Sex-dependent difference in the effect of metformin on colorectal cancer-specific mortality of diabetic colorectal cancer patients.

AIM: To assess factors associated with the higher effect of metformin on mortality in diabetic colorectal cancer (CRC) patients, since the factors related to the effectiveness of metformin have not been identified yet.
METHODS: Between January 2000 and December 2010, 413 patients diagnosed with both stage 3/4 CRC and diabetes mellitus were identified. Patients' demographics and clinical characteristics were analyzed. The effect of metformin on CRC-specific mortality and the interactions between metformin and each adjusted factor were evaluated.
RESULTS: Total follow-up duration was median 50 mo (range: 1-218 mo). There were 85 deaths (45.9%) and 72 CRC-specific deaths (38.9%) among 185 patients who used metformin, compared to 130 total deaths (57.0%) and 107 CRC-specific deaths (46.9%) among 228 patients who did not use metformin. In multivariate analysis, survival benefit associated with metformin administration was identified (HR = 0.985, 95%CI: 0.974-0.997, P = 0.012). Interaction test between metformin and sex after adjustment for relevant factors revealed that female CRC patients taking metformin exhibited a significantly lower CRC-specific mortality rate than male CRC patients taking metformin (HR = 0.369, 95%CI: 0.155-0.881, P = 0.025). Furthermore, subgroup analysis revealed significant differences in CRC-specific mortality between the metformin and non-metformin groups in female patients (HR = 0.501, 95%CI: 0.286-0.879, P = 0.013) but not male patients (HR = 0.848, 95%CI: 0.594-1.211, P = 0.365). There were no significant interactions between metformin and other adjusted factors on CRC-specific mortality.
CONCLUSION: We showed a strong sex-dependent difference in the effect of metformin on CRC-specific mortality in advanced stage CRC patients with diabetes.

Core tip: Evidence from previous studies has identified the anti-tumor effect of metformin; however, the factors related to effectiveness of metformin in diabetic colorectal cancer (CRC) patients have not been identified yet. Identifying subgroup patients who benefit from metformin treatment is important for future clinical application of metformin, and a strong sex-dependent difference of metformin effect in advanced CRC patients has been identified in this present study.

INTRODUCTION

Although the survival rate for colorectal cancer (CRC) has increased because of early detection and intervention at earlier stages, CRC is still the 3rd most common cancer and the 4th leading cause of cancer death in the western and Asian countries[1-3]. Cancer and diabetes, especially type 2 diabetes mellitus (DM), are two of the most prevalent diseases and major causes of morbidity and mortality worldwide[4]. Despite some argument concerning the influence of diabetes on CRC, studies, including meta-analyses, have consistently demonstrated that type 2 DM is an independent risk factor for CRC and that diabetic patients with CRC have worse outcomes than non-diabetics[4,5]. A possible role for anti-hyperglycemic medications in progression and prognosis of CRC has been suggested, based on the hypothesis that tumor growth is promoted by the trophic action of insulin[4,6].

Metformin is broadly used for the treatment of type 2 DM, which successfully decreases circulating levels of glucose and insulin mainly by improving insulin resistance. Evidence from preclinical studies has identified the anti-tumor effect of metformin, showing inhibition of tumor growth and induction of apoptosis in cell lines and animal models of various cancers[7-9]. Several clinical studies, including our previous study[10-18], have shown the ability of metformin to reduce the incidence of CRC and improve survival of CRC patients. As stated in other studies, one of the potential mechanisms of the anti-tumor effect of metformin is via activation of AMP-activated protein kinase (AMPK). AMPK activation has an inhibitory effect on cancer cell growth and new blood vessel formation by prohibiting activation of the mammalian target of rapamycin (mTOR)[19-21]. With these direct cellular effects of metformin, the indirect or systemic effect of metformin is relief of insulin resistance-associated hyperinsulinemia and hyperglycemia, which counteracts the dependence of cancer cells on glucose as predominant source of energy[20,22].

