The Obesity Paradox in Cancer: a Review

BMI is commonly used as an approximation of general body adiposity in studies that have observed the obesity paradox. BMI is appealing as it is routinely measured in primary care and hospital settings and there are well-defined criteria for normal, overweight, and obese categories. However, BMI is a relatively crude measure of body adiposity and body composition and does not differentiate between lean mass and fat mass. In turn, body composition varies with age, sex, and ethnicity [22], such that there are currently no specific age-gender-ethnicity indices to define obesity in a standardized manner. Thus, for example, in a cancer population, overweight individuals (defined by BMI) might be younger with high muscle mass (compared with normal weight), explaining their better outcome compared with normal weight.

The paradox might not exist if alternate measures of body composition or adipose tissue were used. Thus, for example, we found no examples of studies in patients with cancer demonstrating the obesity paradox when anthropometric measures other than BMI or body composition indices were used. Alternate indices include measurements such as waist circumference, waist to hip ratio, skinfold, and body composition assessment techniques such as dual-energy X-ray absorptiometry, CT, and MRI, and quantify different body fat components such as subcutaneous adipose tissue (SAT) and visceral 
adipose tissue (VAT) [34, 35]. Gonzalez and colleagues [36] recently explored this hypothesis and showed that the obesity paradox was present in 175 patients with various cancers (breast, gynecological, head and neck, lung, and gastrointestinal) when BMI was the exposure of interest but disappeared when obesity was defined using fat mass index and fat-free mass index.

Confounding occurs when there are variables that are associated with both the outcome (death) and the exposure (obesity) and are not on the causal pathway between them. A common example is smoking, where BMI values are generally lower in current smokers than in never smokers. Other examples include deprivation, socioeconomic status, physical activity, and diet. It is difficult to adjust for all confounding factors, as many are unobserved. Measurement error may lead to incomplete removal of confounding, and to avoid this in the smoking context, some studies exclude smokers from their analysis [37], but usually, this is at the cost of disregarding a large proportion of the sample. Another approach would be to quantify exposure more accurately, for example, in terms of smoking duration and intensity using pack-years variables or cumulative lifetime exposure.

An example of confounding as a source of a spurious obesity paradox is illustrated in clinical treatment series reported by Hakimi and colleagues [12] in 2119 patients with renal cell carcinoma undergoing surgical resection at Memorial Sloan Kettering Cancer Center. Higher BMI was associated with reduced cancer-specific mortality in univariable analyses (P < 0.005), but this association was lost after adjusting for stage and grade (P > 0.10).

The obesity paradox might be due to a specific form of selection bias, known as the collider stratification bias, caused during the statistical analysis due to conditioning on a subpopulation selected based on a collider variable. In turn, a collider variable is one with at least two causes common to the risk of the variable and the outcome of interest. For example, cancer incidence is a collider variable because it is “caused” by both obesity and other risk factors (e.g., smoking). There is a well-recognized inverse relationship between BMI and smoking. Thus, cancer patients who are not obese are more likely to have other risk factors, such as smoking, and in the analyzed subpopulation, an inverse association is artificially generated (or strengthened) between obesity and the other risk factors. Additionally, Banack and Kaufman [38••] demonstrate how confounding due to smoking is increased in the presence of collider stratification bias. In a contrary direction, Sperrin et al. [39••], using an equation-derived approach within a counterfactual framework, show that the biases attributable to collider stratification are small and cannot explain the large paradoxical relationships seen in epidemiological studies.

A further dimension is detection bias. This is the co-occurrence of two diagnoses together. Thus, for example, being overweight and obese is associated with the development of diabetes and cardiovascular disease. Where patients present with new diagnoses of these conditions, they undergo several investigations, which in turn detect incidental diseases including silent cancers—a form of “opportunistic surveillance”. This overestimation of the occurrence of cancer diagnosis concurrent with a new diagnosis of diabetes is well recognized [40]. These silent cancers might have a low-stage disease with generally good prognosis and account for the obesity paradox in overweight and obese patients. One approach to minimize detection bias is to adjust for tumor stage at presentation or alternatively where the date of diagnosis of, say, diabetes is known, use a washout of 2 years to “bypass” the detection bias.

