American Journal of Respiratory Cell and Molecular Biology | 2021
You Are What You Eat: Diet-Dependent Changes in Pulmonary Surfactant
Abstract
Pulmonary surfactant is a complex mixture of phospholipids, proteins, and neutral lipids, including cholesterol, that is synthesized, secreted, and primarily recycled by alveolar type II (ATII) epithelial cells (1). Surfactant is essential to maintain normal lung function; by lowering the surface tension of the alveolar lining fluid, surfactant facilitates alveolar expansion on inspiration and prevents alveolar collapse at the end of expiration (2). In adults, abnormalities in surfactant composition and/or function are a key pathophysiologic feature of many pulmonary diseases, including pneumonia, acute respiratory distress syndrome (ARDS), asthma, chronic obstructive pulmonary disease, and pulmonary fibrosis (3). Interestingly, however, and for reasons that remain unclear, improving outcomes with surfactant replacement therapy in adults has proven to be more challenging (4). Synthesis of surfactant lipids and proteins clearly depends on the appropriate availability of nutrients. However, the effects of dietary changes on surfactant composition and function have not been investigated in depth. In their paper in this issue of the Journal, Schipke and colleagues (pp. 379–390) investigated the impact of feeding mice starch-rich, sucrose-rich, and fat-rich diets for 30 weeks relative to a standard fiber-rich diet (5). They found that the resulting hypercholesterolemia and hyperinsulinemia are associated with altered lung mechanics in mice fed sucroseor fatrich diets, although ex vivo surfactant function decreased only in the latter group. In line with these functional changes, surfactant phospholipid composition was significantly altered in all three treatment groups, although there were also clear differences in the predominant phospholipid species between mice fed highcarbohydrate diets and those fed excess fat. Finally, dietary modifications were associated with changes in gene expression in ATII cells and, in the case of mice fed a high-starch diet, alterations in ATII cell ultrastructure. The relative contribution of surfactant dysfunction to the alterations in lung mechanics is most clearly seen in the animals receiving the fat-rich diet, as demonstrated by significantly reduced surfactant adsorption, increased hysteresis, and altered pressure–volume curves. Notably, changes resulting from a sucrose-rich diet were very similar but insufficient to achieve significance regarding a decrease in adsorption. The corresponding compositional changes to surfactant lipids are highlighted by significant, but relatively small, changes in the proportion of saturated, monounsaturated, and polyunsaturated fatty acids. Although an overabundance of polyunsaturated fatty acids has been associated with reduced surface activity, the increased amounts in this model are unlikely to fully explain the observed functional changes in adsorption and lung mechanics; it has generally required significantly higher concentrations of polyunsaturated fatty acids, cholesterol, or lysophospholids to significantly affect surface tension–lowering activity (6, 7). Other changes in surfactant composition, such as total surfactant recovery, major phospholipid subclasses present (as a percentage of total lipids), cholesterol content, and proportions of other neutral lipids, can and likely will be explored in this model and potentially yield further insights. These observations may have some important experimental implications in mouse models of pulmonary disease. Although most researchers feed their study subjects standardized chow, many cardiovascular and cancer studies employ modified (often high-fat) diets, and this may be an additional experimental variable that needs to be borne in mind when interpreting changes in lung function in these animals (8, 9). More importantly, it is possible that surfactant function could be altered by changes in food intake associated with either incorporation of unpalatable chemicals in the chow or the onset of experimentally induced disease. For example, the inclusion of tamoxifen in the diet to induce gene knockout often results in initial inappetence, particularly in older mice (10). Likewise, mice with acute influenza pneumonia stop eating altogether (11); if the impact of dietary alterations on surfactant is rapid, this alone could account for some of the lung function abnormalities, such as reduced lung compliance, reported in infected mice. Indeed, it is possible that an acute change in diet could have a greater impact on surfactant lipids than a chronic change; the observed alterations in gene expression could reflect long-term adaptation to a modified diet. Hopefully, future studies will shed additional light on how changes in diet modify surfactant composition and function over time. The potential clinical implications of dietary intake leading to alterations in surfactant composition and function are clear. Although extreme for the sake of mechanistic clarity and analysis, the experimental diets used in these studies reflect dietary habits associated with the obesity crisis. Obesity is a well-established risk factor for common respiratory disorders associated with surfactant dysfunction, including ARDS and asthma (12, 13). During both the H1N1 influenza outbreak in 2009 and the currently ongoing pandemic from severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), the severity of ARDS and mortality among patients with obesity were significantly increased (12, 14). Altered surfactant as a principal mechanism leading to the increased susceptibility of this vulnerable population is plausible and provides a basis for considering obesity as a predictor for enriched responsiveness to surfactant replacement therapy in future clinical trials. The experiments described in this article also provide insights into the mechanisms underlying altered surfactant lipid metabolism