Reflex swallowing vs. thirst-motivated drinking

One of the major differences in regulation of drinking between terrestrial and aquatic animals appears to be the presence or absence of a ‘thirst’ sensation (Takei, 2002). Mammals must feel thirsty to be motivated to seek water and to start a series of drinking behaviors that include searching for water, taking it into the mouth, and swallowing. Meanwhile, as water is always present in the mouth of fishes, they can freely drink water by reflex swallowing without the sensation of thirst. This idea originated from the fact that after removal of forebrain and midbrain, the eel responded to Ang II by drinking (Takei et al., 1979). Later, the site of action of Ang II was suggested to be the area postrema (AP), a circumventricular structure located in the caudal end of hindbrain (Mukuda et al., 2005). The circumventricular organs are highly vascularized tissues lacking a functional blood-brain barrier (BBB). Thus, they serve as a window for the brain to receive chemical information, such as hormones from blood. In fact, electric lesioning of the AP impaired Ang II-induced drinking (Nobata and Takei, 2011). These data strongly suggest that Ang II acts on the AP to induce reflex swallowing, and not thirst-motivated drinking behavior (Fig. 3A). In mammals, Ang II acts on the sensory circumventricular organs in the forebrain, the subfornical organ (SFO) and/ or organum vasculosum of the lamina terminalis (OVLT) to induce thirst (McKinley et al., 2003), and the lesioning of these areas abolished drinking behavior. Thus the cerebral mechanisms subserving drinking differ between terrestrial mammals and aquatic teleosts (Fig. 3A). Recently, however, we identified an OVLT-like structure without BBB in the eel forebrain (Mukuda et al., 2013). Thus, it is possible that teleosts also feel thirsty when Ang II acts there (Fig. 3A), but nevertheless they can drink by induced swallowing through the AP if the OVLT-like structure in the forebrain is removed. The cerebral mechanisms for regulation of drinking in fishes have been reviewed extensively (Takei and Balment, 2009; Nobata et al., 2013).

Inhibitory vs. stimulatory mechanisms

The mechanisms that regulate drinking have been an active target of research in mammals. Drinking is principally induced by three stimuli, cellular dehydration (increased plasma osmolality), extracellular dehydration (decreased blood volume), and increased plasma Ang II concentration (Fitzsimons, 1979, 1998; Takei, 2000) (Fig. 3B). Although all three stimuli induce vigorous drinking in mammals, cellular dehydration is the most potent stimulus for thirst, as the most copious drinking occurs after osmotic stimulus even though blood volume increases and plasma Ang II decreases simultaneously. In eels, however, osmotic stimulus inhibited drinking profoundly although plasma Ang II unexpectedly increased simultaneously (Takei et al., 1988) (Fig. 3B). Furthermore, Ang II induced only small and transient drinking in eels, which is followed by prolonged inhibition of drinking. Thus, overall, the amount of water intake was decreased for 15 min after Ang II injection. In teleosts, therefore, only extracellular dehydration is a reliable but weak stimulus for drinking (Takei, 2002).

Fig. 3.

Differences in regulatory mechanisms of drinking in mammals and teleosts. (A) The site of action of circulating hormones that influence drinking such as angiotensin II (Ang II) in the brain and the route that leads to drinking. In mammals, Ang II acts on the subfornical organ (SFO) and/or organum vasculosus of the lamina terminalis (OVLT) in the forebrain to induce thirst, which motivates a series of drinking behavior ended with swallowing. In teleosts, Ang II acts on the area postrema (AP) in the hindbrain to induce reflex swallowing, but the presence of OVLT-like structure is suggested recently (Mukuda et al., 2013). (B) Relative potency and efficacy of regulatory stimulus for drinking in mammals (Thirst) and teleosts (Swallowing). Obvious difference is the dominance of stimulatory mechanisms (+) in mammals and inhibitory mechanisms (-) in teleosts. ANP, atrial natriuretic peptide; BK, bradykinin.

The dominance of stimulatory mechanisms in mammals and inhibitory mechanisms in teleosts is also supported by the relative potency of regulatory hormones (Fig. 3B). In mammals, hormones that stimulate drinking are much more potent and efficacious than in teleosts. For instance, 100-fold higher doses are required for Ang II to elicit drinking in teleosts and the induced water intake is much smaller than that in mammals (Takei, 2002). In contrast, atrial natriuretic peptide (ANP) injected into the circulation of SW eels almost stopped drinking at low physiological doses that do not change arterial pressure, but ANP is only a weak antidipsogenic hormone in mammals even at much higher hypotensive doses (Takei and Hirose, 2002). Furthermore, many dipsogenic hormones have been identified in mammals, while most hormones that modulate drinking are antidipsogenic in eels (Takei, 2002; Kozaka et al., 2003). For instance, bradykinin is known as a dipsogenic hormone in mammals, but it is a potent antidipsogenic hormone in eels (Takei et al., 2001) (Fig. 3B). Thus, since antidipsogenic mechanisms are dominant in teleosts, dipsogenic mechanisms have developed in mammals, probably during the transition from aquatic to terrestrial life.