Despite substantial evidence from in vivo and in vitro research supporting the possible efficacy of metformin as an anti-cancer agent and numerous clinical studies investigating the effect of metformin on CRC, particular factors or specific groups of patients associated with the effectiveness of metformin have not been identified. Our study assessed factors that may affect the efficacy of the anti-cancer action of metformin on CRC-specific mortality in diabetic CRC patients. Herein, we selected particular factors that might be associated with the “more effective” group (those who benefit from metformin for improving CRC-specific survival) and verified these assumptions using interaction analysis.

MATERIALS AND METHODS

Patients

The electronic records of 9472 consecutive patients with a diagnostic code of colon or rectal cancer seen at a single institution (Severance Hospital, Yonsei University, Seoul, Korea) between January 1, 2000 and December 31, 2010 were identified. A manual retrospective review was conducted for all patients to identify those with a prior history of DM. Among those identified, 1584 had the type 2 diabetes diagnostic code during follow-up, of which 790 were excluded based on the following exclusion criteria: type I diabetes (n = 38), diabetes diagnosed after CRC diagnosis (n = 521), incomplete records (including medication records) (n = 77), metformin use for less than 6 mo (n = 105), and any cancer previous to CRC diagnosis (n = 49). According to our previous studies, only stage 3 CRC patients[12] and resectable stage 4 CRC patients[23] showed a survival benefit from metformin. Considering these results, advanced stage CRC patients in the latter two groups, denoting stage 3 and 4 patients, were selected and analyzed; this group included 185 DM patients treated with metformin and 228 DM patients not taking metformin. There were 135 female patients (32.7%) in the study population.

Patient demographics and clinical characteristics, including age at diagnosis, sex, total follow-up duration, duration of diabetes, body mass index (BMI), family history of colorectal malignancy, smoking history and drinking history were obtained from medical records. BMI was stratified into “underweight” (BMI < 18.5), “normal” (BMI range: 18.5-24.9), “overweight” (BMI range: 25.0-29.9) and “obese” (BMI ≥ 30.0), based on World Health Organization BMI classification[24]. Laboratory findings included plasma glucose levels, glycated hemoglobin (HbA1C) levels, and pretreatment carcinoembryonic antigen (CEA) levels. Information relevant to the CRC diagnosis, such as stage, site, histology, differentiation, resection margin, lymphovascular invasion, microsatellite instability (MSI) status, and treatment modality were reviewed via the medical records as well. The use of other diabetes medications (sulfonylureas, thiazolidinediones, α-glucosidase inhibitors, insulin, etc.) and the use of aspirin were also explored. The date of diagnosis of CRC was defined as the day of pathologic diagnosis. Every enrolled patient had undergone colonoscopy. We identified deaths through medical records, and determined the cause of death in all cases.

The institutional review board of Severance Hospital, Yonsei University, Seoul, Korea approved this study.

Tumor staging and treatment assessment

All patients were diagnosed with pathologically confirmed CRC and were evaluated during their baseline visit to Severance Hospital for appropriate staging according to the 7th version of the AJCC Tumor/Node/Metastatic staging system. Treatment modality was determined by extent and location of the tumor. Based on the National Comprehensive Cancer Network guideline, locally advanced tumors or advanced tumors with resectable metastatic lesions were treated by surgery followed by adjuvant chemotherapy with or without radiotherapy, or by neoadjuvant chemotherapy, or chemoradiation therapy followed by surgery. Advanced CRC with distant metastasis was treated by palliative chemotherapy or conservative care.

