Novel Long‐Acting GLP‐2 Analogue, FE 203799 (Apraglutide), Enhances Adaptation and Linear Intestinal Growth in a Neonatal Piglet Model of Short Bowel Syndrome with Total Resection of the Ileum

Slim, George; Lansing, Marihan; Wizzard, Pamela; Nation, Patrick N.; Wheeler, Sarah E.; Brubaker, Patricia L.; Jeppesen, Palle Bekker; Wales, Paul W.; Turner, Justine

doi:10.1002/jpen.1500

Cited by 35 publications

(44 citation statements)

References 30 publications

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“…In piglet models, both native GLP‐2 and TED treatments have not shown intestinal lengthening 16,17 . Recently, we studied apraglutide (APRA), a GLP‐2 analogue with an even longer half‐life (t 1/2 ) than TED 18 . APRA was associated with intestinal lengthening in our piglet model of SBS with total ileal resection (jejunocolic [JC] anastomosis), a model wherein consistently we have not seen linear intestinal growth without trophic peptide treatment 17 …”

Section: Introductionmentioning

confidence: 99%

Comparing the Intestinotrophic Effects of 2 Glucagon‐Like Peptide‐2 Analogues in the Treatment of Short‐Bowel Syndrome in Neonatal Piglets

Pauline

Nation

Wizzard

et al. 2020

J Parenter Enteral Nutr

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Background In treating short‐bowel syndrome (SBS), autonomy from parenteral nutrition (PN) relies upon intestinal adaptation, which can be augmented by glucagon‐like peptide‐2 (GLP‐2) analogues. In neonatal piglets with SBS, we compared intestinal adaptation following treatment with 2 GLP‐2 analogues: teduglutide (TED) and apraglutide (APRA) Methods Following 75% distal small‐intestinal resection, piglets were allocated to 4 treatment groups: saline (CON: n = 8), twice weekly APRA (5 mg/kg/dose; n = 8), and TED once daily (TED, 0.05 mg/kg/dose; n = 8) or twice daily (TEDBID, 0.05 mg/kg/dose; n = 7). Pharmacokinetic (PK) studies were undertaken, and on day 7, small‐intestinal length and weight were measured and jejunal tissue collected for histology. Results PK profiles were different between the 2 analogues. To achieve a comparable exposure to APRA, TED requires twice daily injection (TEDBID). Compared with CON, APRA and TEDBID increased small‐bowel length (cm) (CON: 141, APRA: 166, TED: 153, TEDBID: 165; P = .004), whereas APRA increased small‐bowel weight (g) (CON: 26, APRA: 33, TED: 28, TEDBID: 31; P = .007) and villus height (mm) (CON: 0.59, APRA: 0.90, TED: 0.58, TEDBID: 0.74; P < .001). Conclusion APRA injected only twice during the 7 consecutive days demonstrated a superior intestinotrophic effect compared with TED injected once daily. Even at more comparable drug exposure, when TED was injected twice a day, APRA showed superior trophic activity at the mucosal level. This is highly relevant for the treatment of pediatric SBS, given the markedly lower dose frequency by subcutaneous injection of APRA.

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Section: Introductionmentioning

confidence: 99%

Comparing the Intestinotrophic Effects of 2 Glucagon‐Like Peptide‐2 Analogues in the Treatment of Short‐Bowel Syndrome in Neonatal Piglets

Pauline

Nation

Wizzard

et al. 2020

J Parenter Enteral Nutr

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“…Indeed, the 13% increase in small intestinal length observed following only 3 weeks of administration of apraglutide is further remarkable given the limited effect of hGly 2 -GLP-2 1-33 reported for this parameter in rodents Hadjiyanni, 2009;Austin, 2015). Apraglutide has also been demonstrated to increase small intestinal length in a neonatal piglet model of short bowel syndrome, leading to the suggestion that the trophic actions of apraglutide may enhance adaptation and weaning from parenteral nutrition in young children with short bowel syndrome (Slim, 2019). Whether enhanced intestinal length will be observed in humans treated with GLP-2R agonists remains to be determined.…”

Section: Discussionmentioning

confidence: 97%

“…The final version may differ from this version. (Slim, 2019). Furthermore, it remains unclear as to whether teduglutide treatment affects the growth of the colon in humans.…”