Absorptive mechanisms

Mammalian intestinal epithelia have two predominant types of cells, absorptive villus cells and secretory crypt cells (Giebel, 2005). However, the teleost intestine seems to lack secretory type cells. This idea originated from the observation that the teleost intestine does not have the crypt-like structures that characterize mammalian intestine (Loretz, 1987). In mammals, fluid secretion is thought to purge from the intestinal lumen harmful bacteria that produce toxins such as bacterial heat-stable enterotoxin (STa) that binds to a guanylyl cyclase-coupled receptor C (GC-C, guanylin receptor) with extremely high affinity, and induces acute bowel movement and Cl^-1 and water secretion into the lumen. However, STa does not bind eel GC-C with high affinity (Yuge et al., 2006), and thus secretory diarrhea may not occur in the eel after the bacterial infection to the intestine. In the intestine of killifish, Fundulus heteroclitus, however, immunohistochemical data suggest the possible presence of a small number of secretory-type enterocytes (Marshall et al., 2002).

There are differences in the mechanism of NaCI and water absorption between the intestines of mammals and marine teleosts. In mammals, NaCl in the luminal fluid is absorbed into the enterocytes via concerted action of Cl^-/ HCO3^- exchanger (SLC26A6) and Na⁺/H⁺ exchanger (NHE3 or SLC9A3) on the apical membrane (Kato and Romero, 2011), but it is mostly via Na⁺-K⁺-2CI^- co-transporter (NKCC2 or SLC12A1) in the marine teleost intestine (Ando, 1980; Musch et al., 1982; Takei and Loretz, 2011). In parallel with the ion absorption, water moves through a water channel (AQP1) into the cell. As the NKCC2 transports four ions (osmolytes) into the cell at a time, water absorption may be more efficient in marine teleosts than in mammals. Little is known about the relevant transporters for NaCI absorption in the intestine of FW teleosts, but mechanisms similar to those of mammals may be at work.

Hormonal regulation

In mammals, studies on hormonal regulation of water and NaCI absorption are rather scanty as most orallyingested water is obligatorily absorbed by the intestine in parallel with Na⁺-coupled nutrient transport (Kato and Romero, 2010). On the other hand, several circulating hormones and transmitters/modulators secreted from the innervating neurons regulate water and NaCI absorption by the intestine of marine teleosts. These studies showed that most of these chemical messengers, including acetylcholine, serotonin, histamine, ANP and vasoactive intestinal peptide, are inhibitory, and that no stimulatory regulators have been identified yet (Ando et al., 2003). Acetylcholine and serotonin seem to be released from the nerve terminals or from enterochromaffin cells of the intestine, since electrical field stimulation mimics the inhibitory effects of these neurotransmitters, which is blocked by the specific antagonists (Mori and Ando, 1991). Despite not being stimulatory when given alone, adrenaline, noradrenaline, dopamine, clonidine (α2-adrenoceptor agonist), somatostatin, and neuropeptide Y diminishes the inhibitory effect of acetylcholine and serotonin, with somatostatin being the most potent in this regard (Ando et al., 2003). It appears that chemical messengers that act on the Gs-coupled receptors and increase intracellular cAMP (or cGMP) inhibit water/NaCl absorption, but those that act on the Gi-coupled receptors and decrease intracellular cAMP restore the absorption.

All of these regulators act from the serosal side of intestinal epithelia. Guanylin is the only intestinal hormone that is secreted into the lumen and acts from the mucosal side. Guanylin was first discovered in mammals as an endogenous ligand for STa receptor (Currie et al., 1992). In the eel intestine, guanylin is produced in the goblet (mucus) cells (Yuge et al., 2003), and acts in a luminocrine fashion (Takei and Yuge, 2007). Guanylin is also a potent inhibitory hormone for NaCI/water absorption across the SW eel intestine (Yuge and Takei, 2007).