Statistical analysis

Differences between the metformin and non-metformin groups with regard to covariates were determined using Pearson’s χ2 test or Student’s t-test when the data were categorical or continuous, respectively. In the primary analyses, the odds of overall and CRC-specific death for patients with diabetes treated with metformin and not treated with metformin were calculated using univariate logistic regression analysis. The multivariate Cox proportional hazards regression method was used to estimate HRs and 95%CIs after adjustment for patient-related variables, including age at diagnosis, sex, stage of cancer, BMI, diabetes duration, smoking history, cancer site, and use of insulin, aspirin, sulfonylurea and thiazolidinedione.

Survival curves were generated using the Kaplan-Meier method and were compared using log-rank statistics. In the secondary analyses, interaction analyses of Cox regression results were performed to reveal the factors associated with metformin use. These variables included age at diagnosis (≥ 50 or < 50), sex (male or female), smoking history (yes or no), tumor stage (III or IV), site (colon or rectum), sulfonylurea use (yes or no), insulin use (yes or no), and DM duration (years).

All P values were two sided, with a P < 0.05 considered significant. Most of the statistical analyses were performed using SPSS version 21.0 (SPSS, Inc., Chicago, IL, United States). SAS version 9.2 (SAS Inc., Cary, NC, United States) was used when identifying the cut-off value of metformin duration that provided the best fit of the log-rank test statistics of overall and CRC-specific survival.

RESULTS

Patients’ demographics and clinical characteristics

The metformin and non-metformin groups had similar patient demographics and clinical characteristics (Table 1). The median age of patients was 64 years (range: 33-91 years). Baseline characteristics, including age at diagnosis, sex, BMI, familial history of cancer, smoking and drinking history, were not significantly different between the metformin group and the non-metformin group. Factors associated with cancer, including tumor stage, tumor site (colon or rectum), tumor differentiation, resection margin positivity, MSI status, and pretreatment CEA level were not significantly different between the two groups. Clinical characteristics associated with diabetic severity status, such as HbA1C levels and duration of diabetes, were similar between the two groups; however, serum fasting glucose levels were lower in the non-metformin group compared to the metformin group (143.8 mg/dL vs 132.4 mg/dL, P = 0.012).

Table 1

Patient demographics and baseline clinical characteristics n (%)

	Metformin group, n = 185	Non-metformin group, n = 228	P value
Age at diagnosis in yr, mean ± SD	63.5 ± 8.789	63.49 ± 10.218	0.991
< 50	12 (6.5)	27 (11.8)	0.064
≥ 50	173 (93.5)	201 (88.2)
Sex			0.921
Male	125 (67.6)	153 (67.1)
Female	60 (32.4)	75 (32.9)
DM duration in yr, median (range)	8 (1-120)	6 (1-40)	0.068
Family history of CRC	8 (4.3)	13 (5.7)	0.526
BMI in kg/m2, mean ± SD	23.6 ± 3.0	23.5 ± 3.0	0.596
Normal < 25	148 (80.0)	173 (76.5)	0.300
Overweight 25-30	33 (17.8)	51 (22.6)
Obese ≥ 30	4 (2.2)	2 (0.9)
Smoking			0.371
Never-smoker	89 (48.1)	123 (53.9)
Ex-smoker	42 (22.7)	40 (17.5)
Current smoker	54 (29.2)	65 (28.5)
Alcohol			0.556
None	82 (44.3)	112 (49.1)
< 1 drink/d	42 (22.7)	51 (22.4)
≥ 1 drink/d	61 (33.0)	65 (28.5)
Aspirin use	50 (27.0)	39 (17.1)	0.015
Insulin use	17 (9.2)	27 (16.2)	0.035
Sulfonylurea use	116 (62.7)	153 (67.1)	0.350
Thiazolidinedione use	18 (9.7)	12 (5.3)	0.082
CEA in ng/mL, median (range)	4.7 (0.2-9100.0)	6.4 (0.1-5946.0)	0.359
HbA1c, mean ± SD	8.7 ± 16.7	7.3 ± 1.4	0.349
Glucose in mg/dL, AC ± SD	143.8 ± 46.1	132.4 ± 41.1	0.012
Cholesterol in mg/dL, total ± SD	167.9 ± 47.8	164.6 ± 39.6	0.483
Tumor stage			0.110
III	136 (73.5)	151 (66.2)
IV	49 (26.5)	77 (33.8)
Tumor site			0.940
Colon	106 (57.9)	130 (58.3)
Rectum	77 (42.1)	93 (41.7)
Histology			0.001
Adenocarcinoma	177 (97.8)	199 (89.6)
Mucinous carcinoma	4 (2.2)	23 (10.4)
Differentiation			0.155
Well differentiated	13 (7.4)	16 (7.8)
Moderately differentiated	148 (84.6)	174 (84.5)
Poorly differentiated	14 (8.0)	12 (5.8)
Resection margin +	3 (1.7)	1 (0.6)	0.371
Lymphovascular invasion	56 (25.9)	76 (50.0)	0.031
MSI state			0.670
MSi	78 (89.7)	68 (90.7)
MSI-low	6 (6.9)	6 (8.0)
MSI-high	3 (3.4)	1 (1.3)
Treatment modality			0.160
Resection only	9 (4.9)	20 (8.8)
Resection + adjuvant chemotherapy	115 (63.2)	126 (55.3)
Resection + chemoradiotherapy	22 (12.1)	24 (10.5)
Neoadjuvant chemotherapy + resection	17 (9.3)	17 (7.5)
Chemotherapy only	17 (9.3)	35 (15.4)
Conservative care	2 (1.1)	6 (2.6)

