Early claims for oligopeptide absorption

A number of articles commonly cited as being evidential of oligopeptide absorption arose before the discovery of the PepT1 H⁺/peptide co-transporter. Agar et al. ⁽ Reference Agar, Hird and Sidhu ^{74 )} demonstrated unequivocally the transmural transport of unhydrolysed dipeptides, such as glycyl–glycine, an observation soon confirmed by other researchers⁽ Reference Newey and Smyth ^{11 ,} Reference Wiggans and Johnston ^{75 )}. Hueckel & Rogers⁽ Reference Hueckel and Rogers ^{76 )} reported an increase in bound hydroxyproline-containing dipeptides but not of free hydroxyproline in the urine of human subjects fed 30 g of gelatin, indicating that these peptides were absorbed intact before being excreted during the succeeding 5·5 h. Interestingly when the same experiment was repeated with rats both bound and free hydroxyproline was present in the urine when the diet contained gelatin. However, in monkeys and dogs the quantities of free and bound urinary hydroxyproline were the same whether the animals ingested a normal diet or one containing gelatin. This discordant result demonstrates that the choice of a human analogue is critical in physiological research. Hellier et al. ⁽ Reference Hellier, Holdsworth and McColl ^{77 )} reported the intestinal absorption of two dipeptides, glycyl-glycine and glycyl-l-alanine, in human subjects and noted that the constituent amino acids were absorbed faster when presented as dipeptides rather than as free amino acids. However, a third dipeptide, glycyl-l-lysine, known to be transported intact from the intestinal lumen, was hydrolysed to its constituent amino acids before reaching the portal venous blood, emphasising that the fate of dipeptides is not always the same. Later, Boullin et al. ⁽ Reference Boullin, Crampton and Heading ^{78 )} reported the absorption of six different dipeptides in the rat. The intact dipeptides were subsequently detected by ion-exchange chromatography in blood samples taken from the superior mesenteric vein.

The early work of Adibi⁽ Reference Adibi ^{79 )} and Silk et al. ⁽ Reference Silk, Perrett and Webb ^{80 )} suggests that not all tripeptides in humans are hydrolysed within the lumen or at the BBM, and that some of the possible 8000 tripeptides produced during the digestion of dietary protein may be absorbed intact. Compelling evidence for the absorption of intact peptides by the gut in humans comes from individuals with genetic disorders involving amino acid transporters; these patients do not appear to suffer from protein malnourishment as the absorption of intact peptides is unaffected⁽ Reference Hellier, Holdsworth and Perrett ^{81 –} Reference Tarlow, Thomas and Seakins ^{84 )}. Whether tetrapeptides can be absorbed by the enterocytes of the human jejunum was studied by Adibi & Morse⁽ Reference Adibi and Morse ^{85 )}. They determined that tetraglycine was not absorbed by the enterocytes by the same mechanism as tri- or diglycine and although they did not discount the absorption of the tetrapeptide they could not detect any tetraglycine within the mucosal cells⁽ Reference Adibi and Morse ^{85 )}. They have suggested that tetraglycine is hydrolysed by mucosal-bound oligopeptidases and the uptake of homologous glycine oligopeptides by the human mucosal epithelium is restricted to diglycine and triglycine. In vivo studies in animals offer only conflicting evidence for the absorption of tetrapeptides. In the rat, Chung et al. ⁽ Reference Chung, Silk and Kim ^{86 )} reported that l-leucyl-triglycine may be absorbed intact before being hydrolysed by cytoplasmic peptidases. On the other hand, a study by Burston et al. ⁽ Reference Burston, Taylor and Matthews ^{87 )} using rings of everted rat and hamster jejunum indicated that intact tetrapeptides were not absorbed but were hydrolysed to tri- and dipeptides by brush-border peptidases before uptake. The absorption of tetrapeptides by passive or facilitated diffusion has been reported by several researchers⁽ Reference Addison, Burston and Payne ^{88 –} Reference Matthews and Payne ^{90 )}. Both Chung et al. ⁽ Reference Chung, Silk and Kim ^{86 )} and Rogers et al. ⁽ Reference Rogers, Heading and Wilkinson ^{91 )} reported that rat small intestine could actively absorb intact tetrapeptides⁽ Reference Chung, Silk and Kim ^{86 ,} Reference Rogers, Heading and Wilkinson ^{91 )}; however, Kerchner & Geary⁽ Reference Kerchner and Geary ^{89 )} were critical of Chung's experimental approach, citing extensive incubation times and the reuse of perfusion jejunum loops, with no correction for substrate entrapped in the extracellular space, insufficient evaluation of the cytoplasmic peptidase activity and the estimation of intact tetrapeptide uptake by an indirect method. They suggest that the unprotected peptides used were rapidly hydrolysed to their amino acid residues by brush-border and cytosol enzymes. With extensive incubation times in an ileum-everted sac preparation coupled with such a very high substrate concentration (20 mm) this investigation would have been unable to determine whether the passage of peptide was active or passive. Kerchner & Geary⁽ Reference Kerchner and Geary ^{89 )} suggest that neither of these studies conclusively demonstrates the presence of an active transport process for oligopeptides.

Evidence for the absorption of larger peptides has been reported for: the pentapeptide metkephamid in the rat⁽ Reference Langguth, Bohner and Biber ^{92 )}; the orally active cyclic octapeptide analogue of somatostatin, octreotide, in the rat⁽ Reference Fricker, Bruns and Munzer ^{93 )}; the renin-inhibiting nonapeptide in the rabbit jejunum⁽ Reference Takaori, Burton and Donowitz ^{94 )}; the nonapeptide vasopressin also in the rabbit⁽ Reference Lundin and Vilhardt ^{95 )}; and in vivo, the decapeptide luteinising hormone-releasing factor⁽ Reference Amoss, Rivier and Guillemin ^{96 )}. Another large peptide that is absorbed via passive diffusion into enterocytes in humans is the orally active immunosuppressive endecapeptide, cyclosporin A⁽ Reference Ptachcinski, Burckart and Venkataramanan ^{97 ,} Reference Drewe, Meier and Vonderscher ^{98 )}. This large peptide is reported as having absolute bioavailabilities between < 5 and 89 %. Using ultrastructural imaging, horseradish peroxidase (HRP; 40 kDa) has been shown to be absorbed across the intestinal wall of the rat via transcytotic vesicles⁽ Reference Walker, Cornell and Davenport ^{99 )}. However, in Ussing chamber experiments the rate of membrane permeation across rabbit jejunum was found to be extremely low (3 pmol/h per cm²)⁽ Reference Heyman, Ducroc and Desjeux ^{100 )}. M-cells in the Peyer's patches of the ileum can transport macromolecules such as lectins or IgA⁽ Reference Neutra, Phillips and Mayer ^{101 ,} Reference Weltzin, Luciajandris and Michetti ^{102 )} although the concentration of proteins reaching the systemic circulation is considered to be very low⁽ Reference Keljo and Hamilton ^{103 )}.

Hemmings et al. ⁽ Reference Hemmings, Hemmings and Patey ^{104 )} reported that the large molecular mass breakdown products of four iodinated proteins were absorbed into the circulation and tissues of orally fed adult rats. In this paper the molecular mass of the breakdown products was not given and the issue of whether the irradiated iodine remains with the protein or if it is transferred to protein synthesised de novo could not be assured. However, in a later study⁽ Reference Hemmings and Williams ^{105 )} these questions were addressed. The molecular mass of the irradiated breakdown products ranged between 20 and 50 kDa and their origin was confirmed immunologically using antisera specific to the original molecule. Using ³H-labelled bovine IgG the authors detected the presence of this large protein, or of fragments sufficient in size to retain the markers in adult ileal epithelial cells by direct deposition autoradiography at the electron microscopic level⁽ Reference Hemmings and Williams ^{106 )}. They suggest there may be a universal necessity for body cells to be permeable to proteins of many types and there is a constant traffic of protein molecules into all body cells. The method by which the human gut might absorb such large protein fragments is unclear although the transcytosis of IgG in the neonatal rat has been reported⁽ Reference Jones and Waldmann ^{107 ,} Reference Mostov ^{108 )} and an increased permeability of tight junctions may permit the passage of larger peptides. Bloch et al. ⁽ Reference Bloch, Wright and Bishara ^{109 )} demonstrated that ¹²⁵I-labelled polypeptide fragments (6–20 kDa) from a pepsin digestion of bovine serum albumin were transferred from the mucosal to the serosal surface of the enterocytes when infused into everted jejunual gut sacs of rats. In subsequent in vivo studies they found that nanogram amounts of unlabelled immunoreactive fragments were detected by RIA of mesenteric and portal venous blood following their infusion into the jejunum. However, they failed to detect such fragments in the systemic circulation and suggest that this must be due to their rapid clearance. Caution is required in the interpretation of these results owing to the direct infusion of the jejunum circumventing hydrolysis by gastric and intestinal peptidases, the small and nutritionally insignificant amounts of the polypeptides detected in the portal and mesenteric venous blood and the short half-life of such fragments in the systemic circulation. On balance it would appear that small quantities of di- and tripeptides are absorbed from the adult human digestive tract, but the evidence for the absorption of larger peptides in other than very small amounts is not strong.

