. A further 11 were identified via an Embase search and 18 from hand searches and grey literature, resulting in a total of 74 potentially relevant papers. Using the above-defined criteria, 55 were excluded (Figure 1).

A total of 19 studies were included in the primary analysis: six cohort, six case cohort, three hospital-based case–control, and four nested case–control studies. Nine studies were conducted in Europe, seven in Asia and three in the USA. Three studies presented data on all solid cancers, five on colorectal cancer, four on prostate cancer, two on breast cancer, two on endometrial cancer and one paper each for pancreatic, renal and hepatocellular cancers (Table 1).

The random effects analysis comparing overall cancer risk by serum glucose levels showed a pooled relative risk (RR) of 1.32 (95% CI: 1.20 – 1.45) for high versus normal levels of serum glucose (Figure 2). The I² statistic showed heterogeneity (I² = 92%; P < 0.05), even though every individual estimate indicated a positive association. Hence, we conducted a ‘remove one’ analysis to gauge each study’s impact; the I² statistic did not fall below 85%. Next, we conducted a sensitivity analysis using studies which included ‘all cancers’ as the outcome versus those with site specific outcomes. The heterogeneity remained high and the RR did not change drastically. When looking at “All cancers” as an outcome, the RR was 1.21(95% CI: 1.09-1.34) with and I² of 92%. When combining all site-specific cancers as an outcome, the RR was 1.38 (95% CI: 1.16-1.63) with an I² of 92%. Tumour-specific analyses were performed for the three most commonly studied cancers and resulted in pooled relative risks of 1.09 (95% CI: 0.95-1.25), 1.35 (95% CI: 1.21-1.51) and 1.14 (95% CI: 1.04-1.26), for breast, colorectal and prostate cancer, respectively. The related I² statistic was 74% for breast, 57% for colorectal, and 53% for prostate.

A stratified analysis by study type showed similar pooled RRs for cohort studies, case-cohort/nested case–control studies and hospital-based case–control studies (Figure 3): 1.24 (95% CI: 1.13-1.37), 1.29 (95% CI: 1.11-1.51), and 1.64 (95% CI: 1.11-2.43). The I² statistic was 92%, 76%, and 93%, respectively (Figure 4).

The overall pooled RR was 1.17 (95% CI: 1.09-1.25) for men and 1.32 for women (95% CI: 1.06-1.63). Studies where it was not possible to stratify by sex showed a pooled RR of 1.55 (95% CI: 1.40-1.71). The I² statistic for these sex-stratified analyses was 48% for men, 96%, for women and 19% where it was not possible to stratify by sex. Including only those with fasting glucose measurements did not have a large effect on the pooled RR either (RR: 1.32 (95% CI: 1.11-1.57). The I² statistic was 92%.

The pooled RR for hormonally driven cancers was 1.34 (95% CI: 1.02-1.77; I²: 96%) versus 1.41 (95% CI: 1.20-1.66; I²: 69%) for the non-hormonally driven cancers. IGF-1-driven cancers showed a pooled RR of 1.21 (95% CI: 1.09-1.36; I²: 67%) versus 1.73 (95% CI: 1.40-2.12; I²: 85%) for those not thought to be driven by IGF.

When assessing publication bias, the funnel plot showed an area of missing studies which includes regions of both low and high statistical significance suggesting that both studies that showed a non-significantly and significantly inverse association between glucose and cancer were missing. Therefore, under the assumption that studies are being suppressed because of a mechanism based on two-sided p-values, publication bias cannot be accepted as the only cause of funnel asymmetry.

This is the first meta-analysis examining the association of serum glucose and cancer risk. We found a consistent positive association, which was not altered strongly by sex, study type, or cancer type.

As previously described, several molecular mechanisms have been postulated in an effort to explain the association between glucose and carcinogenesis. The insulin – IGF-1 axis is the most commonly suggested pathway [93]. Our results showed a weaker association for IGF-1 driven cancers than the overall association or non-hormonally driven cancers, suggesting that if the insulin- IGF- 1 axis does play a role it is likely to be as part of a more complex molecular mechanism.