BMI: Body mass index; CEA: Carcinoembryonic antigen; CRC: Colorectal cancer; DM: Diabetes mellitus; MSI: Microsatellite instability.

The use of other diabetes medications, including insulin, sulfonylurea and thiazolidinedione, was also investigated, because the status of individuals taking these medications could reflect later stage diabetes, and these medications could be associated with tumorigenesis and prognosis. The use of these medications was not significantly different between the two groups, with the exception of insulin use, which was lower in the metformin group than in the non-metformin group (9.2% vs 16.2%, P = 0.035). Aspirin, a drug known to have beneficial effects in cancer survival, was also evaluated and its use was statistically different between two groups (27.0% vs 17.1%, P = 0.015). Meanwhile, there was no difference in the treatment modality used for CRC between the two groups.

Metformin use and survival analysis

The median follow-up duration was 50 mo (range: 1-180 mo). With respect to the entire cohort, there were 129 (31.3%) recurrences, 215 (52.0%) total deaths, and 179 (43.3%) CRC-specific deaths. With respect to metformin use, there were 85 (45.9%) total deaths and 72 (38.9%) CRC-specific deaths among 185 patients who used metformin, compared with 130 (57.0%) total deaths and 107 (46.9%) CRC-specific deaths among 228 patients who did not use metformin. The estimated 5-year CRC-specific survival rates were 65.4% and 52.4% for the metformin and non-metformin groups, respectively, and 10-year CRC-specific survival rates were 50.8% and 43.1%, respectively. These results were significantly different (HR = 0.724, 95%CI: 0.537-0.976, P = 0.032) (Figure 1A). For the metformin and non-metformin groups, the estimated 5-year overall survival rates were 60.8% and 47.9% respectively, and the 10-year overall survival rates were 45.8% and 33.8% respectively, also showing significant differences (HR = 0.706, 95%CI: 0.537-0.929, P = 0.013) (Figure 1B).

Figure 1

Colorectal cancer-specific survival and overall survival according to metformin treatment in colorectal cancer patients with diabetes mellitus. A: Colorectal cancer-specific survival according to metformin treatment; B: Overall survival according to metformin treatment.

