Effect of sodium bicarbonate and beta-alanine supplementation on maximal sprint swimming

During intensive anaerobic exercise with a large glycolytic component, one major cause of fatigue is believed to be acidosis caused by high levels of hydrogen ions (H⁺) in the muscle fibers. The increase in (H⁺) corresponds to a decrease in muscle and blood pH [1], can slow glycolysis [2], interfere with calcium release from the endoplasmic reticulum and calcium ion binding [3, 4], and increase the perception of fatigue after some types of exercises [5]. A number of buffers can be used by the body, but the primary method for buffering the H⁺ is thought to be either bicarbonate or hemoglobin [6]. For the past 35 years, several studies have investigated the use of sodium bicarbonate (SB) as an ergogenic aid. The participants have typically been men, and efficacy (improved performance and a decrease in H⁺ concentration after exercise) has generally been seen at doses of at least 0.3g· kg^-1 body mass [7‐9].

A recent meta-analysis by Carr et al. [10] suggests that ingestion of SB at 0.3 - 0.5g·kg^-1 body mass improves mean power by 1.7 ± 2.0% during high-intensity races of short duration (1–10 min). Timing of ingestion ranging from 60 min - 180 min before exercise did not influence buffering capacity or the ergogenic potential of SB (0.3g·kg^-1 body mass) as assessed by repeated sprint ability. However, visual analog scale scores indicated that at 180 minutes post-ingestion, an individual is less prone to experiencing significant gastrointestinal discomfort [11]. Gao et al. [3] and Siegler et al. [12] have demonstrated that swimmers ingesting 0.3g·kg^-1 body mass of SB can enhance blood buffering potential and positively influence interval swim performance. Lindh and colleagues [13] have also shown that SB supplementation (0.3g·kg^-1 body mass) can improve a single 200 m freestyle performance time in elite male competitors, most likely by increasing extra-cellular buffering capacity.

Beta-alanine (BA) is a non-essential amino acid that combines with L-histidine, to form the dipeptide carnosine. BA is thought to be the rate-limiting step in the synthesis of carnosine [14]. Carnosine acts as an intracellular buffer during high-intensity exercise [15‐18], and elevations in muscle carnosine concentration have been demonstrated to enhance cycling capacity [18], ventilatory threshold, and delay fatigue [19]. A recent meta-analysis [20] has shown a significant ergogenic effect of BA supplementation during high intensity exercise lasting 60–240 s in duration. However, the efficacy of BA supplementation during single exercise durations shorter than 60 s durations is not clear. Although the efficacy of BA on repeated sprint performance is not very well known, studies examining BA and resistance training performance have indicated significant increases in training volume [21, 22], suggesting that BA ingestion would be beneficial for repetitive high intensity exercise activities.

There appears to be only a limited number of studies that have examined a combination of two supplemental buffers on exercise performance. Mero and colleagues [23] indicated that the combined ingestion of SB and creatine (Cr) enhanced performance in two consecutive maximal effort 100-m swims with a 10 min recovery to a greater extent than ingestion of the supplements separately. Hoffman et al. [22] were the first to examine the combination of both BA and Cr supplements. Results of their study demonstrated that this combination significantly improved the training volume more than creatine alone. Specifically, improvements in training volume were found to be associated with significantly greater gains in lean body mass and decreases in fat mass. Sale et al. [24] investigated the effects of the combination of SB and BA (4 weeks loading) on high intensity cycling endurance performance and found that BA alone improved cycling capacity. Despite a 6 s improvement in time to exhaustion with the addition of SB, it did not reach statistical significance. In another cycling study [25] acute SB supplementation significantly improved 4-min cycling performance, but there seemed to be only a minimal additive effect of combined BA and SB supplementation. In the study by Hobson et al. [26] it was shown that both chronic BA and acute SB supplementation alone had positive effects on 2000 m rowing endurance performance. The addition of acute SB to chronic BA supplementation may further enhance rowing performance. Chronic BA and SB supplementation alone equally enhanced high-intensity intermittent maximal upper-body performance (4 × 30 s with three minutes recovery) in well-trained athletes and combining BA and SB promoted a clear additive ergogenic effect [27]. Ducker et al. [28] investigated if combining BA and SB could lead to enhanced repeated-sprint performance (3 sets; 6 × 20 m departing every 25 s, 4 minutes recovery between sets). They concluded that supplementation with acute SB improved repeated-sprint performance more than either a combination of SB and BA or BA alone. In a recent study [29] the swimmers swam maximally at first 200 m and then 100 m with 30 minutes recovery. BA and SB supplementation improved both 200 m and 100 m swimming performance. The co-ingestion of BA and SB induced a further nonsignificant improvement in performance. The performance time in 100 m was a little bit over 60 s (60–64 s). This time limit 60 s [20] is interesting in races e.g. in swimming (100 m) and in running (400 m). Earlier Sostaric et al. [30] reported that SB supplementation lowered circulating potassium, enhanced muscle potassium uptake and sodium delivery with alkalosis, but there are no studies with BA supplementation. These physiological changes are all interesting with preservation of membrane excitability during exercise [30]. Therefore, the purpose of present study was to examine more the effect of SB (extracellular buffer), BA (intracellular buffer) and the combination of SB with BA on a maximal sprint performance under 60 s in swimmers in a simulated competition.

Subjects reported no side effects related to SB intake, but symptoms of paraesthesia was experienced by all subjects consuming BA.

The results of this study indicate that there was a significant improvement in swimming time during the second 100 m swim trial following acute SB supplementation compared to PL, but the addition of chronic BA to acute SB did not provide any additional ergogenic benefit. Results indicate the efficacy of SB supplementation when performing maximal interval swimming lasting under 60 s but do not support any additional benefit of SB combined with BA.