Another proposed mechanism is an increased availability of sex hormones caused by a reduction of SHBG in the presence of hyperinsulinaemia [7, 94]. However, our meta-analysis showed a similar association between elevated serum glucose and risk of hormonally and non-hormonally driven cancers. This suggests that this is not the only underlying mechanism for the link between glucose and cancer. It is possible that other mechanisms, i.e. chronic inflammation [10‐12] or direct actions of glucose [16], may also be playing a role.

To our knowledge this is the first comprehensive meta-analysis looking at epidemiological studies of serum glucose levels and cancer risk. Existing meta-analyses to date focused on the association between serum glucose levels and a specific type of cancer [4, 76]. A breast cancer-specific study including ten cohort studies found that the association between serum glucose levels and risk of breast cancer was small in non-diabetic subjects (pooled RR: 1.11 (95% CI: 0.98-1.25) [4]. The direction of this study is consistent with our findings, however our meta-analysis focused on high serum glucose levels as defined by the WHO definition for metabolic syndrome so that we also included potential diabetic subjects. Thus, when investigating serum levels of glucose, it is also important to consider diabetes. A bladder cancer-specific study showed that diabetes was associated with a 30% increased risk (95% CI: 1.18-1.43), which is consistent with the direction of the association found for serum glucose and cancer in our meta-analyses [76]. Other cancer types which also show a positive association with diabetes include pancreatic, endometrial, breast and colorectal cancer [20‐22, 95], however an inverse association has been observed for prostate cancer [91]. The latter must be interpreted with caution as diabetics have higher morbidity and mortality from other diseases. There may be competing risks masking their risk of prostate cancer [96]. However, it is important to note that diabetes is a slightly different exposure than serum levels of glucose as diabetic treatments may normalise glucose levels and potentially also affect risk of cancer [43].

We made every effort to include all relevant publications available to date through various sources, including grey literature, and the two main online databases (Pubmed and Embase). We were able to also access unpublished data from the MECAN group enabling us to include this large cohort of over 500,000 subjects [18]. In addition, clearly defined objective criteria for exposure, outcome, and other study characteristics were specified a priori. One limitation of our study is the heterogeneity between the different categorization methods for glucose ranges across the include studies. We tried to overcome this by combining the different categories as similarly as possible and believe this cannot significantly affect our findings. Nevertheless, this made it not possible in the current meta-analysis to make a distinction between pre-diabetes and diabetes. The overall results showed a rather large amount of heterogeneity, as suggested by the I² statistic. All of our sensitivity and subgroup analyses showed consistent findings in terms of direction of the association, while the heterogeneity remained high. Only when we conducted tumour specific analysis, the I² statistic reduced. This suggests that heterogeneity is most likely explained by combining studies with different outcomes. However, the consistent finding of a positive association in all our analyses supports the robustness of our findings. Six of the studies included, either had mixed or did not specify fasting status. However, exclusion of these studies did not alter the association observed. A further limitation is the lack of information regarding the diagnosis of diabetes, use of oral hypoglycaemics or insulin in those included in the studies. Future research including adjustment for components such as age, cancer treatment, diabetes (or its treatments), or BMI would be useful in confirming the importance of raised glucose in carcinogenesis. All studies included were soundly designed and executed epidemiological studies, which clearly defined their methodology. However, the size of the studies did vary considerably. The two largest studies [5, 18] did account for well over half of the cases included, but they represent a Korean and European population which we believe can be broadly applicable to all patient populations. Limitations reported by the individual studies overlap widely. They include, having only localised cancer as an outcome, small sample size, specific demographic groups only (i.e. smokers only), lack of information on diabetes and obesity and all but one study [81] used single measurements of glucose for their analysis.

A positive association was found between serum glucose levels and risk of cancer. The heterogeneity observed between studies calls for more translational studies investigating how serum glucose is associated with carcinogenesis. However, given there were seven million deaths from cancer worldwide in 2011 and it is estimated that more than a third were attributable to modifiable risk factors [97], these findings are of public health importance as measures to reduce serum glucose via lifestyle and dietary changes could be implemented to reduce risk of cancer.