In addition, we used the duration of metformin treatment in multivariate survival analysis, and showed this factor to be an independent predictor for CRC-specific mortality in diabetic patients with advanced CRC after adjustment of clinically relevant factors (HR = 0.985; 95%CI: 0.974-0.992, P = 0.012). BMI (HR = 0.514, 95%CI: 0.287-0.919, P = 0.025), tumor stage (HR = 8.401; 95%CI: 5.285-13.355, P < 0.001), and HbA1C level (HR = 1.015, 95%CI: 1.004-1.027, P = 0.01) were also revealed as independent predictive factors (Table 2).

Table 2

Multivariate logistic regression analysis for colorectal cancer-specific mortality

	HR	95%CI	P value
Age at diagnosis of ≥ 50 or < 50	0.723	0.312-1.675	0.449
Sex, female or male	0.592	0.357-0.982	0.042
BMI of ≥ 25 or < 25	0.514	0.287-0.919	0.025
Smoking history as yes or no	0.681	0.359-1.291	0.239
Aspirin use as yes or no	0.802	0.455-1.415	0.446
Metformin treatment duration in mo	0.985	0.974-0.997	0.012
Sulfonylurea use as yes or no	1.300	0.798-2.120	0.292
Insulin use as yes or no	1.041	0.511-2.121	0.912
Stage IV or III	8.401	5.285-13.355	< 0.001
Site as rectum or colon	0.823	0.521-1.299	0.403
Pathology	0.801	0.238-2.701	0.721
Diabetes duration	0.968	0.935-1.001	0.059
HbA1C	1.015	1.004-1.027	0.010

BMI: Body mass index; CRC: Colorectal cancer.

We performed another analysis with the metformin group only, using total duration of metformin treatment. The results showed that improvement of CRC-specific (HR = 0.976, 95%CI: 0.948-0.995, P = 0.012) and overall survival rates (HR = 0.982, 95%CI: 0.967-0.997, P = 0.019) was associated with longer duration of metformin treatment, after adjustment of clinically relevant factors, including age at diagnosis, sex, medication history, tumor stage, tumor site, diabetes duration, and HbA1C. Analysis using Contal and O’Quigley’s method[25] revealed that the cut-off value for metformin treatment duration that fit the CRC-specific survival statistics was 22 mo.

Interaction analysis of survival benefit from metformin treatment

To determine the subgroup with the greater metformin effect, interaction tests between metformin and each clinical factor were performed, after adjustment for other covariates including age at diagnosis, sex, BMI, medication use, stage, site, diabetes duration, and HbA1C. Interaction tests between metformin and sex with adjustment for relevant factors revealed that female CRC patients treated with metformin exhibited a significantly lower CRC-specific mortality rate compared to male CRC patients treated with metformin (HR = 0.369, 95%CI: 0.155-0.881, P = 0.025) (Table 3).

Table 3

Interaction analysis of metformin and relevant factors on colorectal cancer-specific mortality

	HR	95%CI	P value
Metformin-Sex	0.369	0.155-0.881	0.025
Metformin-BMI	1.000	0.974-1.026	0.972
Metformin-Site	0.941	0.441-2.006	0.875
Metformin-HbA1c	0.999	0.926-1.078	0.979

BMI: Body mass index.

Subgroup analysis based on sex was performed and showed a significant difference in CRC-specific mortality between the metformin and non-metformin groups for females (HR = 0.013, 95%CI: 0.286-0.879, P = 0.013) (Figure 2B), while there was no significant difference between the two groups for males (HR = 0.365, 95%CI: 0.594-1.211, P = 0.365) (Figure 2A). Interaction analysis of metformin with other adjusted factors did not show any significant difference in CRC-specific mortality (Table 3). Intriguingly, as documented earlier, the duration of metformin treatment affected both CRC-specific mortality and overall mortality; however, the mean duration of metformin treatment between males and females was not significantly different (33.76 ± 24.45 mo for males and 28.05 ± 20.59 for females, log rank P = 1.06). Subgroup analysis based on metformin treatment showed that female patients had significantly lower CRC-specific mortality than males in the metformin group (HR = 0.332, 95%CI: 0.144-0.764, P = 0.009), while the non-metformin group showed no significant difference in CRC-specific mortality between male and female patients (HR = 0.73, 95%CI: 0.38-1.402, P = 0.345).