The lactotripeptides isoleucine–proline–proline and valine–proline–proline

Some of the most extensively studied food-derived bioactive peptides are those with potential antihypertensive properties and in particular those that may inhibit the angiotensin-converting enzymes (ACE)⁽ Reference Foltz, Cerstiaens and van Meensel ^{117 )}. Séverin & Xia⁽ Reference Séverin and Xia ^{118 )} reported that two lactotripeptides (valine–proline–proline (VPP) and isoleucine–proline–proline (IPP)) from milk were able to cross the intestinal barrier and, post-absorption, inhibit the production of angiotensin II (AngII) in the bloodstream. They caution that not all bioactive peptides may be so absorbed:

…in order to function physiologically in the human body, the active peptides must be absorbed from the intestine in an active form. Di- and tripeptides can be easily absorbed in the intestine; however, it is not clear that larger bioactive peptides containing in excess of three amino acids are absorbed from the intestine and reach the target organ. Most of the claimed physiological properties of the casein-based bioactive peptides have been carried out in vitro or in animal model systems and these hypothesized properties remain to be proven in humans.

The key point of this cautionary note is that bioactive peptides must be absorbed in an active form, a point central to the debate as to whether orally ingested foods can exert physiological changes systemically post-absorption or not.

The research of Nakamura et al. ⁽ Reference Nakamura, Yamamoto and Sakai ^{119 )} is often quoted as demonstrating that ingestion of ‘Calpis’, a Japanese sour milk, or a preparation of the pure tripeptides (VPP and IPP), decreased the systolic blood pressure in spontaneously hypertensive rats (SHR), 6–8 h after oral administration⁽ Reference Vermeirssen, Van Camp and Verstraete ^{20 ,} Reference Haque, Chand and Kapila ^{35 ,} Reference Korhonen and Pihlanto ^{57 ,} Reference Erdmann, Cheung and Schroder ^{116 ,} Reference Séverin and Xia ^{118 ,} Reference Robert, Razaname and Mutter ^{120 –} Reference Escudero, Sentandreu and Arihara ^{126 )}. However, Nakamura et al. ⁽ Reference Nakamura, Yamamoto and Sakai ^{119 )} and others⁽ Reference Miguel, Muguerza and Sanchez ^{122 ,} Reference Muguerza, Ramos and Sanchez ^{127 )} also showed that the Calpis sour milk and mixed tripeptides did not change the systolic blood pressure of the normotensive strain of Wistar–Kyoto rats, important data that many of the researchers citing this paper have not mentioned⁽ Reference Haque, Chand and Kapila ^{35 ,} Reference Korhonen and Pihlanto ^{57 ,} Reference Erdmann, Cheung and Schroder ^{116 ,} Reference Séverin and Xia ^{118 ,} Reference Escudero, Sentandreu and Arihara ^{126 )}. Interestingly, at the conclusion of their 2009 study, Nakamura et al. ⁽ Reference Nakamura, Mizutani and Sasaki ^{128 )} state that it has been determined consistently that in Japanese populations the blood pressure response to the lactotripeptides is much greater than that in other populations, although it is unclear why this is so. It should be emphasised that unlike in their earlier 1995 study⁽ Reference Nakamura, Yamamoto and Sakai ^{119 )} using rats, in this study of human subjects Nakamura et al. ⁽ Reference Nakamura, Mizutani and Sasaki ^{128 )} did not use normotensive subjects or a placebo control with which to compare their data.

Nakamura et al. ⁽ Reference Nakamura, Mizutani and Sasaki ^{128 )} and others have reported that the two lactotripeptides VPP and IPP have been shown to have significant blood pressure-lowering activity⁽ Reference Nakamura, Yamamoto and Sakai ^{119 ,} Reference Mizuno, Matsuura and Gotou ^{123 ,} Reference Hata, Yamamoto and Ohni ^{129 –} Reference Boelsma and Kloek ^{134 )}. They consider that both VPP and IPP are absorbed into the bloodstream and into the cells of the aorta after oral administration and inhibit ACE activity in vascular endothelial cells⁽ Reference Nakamura, Mizutani and Sasaki ^{128 ,} Reference Masuda, Nakamura and Takano ^{135 )}. The 2009 study by Nakamura et al. of human subjects was small (n 12) and not placebo-controlled. In their earlier study, Nakamura and colleagues⁽ Reference Masuda, Nakamura and Takano ^{135 )} suggested that the two lactotripeptides could be transported intact through the intestinal wall via paracellular routes. However, the molecular mass of the lactotripeptides is over 300 Da and, as Lennernäs⁽ Reference Lennernäs ^{66 )} conjectures, compounds with a molecular mass greater than 200 Da are too large for the intercellular space between the enterocytes and that absorption via paracellular transport is unlikely. The latter hypothesis was corroborated by observations that small hydrophilic molecules (for example, creatinine 113 Da) were affected by solvent drag and transported via the paracellular route, whereas larger hydrophilic molecules such as d-glucose (180 Da) and l-DOPA (l-3,4-dihydroxyphenylalanine) (197 Da) were not⁽ Reference Nilsson, Fagerholm and Lennernas ^{136 –} Reference Fagerholm, Nilsson and Knutson ^{138 )}.

In an in vitro study using monolayer-cultured human intestinal Caco-2 cells, Satake et al. ⁽ Reference Satake, Enjoh and Nakamura ^{139 )} also suggested that lactotripeptides were transported across the cells via the paracellular route. They suggest that because the passage of VPP across the Caco-2 cell monolayers was only weakly inhibited by the addition of a competitive substrate, that the PepT1 peptide transporter was not the major pathway. They also reported that no intact VPP was detected in the Caco-2 cells, suggesting that any peptides entering the cells were rapidly hydrolysed by cytosolic peptidases. As the lactotripeptides are only weakly hydrophobic, absorptive transcytosis could also be discounted as a major transport mechanism⁽ Reference Camenisch, Alsenz and van de Waterbeemd ^{140 )}. Likewise, Camenisch et al. ⁽ Reference Camenisch, Alsenz and van de Waterbeemd ^{140 )} predicted that lactotripeptides would not be expected to penetrate Caco-2 cells via transcellular passive diffusion. With little or no evidence that lactotripeptides are absorbed via the PepT1 transporter suggests that this pathway may not be open to all di- and tripeptides. Therefore the belief that the transporter can essentially transport all di- and tripeptides⁽ Reference Daniel ^{21 ,} Reference Adibi ^{23 ,} Reference Rubio-Aliaga and Daniel ^{24 ,} Reference Daniel and Herget ^{141 )} may require amendment. To this end, Brandsch et al. ⁽ Reference Brandsch, Knutter and Bosse-Doenecke ^{142 )} have reported that the PepT1 transporter can accept most but not all proteinogenic di- and tripeptides as substrates.