Aquatic vs. terrestrial habitat

The prototetrapods that moved onto the land were faced with two major challenges: gravity (or the loss of the natural buoyancy provided by the watery habitat) and desiccation. Concerning the gravity issue, they have developed circulatory systems with a powerful heart to pump out the blood throughout the body against gravitational force, resulting in high arterial pressures in mammals and birds. We found that hormones that increase blood pressure and cardiac performance, including Ang II, vasopressin/vasotocin, and endothelin, play critical roles in the circulatory system of these tetrapods (Takei et al., 2007). On the other hand, vasodepressor hormones such as natriuretic peptides, adrenomedullins, and vasoactive intestinal peptides are dominant and play important roles in cardiovascular regulation of fishes. Concerning the desiccation issue, mechanisms that induce thirst and antidiuresis have been strongly developed in mammals to increase the gain and decrease the loss of water as exemplified by potently dipsogenic Ang II and antidiuretic vasopressin. In teleost fishes, however, Ang II is an antidipsogenic hormone at high doses, and vasotocin has no effect on the kidney at low doses and pressure diuresis occurs at high doses (Takei and Loretz, 2005). In contrast to Ang II, ANP is a profound antidipsogenic hormone in teleost fish and its potency and efficacy were 2–3 orders of magnitude higher than those in mammals. This is also true for the effect on the intestine; ANP is a potent inhibitor for water and ion absorption in teleosts but the effect is negligible in mammals. On the renal effect, however, ANP is weakly natriuretic and antidiuretic in SW eels, suggesting that the common action of ANP in mammals and teleosts is to decrease NaCI from the body but not water (Takei and Hirose, 2002).

Incorporating all of the observations and experimental results available to date, the hormonal regulation of fluid balance can be distinguished between terrestrial mammals and aquatic teleosts, with water regulation further being distinguished between FW and SW teleosts. For instance, Ang II did not increase water intake, and ANP decreased water intake and intestinal water absorption in both FW and SW eels, although SW eels must increase these fluxes to cope with dehydration. Possible interpretation of the dominant inhibitory mechanisms in teleosts is as follows. As water is always in the mouth of teleosts, it enters the intestine only by swallowing. Therefore, they are faced with constant threat of excessive drinking in both FW and SW. Overdrinking in SW teleosts results in excessive increases in plasma osmolality as SW contains much higher concentration of NaCl than plasma. This situation is completely different from that in terrestrial animals, which must search for water motivated by thirst before drinking. This is an important difference between aquatic teleosts and terrestrial mammals, but not between teleosts in FW and SW.

Hydrating vs. dehydrating habitat

Both mammals and marine teleosts live in the dehydrating environments, so water acquisition and retention is essential for their survival. By contrast, FW fishes must protect against hypervolemia by reduction in drinking and production of copious dilute urine (Takei, 2000). There is a distinct difference in the need for water between FW teleosts and terrestrial/marine animals. However, the regulatory mechanisms for water acquisition in the latter groups are clearly different between mammals and SW teleosts, as discussed above. More important difference may be in ion regulation; mammals need to ingest NaCI from the environment but marine teleosts must limit and reduce NaCI accumulation to maintain ion balance. Therefore, a possible interpretation for the dominance of inhibitory mechanisms for drinking and intestinal absorption in marine teleosts is to limit excess ion uptake from the environment. As described above, in order to obtain water from SW, more NaCI must be absorbed than water in view of the relative NaCI concentration between teleost plasma and SW. Thus, plasma NaCI concentration certainly increases after drinking SW. This result coincides well with the inhibitory effect of osmotic stimulus on drinking in teleost fishes (Takei, 2002). It seems therefore that the primary goal of body fluid regulation in teleosts may not be to maintain plasma volume but, instead, to maintain plasma osmolality within a narrow range. This is also true in mammals and other terrestrial species (Takei, 2000).

Finally, in closing, what are the consequences of mammals drinking SW? As AQPs are abundant in the digestive tract, in most mammals imbibed SW is diluted by osmotic efflux of water into the lumen, which decreased plasma volume. Water is absorbed together with Na⁺ and Cl^-1 after dilution, but because SW contains high concentrations of divalent ions that are scarcely absorbed by the intestine, most of imbibed volume will be eliminated as diarrhea. Moreover, the mammalian kidney is not capable of concentrating urine above SW as is gill ionocytes of teleosts, which further facilitate the loss of water as urine. By contrast, as discussed herein, the intestine of SW teleosts can absorb more than 80% of imbibed SW, and the excess NaCI that enters the body is adequately excreted by gill ionocytes. Despite the presence of machinery for water acquisition in marine teleosts, it is interesting to note that inhibitory mechanisms are dominant at both drinking and intestinal absorption.