Figure 2

Colorectal cancer-specific survival based on sex. A: CRC-specific survival according to metformin treatment in males; B: CRC-specific survival according to metformin treatment in females. CRC: Colorectal cancer.

DISCUSSION

Two of the most common diseases worldwide, DM and CRC, share numerous risk factors. Previous studies, including meta-analyses, demonstrated the association between DM and increased risk of CRC; moreover, metformin, one of the most commonly prescribed anti-diabetes agents, improved survival of CRC patients[11,12,14,16,18]. We previously showed that CRC patients with diabetes treated with metformin had lower mortality than those not treated with metformin, and that metformin treatment was associated with a decreased incidence of colorectal adenomas in diabetic patients with previous CRC[12,26]. Furthermore, we showed an association between the metformin treatment in stage IV CRC patients with diabetes and lower risk of tumor recurrence after curative resection[23]. However, there has been no study that investigated the specific subgroup within CRC patients with diabetes who obtained a survival benefit from metformin use. In the present study, we aimed to determine the particular subgroup among diabetic CRC patients that could benefit from the anti-cancer effect of metformin and discovered that sex was the single clinical factor that predicted improved survival related to metformin treatment. In addition, by including the duration of metformin treatment as a factor, we showed that longer duration of metformin treatment was associated with improved CRC-specific and overall survival.

Metformin treatment has been associated with decreased risk and improved survival of DM patients with various types of cancer, including colorectal, pancreatic, liver, ovarian, breast, and endometrial[11,18]. The mechanism of action of metformin as an anti-cancer drug has not been clearly identified, although a shared pathogenesis for DM and some cancers is possible, e.g., beta oxidation of fatty acids or mitochondrial function[22]. One of the most well-known mechanisms of metformin is the stimulation of peripheral AMPK with decreased hepatic gluconeogenesis, increased insulin sensitivity, and hepatic fatty acid oxidation[20]. Under physiological conditions, AMPK is an intracellular energy sensor and is activated when the cellular AMP/ATP ratio increases. AMPK activation leads to inhibition of mTOR signaling. mTOR phosphorylation is mainly involved in cell growth, cell cycle progression, and angiogenesis. Inhibition of mTOR signaling can be an excellent cancer therapy target, as the mTOR pathway is commonly decontrolled in numerous types of cancer, and activation of this pathway is associated with poor prognosis and resistance to chemotherapy[21,27,28]. Other suggested anti-cancer mechanisms of metformin include reduced insulin growth factor-1, inhibition of angiogenesis, apoptosis, and induction of cell cycle arrest[6,29,30].

In our study population, females had a higher survival rate associated with metformin treatment after adjustment of other clinically significant factors. No other studies have reported the interaction between sex and survival benefit from metformin in diabetics with CRC. However, the study by Lee et al[18] of a cohort of 800000 Taiwanese showed that metformin effectively reduced the incidence of CRC in diabetic women and liver cancer in diabetic men, which suggested that sex could be an important interaction factor. Numerous explanations for this phenomenon can be suggested, and the higher survival rate of females compared to males among patients with CRC should initiate additional studies.

A Japanese study of 82402 patients with invasive CRC who had undergone surgery between 1985 and 2004 revealed a reduced risk of CRC-specific death for females relative to males that persisted over time[31]. McArdle et al[32] reported that overall survival and CRC-specific survival was significantly higher in females among patients who underwent elective surgery, after adjustment of clinical covariates. One study conducted in Israel by Purim et al[33] also reported sex-age interactions with the incidence of CRC and survival of CRC patients showed lower incidence and better prognosis for females. The answer for this superior CRC survival in females compared to males is usually related to female sex hormone status, particularly serum estrogen levels[31,34,35].