Mizuno et al. ⁽ Reference Mizuno, Matsuura and Gotou ^{123 )}, experimenting with human volunteers, administered the two peptides orally, in tablet form, at four different dose rates. They found that the reduction in systolic blood pressure was dose-dependent and most effective in mildly hypertensive subjects. However, they also found that there was no statistically significant reduction in diastolic blood pressure among their test groups or in comparison with the control group who received a placebo. If such an antihypertensive effect can be sustained, then it may be mediated through receptors on the intestinal wall⁽ Reference Korhonen and Pihlanto ^{57 ,} Reference Picariello, Ferranti and Fierro ^{143 )}.

A study in the pig by van der Pijl et al. ⁽ Reference van der Pijl, Kies and Ten Have ^{144 )} highlighted that efficacy studies usually present end-point measurements (for example, blood pressure), but hardly ever report plasma concentrations of the bioactive peptides involved. They found no data in the literature pertaining to the absolute bioavailability or other pharmacokinetic/pharmacodynamic properties of the lactotripeptides. With respect to the pharmacokinetics of three proline-rich tripeptides (VPP, IPP and leucine–proline–proline) van der Pijl et al. ⁽ Reference van der Pijl, Kies and Ten Have ^{144 )} went to extraordinary lengths to determine the very low concentration of these intact peptides in the bloodstream following intragastric infusion. Using liquid chromatography/MS they found the absolute bioavailability of the three peptides to be approximately 0.1 %. In one experiment the half-lives of absorption and elimination for VPP and IPP following intragastric dosing (4 mg of each lactotripeptide per kg body weight dissolved in 40 ml of iso-osmolar saline) were determined by van der Pijl et al. ⁽ Reference van der Pijl, Kies and Ten Have ^{144 )} to be 12 ± 6 and 9 ± 1 min, respectively. This suggested that the low absorption of these peptides was due to peptidase activity in the lumen, BBM and cytosol. With the effective plasma concentration for the inhibition of ACE being estimated by van Platerink et al. ⁽ Reference van Platerink, Janssen and Haverkamp ^{145 )} to be 5·6 μmol, the plasma concentrations determined by van der Pijl et al. ⁽ Reference van der Pijl, Kies and Ten Have ^{144 )} were approximately 1000-fold less and far below the effective concentration required to have any influence on lowering blood pressure. The pharmacokinetic properties of the tripeptides tested make it unlikely that physiological effects, such as a reduction in blood pressure, are the result of prolonged high plasma peptide concentrations.

In human subjects, following an oral dose of lactotripeptide in enriched yoghurt (250 ml containing approximately 20 mg of both IPP and VPP), Foltz et al. ⁽ Reference Foltz, Meynen and Bianco ^{125 )} determined the maximal plasma concentration of IPP to be less than 1 pmol/ml and concluded this to be far below its effective concentration for ACE inhibition determined in vitro. The required plasma concentration of the lactotripeptides known to exert ACE inhibition are approximately 1000-fold higher than reported plasma concentrations in animal or human trials⁽ Reference Foltz, Meynen and Bianco ^{125 )}.

Despite these results demonstrating a low bioavailability for the peptides leading to plasma concentrations below the effective concentration for ACE inhibition⁽ Reference Foltz, Meynen and Bianco ^{125 ,} Reference van der Pijl, Kies and Ten Have ^{144 )}, many researchers continue to report that lactotripeptides are absorbed in physiologically meaningful amounts (for reviews, see Korhonen⁽ Reference Korhonen ^{146 )} and Ricci et al. ⁽ Reference Ricci, Artacho and Olalla ^{147 )}).

Both Fitzgerald et al. ⁽ Reference Fitzgerald, Murray and Walsh ^{148 )} and Foltz et al. ⁽ Reference Foltz, Meynen and Bianco ^{125 )} report that previously studied ACE-inhibitory bioactive peptides failed to lower blood pressure in in vivo studies, highlighting the intestinal breakdown of the so-called stable proline-rich tripeptides⁽ Reference Vermeirssen, Van Camp and Verstraete ^{20 ,} Reference Matsufuji, Matsui and Seki ^{149 )}. Only a few of the great number of the milk peptides that have been identified as having antihypertensive properties in in vitro experiments have so far been proven to be clinically effective in vivo, in either animal or human studies⁽ Reference Vermeirssen, Van Camp and Verstraete ^{20 ,} Reference Fitzgerald, Murray and Walsh ^{148 ,} Reference Yamamoto, Ejiri and Mizuno ^{150 –} Reference Gobbetti, Minervini and Rizzello ^{152 )}.

Having studied the lactotripeptides in detail⁽ Reference Foltz, Cerstiaens and van Meensel ^{117 ,} Reference Foltz, Meynen and Bianco ^{125 ,} Reference van der Pijl, Kies and Ten Have ^{144 )}, Foltz et al. ⁽ Reference Foltz, van der Pijl and Duchateau ^{30 ,} Reference Foltz, Meynen and Bianco ^{125 )} and van der Pijl et al. ⁽ Reference van der Pijl, Kies and Ten Have ^{144 )} stated that although these peptides possess high proteolytic stability their bioavailability in pigs is less than 0·1 %, with a very low elimination half-life. In humans the maximal plasma concentration was no greater than high picomolar concentrations⁽ Reference Foltz, van der Pijl and Duchateau ^{30 )}. Foltz et al. ⁽ Reference Foltz, van der Pijl and Duchateau ^{30 )} argue that there is no scientific evidence that any other dietary peptides have better absorption than the lactotripeptides or plasma clearance profiles that could result in acceptable bioavailability or transiently high, free plasma concentrations.

A very low bioavailability for the dipeptide valine–tyrosine (VY), extracted from sardine muscle, was observed in a study by Matsui et al. ⁽ Reference Matsui, Tamaya and Seki ^{153 )}. From a maximal oral dose of 12 mg dissolved in 100 ml of water the highest plasma concentration of VY was determined to be 1·9 pmol/ml (equivalent to 532 pg/ml), 2 h after its administration. Although the plasma peptide concentration increased post-ingestion it did so in a non-linear dose-dependent manner. The maximum plasma concentration was determined to be 1/300 of the IC₅₀ (half-maximal inhibitory concentration) for VY. They did not find any statistically significant differences in blood pressure or blood chemistry between VY and the control groups in normotensive subjects. Matsui et al. ⁽ Reference Matsui, Tamaya and Seki ^{153 )} concluded that this very low degree of absorption was the result of hydrolysis from membrane-bound peptidases. They considered that alternatively VY was absorbed intact into the circulatory system and then rapidly accumulated in organs such as the aorta and kidney, resulting in a low and slow release of VY into the blood.