Reverse causality refers to the phenomenon that some normal-weight patients may have previously been obese but lost weight due to illness, here cancer. Cancer is known to cause weight loss by loss of appetite or increased metabolic demands. The extent of weight loss correlates with initial BMI and occurs in patients with early-stage as well as late-stage tumors [41]. The potential causal link of reverse causality with the obesity paradox has been shown in several examples. Thus, Gelber and colleagues [42] evaluated the relationship between BMI and mortality in 99,253 male physicians in the Physicians’ Health Study and initially showed a U-shaped association with all-cause mortality, which converted to a linear relationship in their optimal model excluding men who died within 2 years of initial assessment. Similarly, Tseng [43] evaluated a nationally representative cohort of 89,056 Taiwanese patients with type 2 diabetes, matched with the National Death Certificate Database, and on initial analysis found that BMI was inversely associated with mortality from all-cause, cancer, and diabetes complications, but after excluding patients with a follow-up duration less than 2 years, BMI categories were not significantly prognostic for cancer-related mortality, suggesting a bias induced by cancer-induced weight loss.

Reverse causality is better explored and minimized by using longitudinal data to obtain a description of the patient’s usual weight and its trajectory up to cancer diagnosis. Weight histories (repeated weight measurements) give a useful dimension of obesity exposure, but there is a paucity of such data. Research to define obesity-equivalence of pack-years will be informative. A simpler approach when weight histories are not available is to include an individual’s maximum lifetime BMI and is robust to confounding by illness-induced weight loss. Stokes and Preston [37] have illustrated this approach demonstrating a reduction in biases when including maximum lifetime BMI into their models. This approach is similar to evaluating weight change, for example, the rate of change and size of variability over time [28, 44].

There are some examples where tumors among obese patients have less aggressive characteristics compared with those among normal-weight patients. In obese women with endometrial cancer, there is a predominance of good prognosis type 1 tumors compared with poor prognosis type 2 endometrial cancer. Tumors are molecularly heterogeneous, and it is speculated that obesity is associated with less aggressive biological subtypes. For renal carcinoma, obesity is associated with more indolent molecular variants (for example, reduced fatty acid synthase, FASN, gene expression) [12], while in contrast, for ovarian cancer, elevated BMI is associated with good prognosis cancers (low-grade serous and endometrioid), but within this histological type subpopulation, there is a linear positive association between BMI and mortality, which is absent in high-grade serous ovarian cancers [45].

The overweight and obese state might influence treatment outcomes, both in terms of how the tumor (changed for consistency) behaves to treatment and in terms of the differential pharmacokinetics of cancer treatment regimens. For example, high-intra-abdominal fat volume predicts for greater doxorubicin exposure and hematologic toxicities in women with breast cancer compared with body surface area [46]. Similarly, overweight and obese patients might be differentially allocated to less radical cancer surgery, though Gurunathan and Myles [47] point out the limitations of BMI as a predictor of peri-operative complication risk and indicate that mildly obese and overweight patients outperform normal-weight patients after many types of surgeries.

A specific mention is worthwhile for the complex inter-relationships between adjuvant chemotherapy (after curative resection) and the overweight/obese state. There is a well-recognized clinical practice among many oncologists to dose cap chemotherapy in obese patients with body surface area (BSA) greater than 2.0, and together with differential allocation and differential adherence to adjuvant chemotherapy, obese patients may simply have poorer outcomes compared with normal-weight patients because they are sub-optimally treated. This is illustrated by Sinicrope and colleagues [48], who examined the prognostic impact of BMI in 25,291 patients with stage II and III colon carcinoma within the Adjuvant Colon Cancer Endpoints (ACCENT) database, a consortium of randomized trials of 5-fluorouracil-based adjuvant chemotherapy. With disease-free survival (DFS) as a key outcome measure, compared with normal-weight patients, they showed a significant reduction in DFS limited to men with class 2 and 3 obesity (BMI ≥35.0 kg/m²) but an improved survival for overweight and class 1 obese (BMI 25.0 to 34.9 kg/m²) men, i.e., the obesity paradox. There were different dose-capping practices among the trials, and there was lack of data on chemotherapy adherence by BMI status, such that the study was unable to conclude whether or not these confounders contributed to the differential impact of BMI states on survival.

A third hypothesis is that excess adipose tissue serves as a nutrient reserve and confers a survival advantage in times of stress, such as anti-cancer treatment. This is akin to the hibernation theories in evolutional biology whereby species store up energy in anticipation of harsh times ahead. On a parallel note, it remains unclear if obesity drives cancer progression, whether it is due to excess adiposity or the energy imbalance [49].