Circulating levels of 17b-estradiol (E2), the main estrogenic compound, are exceedingly higher in females compared to males and decrease with increasing age. While females are exposed to relatively high levels of endogenous E2 between adolescence and the 4th or 5th decade of life, in males, E2 levels remain low and steady, and drop minimally with aging. However, after menopause, serum E2 levels of females decline to levels similar to those of males. Moreover, the effect of estrogen on the gastrointestinal tract is well known, and in esophageal, gastric, and colon cancers, which have higher incidence and mortality rates among males, the role of estrogen has been investigated[36,37]. Wang et al[38] reported that people at risk of esophageal cancer have low levels of estrogen compared to healthy subjects. This finding was supported by experimental studies showing that estrogen regulates growth, cell differentiation, and cell function in the gastrointestinal tract. The possible role of estrogen in CRC development has been suggested by several lines of epidemiological, clinical and experimental evidence; however, the effect of estrogen in the progression of CRC has not been clearly identified[37,39].

With respect to metformin and female hormones, we hypothesized that metformin acts on the estrogen pathway to affect progression of CRC. This can be inferred from another result of Cossor et al[40], showing no significant survival benefit of metformin in post-menopausal females. Reports of the anti-cancer effect of metformin in estrogen receptor (ER)-positive breast cancer and the anti-estrogenic effect of metformin in control of abnormal endometrial proliferative disorders support this hypothesis[41,42]. The decrease in ER expression in tumors from females with endometrial cancer and DM treated with metformin compared to women treated with insulin also supports this hypothesis[42]. In addition, metformin repressed protein and mRNA expression of E2/ERα-regulated genes to a greater degree than tamoxifen, which resulted in inhibition of cell proliferation of ERα-positive breast cancer cells[41].

Interestingly, estrogen (E2) primarily prevented the development of CRC; however, in CRC patients, E2 promoted cancer progression[43]. Proliferation of CRC cells is known to be mediated by ERα, while the level of ERα expression is usually low in normal colon tissue and CRC tissue[43]. However, when the expression of ERβ in cancer cells decreases and the ratio of ERα/ERβ rises, ERα expression becomes dominant and results in cell proliferation and inhibition of apoptosis[43,44]. Interestingly, studies have demonstrated sex differences in ER expression in CRC[44,45]. Nüssler et al[44] reported a significant increase in ERα protein expression in males but not in females, while there was no significant difference in ERα and ERβ protein in normal colon mucosa between males and females. In the same study, ERβ protein expression in CRC cells was significantly decreased in both males and females, but far more in males[44].

Another study conducted by Press et al[45] reported the correlation between ERβ protein expression in CRC cells, overall survival and sex. Higher ERβ protein expression was associated with better overall survival in females but worse survival in males[45]. From these reports, we inferred that ER status in CRC tissue might have a role in cancer progression that could be different between males and females. The effect of metformin might be related to estrogen, regulation of ERα or ERβ expression, or, possibly, E2/ERα ratio as well. Although these relationships have not been elucidated thus far, we postulate that our findings provide the basis for future studies.

As confounding factors, DM severity and treatment with other drugs could affect the survival benefit conferred by metformin. Severity and duration of DM are important factors for cancer progression, considering that persistent hyperglycemia and hyperinsulinemia might alter the immune system and cause a chronic pro-inflammatory condition[4,5]. This pathologic state is due to the metabolic abnormalities that characterize diabetes, especially under conditions of poor metabolic control. In the present study, we measured glycated hemoglobin to represent the severity of DM, and total duration since diagnosis of DM. In addition, other anti-hyperglycemic agents may conceal or diminish this metformin-related cancer protection.