Other bioactive peptides present in milk

Milk, in particular, is known to be a rich source of bioactive peptides. The physiological properties and structural composition of the many milk-derived bioactive peptides have been comprehensively reviewed⁽ Reference Meisel ^{52 ,} Reference Clare and Swaisgood ^{154 –} Reference Meisel ^{157 )} and many of the effects of such bioactive peptides contained within milk proteins, both bovine and human, are listed in Table 1. Such bioactive components of milk are encrypted within the major milk protein precursors and are released during the digestive process by enzymic proteolysis. A recent paper by Martínez-Maqueda et al. ⁽ Reference Martínez-Maqueda, Miralles and Recio ^{158 )} lists 134 different peptides with antihypertensive properties derived from a variety of plant and animal proteins, including forty-nine derived from milk. The principal mechanism of action for peptides with antihypertensive effects, as discussed above, is the inhibition of angiotensin-I-converting enzyme (ACE). ACE is a constituent enzyme of the renin–angiotensin system (RAS), a mechanism that plays a crucial role in the regulation of blood pressure together with fluid and electrolyte balance⁽ Reference Fitzgerald and Meisel ^{159 )}. Although the blood pressure-lowering capability of the peptides described by Martínez-Maqueda et al. ⁽ Reference Martínez-Maqueda, Miralles and Recio ^{158 )} was reported as having been demonstrated in in vivo assays involving animal models (for example, SHR and humans), the different mechanisms of action that contribute to their antihypertensive effect still require further investigation. The absorption of ACE-inhibiting peptides in humans was reported by Martínez-Maqueda et al. ⁽ Reference Martínez-Maqueda, Miralles and Recio ^{158 )} for the peptide histidine–leucine–proline–leucine–proline (HLPLP), just one of seventeen small ACE-inhibitory peptides studied by van Platerink et al. ⁽ Reference van Platerink, Janssen and Horsten ^{160 )}. An alternative to absorption suggested by Martínez-Maqueda et al. ⁽ Reference Martínez-Maqueda, Miralles and Recio ^{158 )} involves the action of small peptides on opioid receptors present in the gut wall. A large number of studies have focused on the opioid properties that many of these peptides exhibit and the physiological effects that these molecules might have (see Table 2). Dietary exogenous opioid molecules have been termed exorphins⁽ Reference Klee, Zioudrou and Streaty ^{161 )} and as well as being in milk they have been found in a variety of other proteinaceous staple foods including gluten in cereals⁽ Reference Fukudome and Yoshikawa ^{162 ,} Reference Fanciulli, Dettori and Demontis ^{163 )} and Hb in meat⁽ Reference Ivanov, Karelin and Philippova ^{164 ,} Reference Zhao, Garreau and Sannier ^{165 )}. From as early as 1979⁽ Reference Brantl, Teschemacher and Henschen ^{166 ,} Reference Zioudrou, Streaty and Klee ^{167 )}, many of the bioactive peptides derived from milk, and casein in particular, have been demonstrated to have opioid properties such as those described in Table 2. Although exorphins may not be absorbed intact, their physiological influence resulting from their interaction with opioid receptors in the GIT is in little doubt. Several studies report that small opiate-acting peptides released during digestion by proteolytic hydrolysis can affect intestinal function⁽ Reference Teschemacher ^{168 –} Reference Meisel and Fitzgerald ^{170 )}.

Table 1

Examples of bioactive peptides derived from bovine milk proteins

ACE, angiotensin-converting enzyme; S*, phosphoserin.

† One-letter amino acid codes were used.

‡ Lactoferrin is a neutrophil-derived glycoprotein found in secreted mammalian fluids⁽ Reference Meisel and Fitzgerald ^{170 )}.

Table 2

Exorphins: peptides derived from milk having opioid properties

* Represents opioid activity with low potency.

† Schulte-Frohlinde et al. ⁽ Reference Schulte-Frohlinde, Schimd, Brantl, Brantl and Teschemacher ^{183 )}, Teschemacher et al. ⁽ Reference Teschemacher, Koch, Brantl, Brantl and Teschemacher ^{178 )}, Froetschel⁽ Reference Froetschel ^{184 )} and Allescher et al. ⁽ Reference Allescher, Storr and Brechmann ^{185 )}.

‡ Brandsch et al. ⁽ Reference Brandsch, Brust, Neubert, Brantl and Teschemacher ^{186 )}.

§ Daniel et al. ⁽ Reference Daniel, Vohwinkel and Rehner ^{187 )}.

∥ Matthies et al. ⁽ Reference Matthies, Stark and Hartrodt ^{188 )} and Taira et al. ⁽ Reference Taira, Hilakivi and Aalto ^{189 )}.

¶ Taira et al. ⁽ Reference Taira, Hilakivi and Aalto ^{189 )}.

** Represents low affinity to this receptor.

†† Yoshikawa et al. ⁽ Reference Yoshikawa, Tani, Shiota, Brantl and Teschemacher ^{192 )}.

The existence of three opioid receptors (μ, δ and κ) was described simultaneously by three different groups of researchers in 1973⁽ Reference Simon, Hiller and Edelman ^{171 –} Reference Terenius ^{173 )} and have been exhaustively reviewed in the Handbook of Experimental Pharmacology ⁽ Reference Mansour and Watson ^{174 )}. It is supposed that the μ, δ and κ opioid receptors belong to the G-protein-coupled receptor family and have seven transmembrane helices which are characteristic of the group⁽ Reference Satoh and Minami ^{175 )}. All three of these receptors have been detected in the small intestine and are located in the myenteric plexus⁽ Reference Nishimura, Buchan and McIntosh ^{176 ,} Reference Karras and North ^{177 )}.

Opioid receptor ligands are classified into two groups ‘typical’ and ‘atypical’ designated by Teschemacher et al. ⁽ Reference Teschemacher, Koch, Brantl, Brantl and Teschemacher ^{178 )}. The ‘typical’ peptides all originate from three endogenous precursor proteins pro-opiomelanocortin (endorphins), pro-enkephalin (enkephalins) and pro-dynorphin (dynorphins)⁽ Reference Höllt ^{179 )}. All the typical opioid peptides share the same N-terminal amino acid sequence, YGGF. Although they can bind to more than one type of receptor, they usually have a greater affinity for just one, dynorphins for κ-receptors, the enkephalins for δ-receptors and the endorphins for μ-, δ- and ε-receptors⁽ Reference Paterson, Robson and Kosterlitz ^{180 )}. The ‘atypical’ receptor ligands originate from a variety of precursor proteins either endogenous or exogenous and, although their N-terminal amino acid sequence may vary, they all have a terminal tyrosine residue in common (all except opioid receptor ligands that originate from α-casein) and another aromatic amino acid residue, such as tyrosine or phenylalanine, in the third or fourth position. The biological activity of these peptides is dependent upon the terminal tyrosine residue, as its absence eliminates all bioactivity⁽ Reference Chang, Killian and Hazum ^{181 )}. A proline residue at position 2 also appears to be necessary for the correct orientation of the peptide when it binds to the opioid receptor⁽ Reference Mierke, Nossner and Schiller ^{182 )}. Opioid antagonists have much in common with the ‘atypical’ agonists though they do not usually have a similar N-terminal amino acid sequence. The antagonistic potency of naturally occurring milk-borne peptides is relatively low though some synthetic derivatives have very high potency and receptor selectivity. The synthetic alkaloid agonists naloxone and naltrexone are often used in opioid peptide research as inhibitory confirmation of the presence of an agonistic opioid receptor ligand.

Of the forty-nine antihypertensive peptides derived from milk listed by Martínez-Maqueda et al. ⁽ Reference Martínez-Maqueda, Miralles and Recio ^{158 )}, five have amino acid motifs of reported opioid agonists⁽ Reference Teschemacher, Koch, Brantl, Brantl and Teschemacher ^{178 ,} Reference Schulte-Frohlinde, Schimd, Brantl, Brantl and Teschemacher ^{183 –} Reference Taira, Hilakivi and Aalto ^{189 )}. These opioid peptides might lower blood pressure through receptors expressed within the gut wall to bring about ACE inhibition, implying that no absorption is required⁽ Reference Yamada, Matoba and Usui ^{190 )}. Two of the other small peptides listed by Martínez-Maqueda et al. ⁽ Reference Martínez-Maqueda, Miralles and Recio ^{158 )} (attributed to Jiang et al. ⁽ Reference Jiang, Tian and Brodkorb ^{191 )} as having ACE-inhibitory properties) have amino acid motifs reported by Yoshikawa et al. ⁽ Reference Yoshikawa, Tani, Shiota, Brantl and Teschemacher ^{192 )} to be opioid antagonists. Derived from κ-casein there are four more peptides (casoxins) present in milk known to be opioid antagonists⁽ Reference Yoshikawa, Tani, Shiota, Brantl and Teschemacher ^{192 )}. The small peptides listed by Martínez-Maqueda et al. ⁽ Reference Martínez-Maqueda, Miralles and Recio ^{158 )} are different in that they contain di- and tri-amino acid sequences that are reported to have antihypertensive properties (for example, tyrosine–proline (YP) and leucine–phenylalanine–phenylalanine (LLF)). It is possible that many of the listed peptides may be degraded by enzymic hydrolysis to release di- and tripeptides which may then be absorbed via the PepT1 peptide transporter.

