Skeletal muscle is a critical and often unappreciated organ that not only supports human locomotion but its mass is also a robust predictor for all-cause mortality (Kallman et al., 1990; Metter et al., 2002). Furthermore, given that the human body is 45% skeletal muscle by mass, sustaining skeletal muscle mass throughout life is essential for promoting both athletic performance and longevity. Despite its importance, several of the physiological mechanisms that regulate the size of human muscle mass have only recently been elucidated, and many are still unknown. What is known is that the interaction between amino acid feeding-induced changes in rates of muscle protein synthesis (MPS) and rates of muscle protein breakdown (MPB) ultimately dictate net muscle protein balance (NPB) (Phillips et al., 1997). However, the composition, dose, timing, and daily distribution of protein intake (and subsequent effect on aminoacidemia) throughout the day that induces optimal MPS remains a topic of intense research and debate. Moreover, how these variables influence the cellular and molecular regulators that mediate amino acid-induced increases in MPS, particularly those involved in translation initiation and elongation, remain largely unknown. The aim of this chapter is to provide a critical evaluation of our current understanding of how amino acid ingestion, mainly in the form of intact protein sources, following loading (resistance exercise) influences MPS at both the cellular and molecular level. For the purposes of concision and relevance to the human model, data reported primarily derived from human studies will be cited but, where appropriate, work from other experimental models will be introduced to substantiate points of discussion.

The size of human skeletal muscle mass is dependent upon the coordinated interaction between changes in rates of MPS and MPB (Phillips et al., 1997). The basal and fasted state rates of MPB are known to exceed those of MPS and thus, skeletal muscle net protein balance (NPB=MPS minus MPB) is negative. Over two decades ago, using stable isotopic infusions, it was demonstrated that a mixed macronutrient meal was capable of increasing rates of MPS above rates of MPB and that the amino acids contained within the meal were primarily responsible for this increase (Bennet et al., 1990; Rennie et al., 1982). However, after approximately 2–3 h rates of MPS are known to decline to postabsorptive levels until the consumption of the next amino acid-containing meal (Areta et al., 2013; Atherton et al., 2010). Interestingly, performing exercise, particularly resistance exercise, prior to consuming amino acids has been shown to potentiate rates of MPS (Phillips et al., 2012; Witard et al., 2009). It is this potentiation by resistance exercise of feeding-induced increases in MPS that is responsible for the hypertrophic phenotype observed with resistance exercise training and protein feeding over time (Fig. 6.1). Importantly, not all amino acids exert the same stimulatory effect of MPS in skeletal muscle either at rest or following exercise, and identifying the relevant amino acids, optimal amino acid/protein dose and/or composition of amino acids to promote gains in muscle size and function is of great scientific interest.

While resistance exercise will remain the focus of this chapter it is important to recognize that even aerobic exercise can stimulate MPS (Carraro et al., 1990; Harber et al., 2010) and even result in protein accretion (Harber et al., 2009, 2012). However, the fraction of muscle proteins that are predominantly turned over in response to exercise is specific to the intensity and duration of the exercise bout, as well as the training status of the individual (Burd et al., 2010; Wilkinson et al., 2008). For example, in an untrained state, resistance exercise stimulates an increase in both myofibrillar and mitochondrial MPS; however, in the trained state, resistance exercise only stimulates an increase in myofibrillar MPS (Table 6.1). Endurance exercise on the other hand stimulates an increase in mitochondrial MPS in both the trained and untrained state, but does not result in a stimulation of myofibrillar MPS (Wilkinson et al., 2008). These differences are important considerations when evaluating the efficacy of a given exercise or nutritional stimulus to alter protein turnover as the assessment of mixed MPS can mask any potential protein fraction-specific differences in rates of synthesis (Kim et al., 2005). It is also known that high intensity intermittent exercise training (HIIT), a stimulus that could be considered a “hybrid” of both resistance and endurance exercise, has the capacity to stimulate both myofibrillar and mitochondrial MPS (Bell et al., 2015; Scalzo et al., 2014). Although ingestion of protein (and the subsequent aminoacidemia) is thought to influence the adaptive response to all modes of exercise, the effect is most profound following resistance exercise (Cermak et al., 2012, 2013). As a result, the continuing theme of this chapter will be how protein/amino acid feeding alters the protein synthetic response to resistance exercise with some discussion relating to the role of endurance and HIIT exercise.

A major independent variable that drives MPS is the digestion rate and subsequent aminoacidemia of ingested proteins. This factor can largely be influenced by the quality of intact proteins as defined by various scoring systems such as the Digestible Indispensible Amino Acid Score (for an expanded review see van Vliet et al., 2015). The most widely studied categories of dietary isolated protein are whey, casein and soy, all of which have differing digestion and absorption kinetics as well as amino acid composition. In this regard, isolated whey and soy proteins, since both are acid-soluble, are relatively rapidly digested resulting in a heightened but transient hyperaminoacidemia (Devries and Phillips, 2015). Soy protein however, contains a greater proportion of nonessential amino acids than whey protein (Mahe et al., 1996). Casein in its micellar form (as it exists in milk) is acid insoluble and coagulates in the stomach, which slows transit time into the intestine and thus results in an aminoacidemia that is smaller in amplitude but greater in duration than whey (Boirie et al., 1997).