Therefore, we adjusted DM severity and duration, along with other anti-hyperglycemic agents, to assess the dose-dependent survival benefit of metformin. Several studies have investigated the relationship between metformin duration or dosage-related numerical values and the incidence of CRC. While there are some discrepancies between the study results, one study showed that patients treated with metformin for over 3 years showed a significantly reduced relative risk of CRC (HR = 0.643, 95%CI: 0.490-0.845) compared to patients not treated with metformin[46]. Interestingly, Lee et al[18] demonstrated that total cancer incidence was significantly associated with mean daily dose of metformin. Furthermore, subgroup analysis of males and females showed other intriguing results; only the hazard ratio of liver cancer incidence was significantly associated with mean daily dose of metformin in males, while CRC incidence was significantly associated with mean daily dose in females[18]. Our study results showed the relationship between the cumulative effect of metformin and CRC-specific survival. In addition, duration of DM since diagnosis, duration of metformin treatment, and level of glycated hemoglobin were not significantly different between males and females, which showed that the severity of DM or months of metformin treatment had no effect on the sex-related interaction.

While this study provided notable associations between metformin treatment and sex in the survival of CRC patients with DM, there were some limitations. First, we could not capture metformin treatment non-compliance, which could have resulted in exposure misclassification and biased the results toward the null hypothesis. Additional study limitations included a small sample size, which reduced the power to detect significant differences in survival, even though our findings were similar to previous studies of metformin treatment and CRC outcomes. Data regarding the specific cancer location, such as right or left sided, were not available for this study. Location of cancer is an important difference between males and females, where females develop more proximal, and males more distal colon and rectal cancers[47,48]. Finally, because the data analyzed in this study population were collected from a tertiary medical care unit, results may not be generalizable to the general population. Further studies with a larger and more diverse population should be conducted to strengthen the relationship between sex and the anti-cancer effect of metformin in CRC patients with DM. Moreover, future prospective studies should consider this sex-specific difference when performing clinical trials using metformin as an additive therapeutic agent for diabetic and non-diabetic CRC patients.

COMMENTS

Background

Previous studies showed metformin use was associated with decreased colorectal cancer (CRC) mortality. The identification of factors associated with the effect of metformin on mortality in diabetic CRC patients will provide useful information when applying metformin in cancer treatment.

Research frontiers

Despite substantial evidence from in vivo and in vitro research supporting the possible efficacy of metformin as an anti-cancer agent and numerous clinical studies investigating the effect of metformin on CRC, particular factors or specific groups of patients associated with the effectiveness of metformin have not been identified. Herein, authors selected particular factors that might be associated with the “more effective” group, i.e., those who benefit from metformin for improving CRC-specific survival, and verified these assumptions using interaction analysis.

Innovations and breakthroughs

The authors discovered that sex was the single clinical factor that predicted improved survival related to metformin treatment. This is also the first study to report the interaction between sex and survival benefit from metformin in diabetics with CRC. Furthermore, results of this study showed the relationship between the cumulative effect of metformin and CRC-specific survival.

Applications

The results from this study showing sex-related effectiveness of metformin in survival of diabetic CRC patients can be applied to the additional usage of metformin in conventional adjuvant chemotherapy. These future prospective studies should consider this sex-specific difference when performing clinical trials using metformin as an additive therapeutic agent for diabetic and non-diabetic CRC patients.

Terminology

Metformin is an oral medication which is broadly used for the treatment of type 2 diabetes mellitus by decreasing circulating levels of glucose and insulin and mainly by improving insulin resistance. AMP-activated protein kinase and mammalian target of rapamycin are intracellular molecules associated with cell metabolism and growth.

Peer-review

This is a very good work, the authors addressed the factors associated with the effect of metformin on mortality in diabetic CRC patients. Interestingly, the results showed that female CRC patients taking metformin exhibited a significantly lower CRC-specific mortality rate than male CRC patients taking metformin. Identifying subgroup patients who benefit from metformin treatment is important for further study in this field and this manuscript provided interesting and valuable findings.