Opioid-acting peptides

In a recent review, Hernández-Ledesma et al. ⁽ Reference Hernández-Ledesma, del Mar Contreras and Recio ^{193 )} also suggested that opioid receptors are probably involved with antihypertensive effects, citing α-lactorphin, β-lactorphin and human casein-derived fragments as examples of peptides in which their antihypertensive effects are abolished by the opioid receptor antagonist naloxone. In earlier studies Nurminen et al. ⁽ Reference Nurminen, Sipola and Kaarto ^{194 )} determined that following a single subcutaneous injection of the tetrapeptide YGLF, derived from α-lactalbumin, both the systolic and diastolic blood pressures were lowered in SHR and normotensive rats. Using mesenteric arterial preparations Sipola et al. ⁽ Reference Sipola, Finckenberg and Vapaatalo ^{195 )} proposed that the blood pressure-lowering effect of YGLF in SHR is mediated via vasodilation in mesenteric arteries following peripheral opioid receptor stimulation and subsequent NO release. Strangely, YGLF did not alter the vascular responses in the mesenteric arteries from age-matched normotensive Wistar–Kyoto rats⁽ Reference Sipola, Finckenberg and Vapaatalo ^{195 )}. Ovokinin(2-7) (RADHPF), another NO-dependent vasorelaxing peptide, isolated from a chymotryptic digest of ovalbumin, has also been demonstrated to lower the blood pressure of SHR and to have no effect on the blood pressure of normotensive Wistar–Kyoto rats⁽ Reference Yamada, Matoba and Usui ^{190 )}. Studies such as these suggest that such opioid peptides may lower blood pressure through receptors expressed in the GIT, implying that no absorption is required. Miguel et al. ⁽ Reference Miguel, Gómez-Ruiz and Recio ^{196 )} noted that mechanisms other than ACE inhibition have been reported to explain the antihypertensive effect of various peptide sequences, for example, vasodilation⁽ Reference Miguel, Manso and López-Fandiño ^{197 –} Reference Miguel, Alvarez and López-Fandiño ^{199 )} and antioxidant activity⁽ Reference Dávalos, Miguel and Bartolome ^{200 –} Reference Hirota, Ohki and Kawagishi ^{202 )}.

Interestingly a local RAS has been reported to be present in the small intestine, with the key components being expressed at the gene and protein levels of the jejunal and ileal enterocytes⁽ Reference Wong, Debnam and Leung ^{203 )}. Angiotensinogen, ACE, together with angiotensin I (AngI) and AngII receptors, are localised in the microvilli of the BBM⁽ Reference Leung and Leung ^{204 –} Reference Bruneval, Hinglais and Alhenc-Gelas ^{206 )}. ACE, a metalloproteinase, hydrolyses AngI (a decapeptide) to AngII (an octapeptide). The AngII released then binds to AngII receptors in the BBM⁽ Reference Wong, Debnam and Leung ^{203 ,} Reference Cox, Munday and Poat ^{207 )} and at low doses AngII stimulates jejunal Na and water absorption. At higher doses of AngII, fluid absorption is inhibited via an AngI receptor-dependent process⁽ Reference Jin, Wang and Siragy ^{208 )}. Enterocyte-derived AngII is also involved in the regulation of Na⁺-d-glucose cotransporter 1 (SGLT1)-mediated intestinal glucose transport at the BBM⁽ Reference Leung and Leung ^{204 )}. Yoshioka et al. ⁽ Reference Yoshioka, Erickson and Woodley ^{209 )} proposed that ACE associated with the BBM may function as a membrane-bound peptidase. A comparison of intestinal fluid absorption between male SHR and normotensive male controls has been reported, with enhanced fluid absorption in both hypertensive adults and in young SHR before hypertension has developed⁽ Reference Dorey, King and Munday ^{210 )}. Na and fluid homeostasis is therefore abnormal in SHR compared with normotensive rats⁽ Reference Catalanotto, Schechter and Henkin ^{211 )}, and in view of a possible relationship between high salt intake and hypertension⁽ Reference Dahl ^{212 )} it would appear possible that an abnormality in Na and fluid homeostasis may be significant in the development of hypertension in SHR and possibly in human hypertension⁽ Reference Dorey, King and Munday ^{210 )}. By administering captopril intravenously or by bilateral nephrectomy, Dorey et al. ⁽ Reference Dorey, King and Munday ^{210 )} demonstrated that the circulating RAS was not responsible for the high level of fluid transport in SHR as neither of these procedures suppressed fluid transport. However, the presence of the intestinal RAS was not known to these authors at the time, and Na and fluid transport across the gut wall, controlled by the local RAS, would not be affected by either procedure adopted by Dorey et al. ⁽ Reference Dorey, King and Munday ^{210 )}. As ACE inhibitors (for example, Ramipril) have been shown to inhibit human brush-border ACE activity⁽ Reference Stevens, Fernandez and Kneer ^{205 )} it follows that the absorption of Na and fluid across the gut wall will be affected. Such changes are therefore consistent with the hypothesis that antihypertensive drugs and dietary bioactive peptides have an extracellular effect on the intestinal RAS by changing the passage of Na and fluid across the gut wall and thus lowering systemic blood pressure. This might explain why the lactotripeptides VPP and IPP have been shown to lower blood pressure⁽ Reference Mizuno, Matsuura and Gotou ^{123 )} with plasma concentrations below the effective concentration for ACE inhibition⁽ Reference Foltz, Meynen and Bianco ^{125 ,} Reference van der Pijl, Kies and Ten Have ^{144 )}.

The nonpeptide (for example, captopril) and peptidomimetic dipeptide (for example, enalapril) ACE-inhibitory drugs are active-site-directed, competitive inhibitors with sub-nanomolar K_i values of 10^− 10–10^− 11(213) that have been reported by many researchers to be transported across the gut wall via the PepT1 peptide transporter⁽ Reference Amidon and Sadée ^{214 ,} Reference Bai and Amidon ^{215 )}. However, according to Brandsch et al. ⁽ Reference Brandsch, Knutter and Bosse-Doenecke ^{142 )}, transport of these compounds remains a matter of controversy. Whichever way they are transported across the gut wall, the pharmacological effectiveness of these compounds lies in their absorption from the intestinal lumen and into the hepatic portal system to react directly with the cardiovascular RAS and is therefore not restricted to stimulating the extracellular intestinal RAS.

Absorption of larger peptides

Although the absorption into the enterocytes of di- and tripeptides has been demonstrated, there are conflicting views regarding the absorption of larger peptides⁽ Reference Silva and Malcata ^{33 ,} Reference Chabance, Marteau and Rambaud ^{216 )}.

Many in vitro studies have demonstrated that milk is a rich source of bioactive peptides⁽ Reference Meisel ^{34 ,} Reference Korhonen and Pihlanto ^{57 ,} Reference Clare and Swaisgood ^{154 ,} Reference Meisel ^{157 ,} Reference Meisel and Schlimme ^{217 –} Reference Korhonen and Pihlanto ^{220 )}; however, few peptides have been shown to be biologically active in vivo following the ingestion of milk or fermented milk products (i.e. it has not been ascertained whether the functional domains of milk proteins survive digestion and reach the blood in concentrations of any physiological significance⁽ Reference Picariello, Ferranti and Fierro ^{143 )}). For example, Petrilli et al. ⁽ Reference Petrilli, Picone and Caporale ^{221 )} demonstrated that β-casomorphins, the family of bioactive peptides derived from milk β-casein⁽ Reference Kreil, Umbach and Brantl ^{222 ,} Reference Daniel and Hahn ^{223 )}, do not survive digestive degradation. In addition, Schmelzer et al. ⁽ Reference Schmelzer, Schöps and Reynell ^{224 )} determined that no significant amounts of β-casomorphins or other known bioactive peptides are formed during the peptic digestion of bovine β-casein under simulated gastric conditions. Vermeirssen et al. ⁽ Reference Vermeirssen, Van Camp and Verstraete ^{20 )} also came to a similar conclusion, stating that no intact transepithelial passage has been detected for these peptides. However, there are many papers outlining physiological effects/functions of milk-borne bioactive peptides⁽ Reference Silva and Malcata ^{33 ,} Reference Kitts and Weiler ^{50 ,} Reference Meisel ^{52 ,} Reference Rutherfurd-Markwick and Moughan ^{56 ,} Reference Korhonen and Pihlanto ^{57 ,} Reference Yamamoto, Ejiri and Mizuno ^{150 ,} Reference Clare and Swaisgood ^{154 ,} Reference Meisel ^{157 ,} Reference Teschemacher ^{168 ,} Reference Meisel and Fitzgerald ^{170 ,} Reference Korhonen and Pihlanto ^{220 ,} Reference Tome and Debabbi ^{225 ,} Reference Pihlanto-Leppala ^{226 )}. The prevailing current opinion is that the majority of the known bioactive peptides do not pass into the bloodstream in meaningful amounts and that any known physiological effects are mediated through receptors on the intestinal wall⁽ Reference Korhonen and Pihlanto ^{57 ,} Reference Picariello, Ferranti and Fierro ^{143 )}.

One of the most quoted/misquoted papers on the subject is that of Gardner⁽ Reference Gardner ^{227 )} stating that it has been observed that large peptides or proteolysis-resistant proteins can enter the bloodstream, albeit in small amounts. However, Gardner did not give any direct evidence for the absorption of intact protein in humans; instead the following was offered in support of the hypothesis that intact proteins and macromolecular fragments of them may be absorbed:

1. (a) That antibodies to many food proteins and their immune complexes have been detected in the circulation of healthy individuals⁽ Reference Paganelli and Levinsky ^{228 –} Reference Cunningham-Rundles, Brostoff and Challocombe ^{232 )}. However, he qualified this statement by suggesting that such antibodies may arise through the intestinal immune system responding to luminal proteins rather than absorbed ones.

2. (b) That RIA techniques⁽ Reference Husby, Foged and Høst ^{233 ,} Reference Jakobsson, Lindberg and Lothe ^{234 )} show the presence of orally administered proteins such as ovalbumin in the blood. However, referring back to the researchers cited by Gardner, Husby et al. ⁽ Reference Husby, Foged and Høst ^{233 )} fed ten children (aged 2.5–13 years) a test meal containing 2 ml of raw egg and 10 ml cows' milk per kg body weight through a gastric tube placed adjacent to the ligament of Treitz. Five of the children had been diagnosed with coeliac disease and the five controls were also suspected of having coeliac disease. Although they found ovalbumin in the plasma of three of the five coeliac patients and all five of the controls, the feeding conditions and all the experimental subjects being children, with or suspected of suffering from coeliac disease, suggest their results should be treated with caution. With respect to Jakobsson et al. ⁽ Reference Jakobsson, Lindberg and Lothe ^{234 )}, the target protein was not found to be absorbed in all subjects. The protein α-lactalbumin purified from human milk was not detected ( < 5 μg/l) in the serum of adult men, non-pregnant women or in the serum from formula-fed infants. However, α-lactalbumin was found in serum from pregnant women, cord blood and from newborn non-fed infants.

3. (c) That intact or largely intact HRP was found in the blood of carp and trout⁽ Reference McLean and Ash ^{235 ,} Reference McLean and Ash ^{236 )}. However, it must be questioned as to whether observations in fish apply to adult humans. Interestingly, Heyman⁽ Reference Heyman ^{58 )} reported that during active cows' milk allergy there was an eightfold increase in the absorption of the bystander protein HRP and an alteration of the epithelial integrity. However, after several months on a cows' milk-free diet and during a symptom-free period the absorption of HRP and paracellular permeability returned to normal values, indicating that the increased intestinal permeability to antigens was not the primary cause of the condition⁽ Reference Heyman ^{58 )}.

Further, Gardner⁽ Reference Gardner ^{227 )} cited the work of Walker et al. ⁽ Reference Walker, Abel and Wu ^{237 ,} Reference Walker, Wu and Isselbacher ^{238 )} who studied the in vitro absorption of dietary antigen and antigen–antibody complexes to corroborate their hypothesis. This will be discussed in more detail below, relative to the work of Roberts et al. ⁽ Reference Roberts, Burney and Black ^{115 )}. Another paper often quoted is that of Fiat et al. ⁽ Reference Fiat, Miglioresamour and Jolles ^{239 )} who cite Gardner⁽ Reference Gardner ^{227 )}. Gardner describes the GIT as a major site of immunological competence, as substantial numbers of lymphocytes and macrophages are found throughout the intestinal lamina propria. He hypothesises that absorption occurs predominantly by transcellular endocytosis in the M-cells (or lymphoepithelial cells⁽ Reference Wolf, Rubin and Finberg ^{240 )}) and that this allows subepithelial lymphocytes direct access to luminal antigens. Transcellular endocytosis occurs when protein molecules bind to receptors on the BBM, which are then encapsulated into phagolysosomes. Proteolysis in the phagolysosomes minimises the entry of intact bioactive peptides into the circulation, which Gardner⁽ Reference Gardner ^{241 )} states is likely to be deleterious. So, although antibodies to numerous food proteins may occur in the circulation of healthy individuals, this should not be taken as evidence for the presence of the original peptide antigens within the blood. Gardner also states that it is not yet possible to state with reliable accuracy what fraction of the protein will enter the circulation in macromolecular form.

Much more work has been undertaken since Gardner wrote his paper in 1988⁽ Reference Gardner ^{227 )}, yet still little is known about the absorption of the larger bioactive peptides. Teschemacher et al. ⁽ Reference Teschemacher, Umbach and Hamel ^{242 )}, in a classic review, suggested that β-casomorphins and their precursors have not been identified in the cardiovascular compartment in more than negligible concentrations and it is unlikely that they have any functional role in adult mammals outside the GIT. Teschemacher also states that enzymic degradation in the intestinal wall and in the blood appears to prevent the accumulation of peptides in plasma⁽ Reference Teschemacher, Umbach and Hamel ^{242 –} Reference Read, Lord and Brantl ^{244 )}. For example dipeptidyl-peptidase is one of the enzymes that effectively degrades β-casomorphins in plasma⁽ Reference Kreil, Umbach and Brantl ^{222 )} and in the intestinal brush border⁽ Reference Tiruppathi, Miyamoto and Ganapathy ^{245 )}. Meisel & Fitzgerald⁽ Reference Meisel and Fitzgerald ^{170 )} also point out that opioid casein fractions have not been detected in the plasma of adult mammals and that only in the neonate is the intestine permeable to casomorphins and their precursors. Teschemacher et al. ⁽ Reference Teschemacher, Umbach and Hamel ^{242 )} and the reviews by Clare & Swaisgood⁽ Reference Clare and Swaisgood ^{154 )}, Gill et al. ⁽ Reference Gill, Doull and Rutherfurd ^{246 )} and Shah⁽ Reference Shah ^{155 )} reach similar conclusions to that of Gardner⁽ Reference Gardner ^{227 )}. Froetschel⁽ Reference Froetschel ^{184 )} found that there is no evidence to support the theory that opioid peptides, such as the β-casomorphins, are transported into the bloodstream to the brain, or that they can cross the blood–brain barrier. No bioactive peptides or their native proteins have any established physiological role though they do have a variety of physiological effects.

However, to demonstrate the physiological effects of the multitude of bioactive peptides, researchers have often introduced them directly into the blood⁽ Reference Bray ^{247 )}, the cerebrospinal fluid⁽ Reference Zhao, Garreau and Sannier ^{165 ,} Reference Bakalkin, Demuth and Nyberg ^{248 ,} Reference Nyberg, Sanderson and Glamsta ^{249 )} or even directly into the brain⁽ Reference Yoshikawa, Tani and Ashikaga ^{250 –} Reference Hedner and Hedner ^{252 )}. Conclusive evidence for the functional significance of milk-derived opioid peptides has not yet been presented⁽ Reference Teschemacher, Koch and Brantl ^{169 )} and the effects demonstrated by researchers for isolated or synthesised peptides derived from milk represent evidence of a pharmacological activity and not of a physiological role.

Roberts et al. ⁽ Reference Roberts, Burney and Black ^{115 )} studied the effect of amino acid chain length on the absorption of biologically active peptides from the GIT. Studying the absorption of just three peptides of differing chain length (thyrotropin-releasing hormone, a tripeptide; luteinising hormone-releasing hormone, a decapeptide; and human insulin, a fifty-one-amino acid polypeptide), they concluded that ‘large peptides’ (sic) as large as fifty-one amino acids generated from dietary proteins can be absorbed intact through the intestine and produce biological effects at the tissue level. This conclusion has been quoted by many other researchers⁽ Reference Vermeirssen, Van Camp and Verstraete ^{20 ,} Reference Erdmann, Cheung and Schroder ^{116 ,} Reference Robert, Razaname and Mutter ^{120 ,} Reference Zaloga and Siddiqui ^{121 ,} Reference Escudero, Sentandreu and Arihara ^{126 ,} Reference van der Pijl, Kies and Ten Have ^{144 ,} Reference Cheng, Liu and Wan ^{253 )}.

A number of factors need to be considered, however, to critically test such a claim:

1. (a) The study of Roberts et al. ⁽ Reference Roberts, Burney and Black ^{115 )} was undertaken using rats. Although this is an accepted animal model for simple-stomached mammals in general, the results do not necessarily relate to humans.

2. (b) The polypeptides were administered into the small intestine of the animal distal to the pancreatic duct and level with the ligament of Treitz, effectively bypassing both gastric and pancreatic degradative hydrolysis.

3. (c) The authors stated that the absorptive capacity of the small intestine in the experimental animals was not assessed and that the animal received a surgical procedure which placed a feeding tube within the small intestine that ‘may have altered gut permeability and absorption’. It is known, for example, that such a naso-ileal tube affects gastric emptying⁽ Reference Medhus, Sandstad and Bredesen ^{254 ,} Reference Fone, Horowitz and Heddle ^{255 )}, increases intestinal transit time⁽ Reference Read, Aljanabi and Bates ^{256 )}, can stimulate intestinal secretions⁽ Reference Read, Aljanabi and Bates ^{256 ,} Reference Hendrix and Bayless ^{257 )}, and that the effect of a gastrointestinal tube on the absorption and secretion of other substances has not been fully investigated.

4. (d) Although Roberts et al. ⁽ Reference Roberts, Burney and Black ^{115 )} measured serum insulin in the plasma of the experimental animals they did not state if this compound was the human insulin administered enterally or native rat insulin. In addition they did not determine the serum levels of the peptides administered, only their physiological effect (i.e. for thyrotropin-releasing hormone by determining serum thyroid-stimulating hormone levels and for luteinising hormone-releasing hormone they determined serum follicle-stimulating hormone levels). They also did not rule out that the physiological effects may have been mediated directly via the gut lumen or through receptors on the BBM.

5. (e) Roberts et al. ⁽ Reference Roberts, Burney and Black ^{115 )} tested for the absorption of human insulin, which has a different amino acid sequence to that of rat insulin, and used a very large enteral dose of 25 mg (avoiding both gastric and upper small intestine digestive hydrolysis) to produce the measurable physiological effect.

Considering the above, Roberts et al. ⁽ Reference Roberts, Burney and Black ^{115 )} may possibly have over-extrapolated their conclusions by assuming that: (a) the oral intake of dietary peptides would be the same as enteral administration; (b) that gastric and pancreatic hydrolysis of such dietary peptides would be negligible; and (c) that all dietary peptides resistant to digestive degradation would be absorbed from the small intestine to the same extent as their experimental peptides (human insulin, thyrotropin-releasing hormone and luteinising hormone-releasing hormone).

Jahan-Mihan et al. ⁽ Reference Jahan-Mihan, Luhovyy and El Khoury ^{111 )} claim that the absorption of intact proteins and peptides was demonstrated after animals were exposed to an intraduodenal infusion of somatostatin and with an increased concentration of somatostatin found in the blood. The paper they cite in support of this conjecture is that of Rao et al. ⁽ Reference Rao, Koldovsky and Davis ^{258 )}, who demonstrated the absorption of radioisotope-labelled [Reference Foltz, Meynen and Bianco ¹²⁵ I][TyrReference Newey and Smyth ¹¹ ]somatostatin-14 following its intraduodenal administration in anaesthetised adult and neonatal rats. Somatostain-14 is a peptide-inhibitory hormone containing fourteen amino acids and with a molecular mass of 1638 Da. Intraduodenally administered somatostatin-14 has been shown to inhibit pancreatic secretions in rats⁽ Reference Sarfati and Morisset ^{259 )} and dogs⁽ Reference Konturek, Tasler and Cieszkowski ^{260 ,} Reference Konturek, Bilski and Jaworek ^{261 )}. Rao et al. ⁽ Reference Rao, Koldovsky and Davis ^{258 )} demonstrated that intraduodenally administered [¹²⁵I][Tyr¹¹]somatostatin-14 rapidly disappeared from the duodenal lumen of both suckling and adult rats (half-life being 2 min). The loss of radioactivity from the lumen coincided with its simultaneous appearance in the tissues of the duodenal wall, blood, liver and kidney. Using C 18 Bond Elut cartridges and HPLC no intact [¹²⁵I][Tyr¹¹]somatostatin-14 was found in any of those tissues and suggests that the [¹²⁵I][Tyr¹¹]somatostatin-14 was rapidly metabolised intraduodenally and that no somatostatin had been absorbed by the gut wall and transferred to the blood or other organs. Rao et al. ⁽ Reference Rao, Koldovsky and Davis ^{258 )} suggest that the inhibition of pancreatic secretions observed by Sarfati & Morisset⁽ Reference Sarfati and Morisset ^{259 )} in rats and of Konturek et al. ⁽ Reference Konturek, Tasler and Cieszkowski ^{260 ,} Reference Konturek, Bilski and Jaworek ^{261 )} in dogs is mediated by somatostatin receptors in the duodenal wall. The argument that deiodination may occur before intestinal absorption⁽ Reference Jones ^{262 )} appears to be unfounded, as Rao et al. ⁽ Reference Rao, Koldovsky and Davis ^{258 )} found no free ¹²⁵I in any of the tissues described and unlabelled somatostatin-14 disappeared from the duodenal lumen at the same rate as that of the labelled compound. Such results suggest that peptidases in the duodenal lumen and at the surface of the BBM were responsible for the metabolism of the somatostatin-14. Rao et al. ⁽ Reference Rao, Koldovsky and Davis ^{258 )} also observed that the duodenal half-life for the [¹²⁵I][Tyr¹¹]somatostatin-14 was longer for the neonatal rats than in the adult rats, suggesting that milk-borne somatostatin may be more hydrolytically stable and biologically active for longer in the gut of the neonate rat, protected by peptidase inhibitors within the milk⁽ Reference Rao, Koldovsky and Davis ^{258 )}.

Historically it has been claimed that various digestive enzymes are selectively absorbed intact from the intestinal lumen directly into the bloodstream⁽ Reference Moriya, Moriwaki and Akimoto ^{263 –} Reference Warshaw, Walker and Isselbacher ^{273 )} via the superior mesenteric vein from where they are extracted by the pancreas during the passage of blood through the pancreatic capillary bed. Having reclaimed pancreatic digestive enzymes from the circulation it was hypothesised that they are then resecreted by the exocrine pancreas into the duodenum along with other components of pancreatic juice in what has been controversially described as enteropancreatic circulation⁽ Reference Rothman, Liebow and Isenman ^{274 –} Reference Liebow and Rothman ^{276 )}. While there is evidence of the absorption of small quantities of digestive enzymes from the small intestine (for example, < 0·2 % pancreatic amylase⁽ Reference Levitt, Ellis and Murphy ^{277 ,} Reference Rosenblum, Raab and Alpers ^{278 )}) such quantities are insufficient to support the existence of a physiologically significant enteropancreatic circulation mechanism⁽ Reference Levitt, Ellis and Murphy ^{277 –} Reference Rohr, Kern and Scheele ^{280 )}. Interestingly, Levitt et al. ⁽ Reference Levitt, Ellis and Murphy ^{277 )} reported that the net flux of amylase was from the pancreas into the blood and not the other way round; evidence contrary to the theory that circulating enzymes can be reclaimed by the pancreas. Following the publication of two articles by Levitt and colleagues⁽ Reference Levitt, Ellis and Murphy ^{277 ,} Reference Levitt ^{279 )} and another by Rosenblum et al. ⁽ Reference Rosenblum, Raab and Alpers ^{278 )} and the study by Rohr et al. ⁽ Reference Rohr, Kern and Scheele ^{280 )}, Rothman & Grendell⁽ Reference Rothman and Grendell ^{281 )} sought to justify their hypothesis by dismissing the contrary experimental evidence reported in the three papers. The authors of the four papers cited by Rothman & Grendell⁽ Reference Rothman and Grendell ^{281 )} vehemently defended their findings and reiterated there was no evidence to support the existence of a physiologically important enteropancreatic circulation of enzymes and a good deal of evidence to the contrary⁽ Reference Levitt ^{279 ,} Reference Rohr, Kern and Scheele ^{282 )}. Rosenblum et al. ⁽ Reference Rosenblum, Raab and Alpers ^{283 )} suggested that although further studies under different experimental conditions might modify their conclusions, those who champion the importance of enteropancreatic circulation should support their belief with new data. In an effort to reignite the enteropancreatic circulation debate, Rothman et al. ⁽ Reference Rothman, Liebow and Isenman ^{274 )} published an extensive review citing many papers in support of their hypothesis.

One widely reported dietary protein that may be absorbed across the gut wall and enter the bloodstream intact is ovalbumin⁽ Reference Joo and Kato ^{284 –} Reference Moreno ^{288 )}. Ovalbumin is the predominant protein in egg white, it contains 385 amino acids, has a molecular mass of 46.4 kDa⁽ Reference Wharton ^{289 )} and a cross-sectional diameter of 4 nm⁽ Reference Soderholm, Peterson and Olaison ^{290 )}. The intestinal absorption of ovalbumin is known to invoke systemic immunological tolerance⁽ Reference Chehade and Mayer ^{291 )} and a mucosal secretion of IgA⁽ Reference Frossard, Hauser and Eigenmann ^{292 )}. However, in individuals with food allergy, ovalbumin can also stimulate the development of IgE-mediated food allergy⁽ Reference Dannaeus, Inganas and Johansson ^{293 –} Reference James ^{295 )}. Castell et al. ⁽ Reference Castell, Friedrich and Kuhn ^{296 )} have suggested that the absorption of macromolecules, including intact proteins, may occur under specific circumstances and that this phenomenon could be involved in the pathophysiology of certain intestinal diseases (for example, cows' milk allergy and inflammatory bowel disease)⁽ Reference Sanderson and Walker ^{5 ,} Reference Heyman ^{58 ,} Reference Castell, Friedrich and Kuhn ^{296 –} Reference Heyman ^{298 )}.

Oral delivery of pharmacologically active proteins and peptides

Pharmacologically active proteins and peptides are currently emerging as an imperative part of various treatment protocols and in particular cancer therapeutics⁽ Reference Gupta, Jain and Chakraborty ^{299 )}. However, despite extensive research, the administration of therapeutic peptides and proteins orally remains a challenge for pharmaceutical industries and researchers. Acidity and high enzymic proteolysis within the GIT are significant barriers to the successful delivery of intact proteins/peptides to the targeted site. Gupta et al. ⁽ Reference Gupta, Jain and Chakraborty ^{299 )} emphasise in their recent review that low permeability of the intestinal barrier is also a factor adding to the low bioavailability of any orally delivered proteins and peptides. Added to which, the short circulatory half-life exhibited by such peptides in vivo requires them to be administered frequently, which in turn increases the cost of treatment and results in low patient compliance⁽ Reference Rabanel, Aoun and Elkin ^{300 )}. One solution to this is the development of nano-carrier-based delivery that protects therapeutic proteins from degradation. As the surface of these particles can be modified towards hydrophilic or lipophilic properties, these systems promise high enterocytic permeability. Gupta et al. ⁽ Reference Gupta, Jain and Chakraborty ^{299 )} have suggested that nano-encapsulated proteins and peptides may also have enhanced stability in vivo that leads to increased circulation half-lives so the active peptides can reach the target tissue in effective concentrations. However, despite this, there are currently only a few orally delivered peptide/protein biopharmaceutical systems available and continued research is required to reap the promised effectiveness of these systems.

Essential in the treatment of diabetes mellitus is the peptide hormone insulin, which is currently administered to sufferers via subcutaneous injections. For patients who require daily injections of insulin the development of a less invasive route of administration would increase their quality of life significantly. Although the oral administration of insulin meets this criterion, Kamei et al. ⁽ Reference Kamei, Nielsen and Khafagy ^{301 )} point out that two barriers must be overcome: the impermeability of insulin through the epithelial membranes and local digestion and enzymic degradation. To overcome the poor pharmacokinetics of oral administered insulin cell-penetrating peptides (CPP) could deliver exogenous proteins into cells and have the potential to facilitate effective insulin permeation from the intestinal lumen into the systemic circulation. In their review Kamei et al. ⁽ Reference Kamei, Nielsen and Khafagy ^{301 )} describe how the co-administration of insulin with the short hydrophilic peptide penetratin, a typical CPP, increased intestinal insulin bioavailability to 35 %. The development of more effective CPP requires further research at this time. Recently, Renukuntla et al. ⁽ Reference Renukuntla, Vadlapudi and Patel ^{302 )} renewed the debate on the barriers to the oral delivery of peptide and protein drugs and reviewed many of the novel pharmaceutical approaches to circumvent these barriers and enhance oral bioavailability of these macromolecules.

Although liposomes have been used for the past 30 years as carriers of proteins and peptides requiring protection from the deleterious effects of the GIT, Swaminathan & Ehrhardt⁽ Reference Swaminathan and Ehrhardt ^{303 )} note that the majority of data generated has been from in vitro studies or from work using rodents. Even though many of these studies have demonstrated that liposomes are effective carriers, the extrapolation from such models to human pharmacotherapy is challenging. Recently, liposomes loaded into alginate–chitosan microspheres or hyaluronic acid gels have been found to be promising vectors in the oral administration of protein or peptide drugs⁽ Reference Zhang, Wei and Lv ^{304 )}, for example, insulin delivery⁽ Reference Mukhopadhyay, Mishra and Rana ^{305 )}.

Absorption, distribution, metabolism and excretion

Foltz et al. ⁽ Reference Foltz, van der Pijl and Duchateau ^{30 )} have cautioned us all, stating that although peptide absorption and peptide stimulatory/inhibitory effects may have been demonstrated in vitro, ex vivo and in vivo evidence for the absorption of oligopeptides in humans is lacking. Although selected peptides (for example, C-terminal proline-containing peptides) exhibit resistance to luminal peptidases, they remain susceptible to brush-border and cytosolic peptidases so that only minor fragments are expected to reach the systemic circulation⁽ Reference Foltz, van der Pijl and Duchateau ^{30 )}. Knowing the plasma concentrations and kinetics of orally administered peptides is essential for planning meaningful studies to assess the bioactivity of dietary peptides. Foltz et al. ⁽ Reference Foltz, van der Pijl and Duchateau ^{30 )} have stated that it is only valid to propose in vivo efficacy for bioactive peptides when the peptide exhibits reasonable proteolytic stability and physiologically relevant absorption, distribution, metabolism and excretion (ADME) profiles. Currently there is a lack of scientific evidence demonstrating that peptides, originating from dietary sources, have absorption or plasma clearance profiles that result in acceptable bioavailability. Foltz et al. ⁽ Reference Foltz, van der Pijl and Duchateau ^{30 )} concur with others that ADME properties may be conducive to supporting peptide activity only under certain pathophysiological conditions such as food allergies or inflammatory bowel disease⁽ Reference Ingersoll, Ayyadurai and Charania ^{46 ,} Reference Heyman ^{58 ,} Reference Diesner, Knittelfelder and Krishnamurthy ^{294 ,} Reference Olaison, Sjodahl and Tagesson ^{306 –} Reference Dalmasso, Nguyen and Charrier-Hisamuddin ^{309 )}. The majority of in vitro studies, to identify bioactive peptides, have been conducted at high micromolar and even millimolar concentrations with incubation times lasting as long as 24 h. These conditions are often not realistic nor physiologically relevant⁽ Reference Foltz, van der Pijl and Duchateau ^{30 )}.