Section: Clinical Perspectivementioning

confidence: 99%

“…However, given that many previous pre-clinical studies on the intestinotrophic effects of GLP-2 in the normal murine intestine have been successfully translated to humans, these findings suggest that this novel action of apraglutide may benefit patients through expansion of the residual, healthy tissue. Finally, the half-life of apraglutide is prolonged (t½ = 30 hr) as compared to both native GLP-2 and hGly 2 -GLP-2 1-33 (~6 min and 1-3 hr, respectively), due to both dipeptidylpeptidase IV-resistance and binding to proteins in the circulation (99.8%) (Tavares, 2000;Marier, 2010;Slim, 2019). As a consequence, apraglutide was administered only 3-times per week in the present study, as compared to the current requirement for daily treatment with hGly 2 -GLP-2 1-33 and teduglutide, although it is acknowledged that the dose of apraglutide utilized in the current study on mice is ~3-times greater than that currently being tested for human use (Bolognani, 2019).…”

Section: Clinical Perspectivementioning

confidence: 99%

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Site-Specific and Temporal Effects of Apraglutide, a Novel Long-Acting Glucagon-Like Peptide-2 Receptor Agonist, on Intestinal Growth in Mice

Martchenko

Sweeney

Dimitriadou

et al. 2020

J Pharmacol Exp Ther

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Long-acting glucagon-like peptide-2 receptor (GLP-2R) agonists are well-established to increase intestinal growth in rodents and, most notably, humans with short bowel syndrome. Most of the trophic effects of GLP-2R agonists are reported to be mediated through increased growth of the crypt-villus axis, resulting in enhanced mucosal mass and improved intestinal function. The present study examined the effects of apraglutide, a novel GLP-2R agonist, on the growth of the small and large intestines, after 3, 7 and 10 weeks of treatment in male and female mice. Apraglutide (3mg/kg; 3-times per week) significantly increased small intestinal weight (p<0.001) and length (p<0.001) after 3 weeks of administration, with a further increase in effectiveness after 10 weeks (p<0.01). Crypt depth and villus height were both markedly increased after 3 weeks of apraglutide administration (p<0.001) but did not show any further increase with duration of treatment, whereas crypt number and intestinal circumference were increased after 7 and 10 weeks (p<0.01) but not after 3 weeks of apraglutide treatment. Both the weight and the length of the colon were also enhanced by apraglutide treatment for 3 weeks (p<0.001), and these effects were maintained but did not improve further with continued apraglutide administration. The results of this study demonstrate that the novel, long-acting GLP-2R agonist, apraglutide demonstrates unexpected marked ability to increase intestinal length, as well as exerting time-and location-dependent specificity in its intestinotrophic actions. Significance: The novel long-acting GLP-2R agonist, apraglutide, enhances intestinal weight as well as intestinal length in a time-and site-dependent fashion.

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“…[ 227 ] This could be used in combination with novel GLP‐2 analogues with low systemic clearance such as apraglutide. [ 228 ] Based on the key role of BA signaling in the gut–liver axis, the use of BAs or analogs such as the hydrophilic ursodeoxycholic acid, as supplements to TPN, could be of potential interest. [ 229 ] Ursodeoxycholic acid is a naturally occurring BA (≈5% of the total human BA pool) and is used in the treatment of primary biliary cirrhosis and cholesteric hepatitis.…”

Section: Strategies To Prevent Tpn‐associated Adverse Effectsmentioning

confidence: 99%

Novel Strategies to Prevent Total Parenteral Nutrition‐Induced Gut and Liver Inflammation, and Adverse Metabolic Outcomes

Lucchinetti

Lou

Wawrzyniak

et al. 2020

Molecular Nutrition Food Res

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Total parenteral nutrition (TPN) is a life‐saving therapy administered to millions of patients. However, it is associated with significant adverse effects, namely liver injury, risk of infections, and metabolic derangements. In this review, the underlying causes of TPN‐associated adverse effects, specifically gut atrophy, dysbiosis of the intestinal microbiome, leakage of the epithelial barrier with bacterial invasion, and inflammation are first described. The role of the bile acid receptors farnesoid X receptor and Takeda G protein‐coupled receptor, of pleiotropic hormones, and growth factors is highlighted, and the mechanisms of insulin resistance, namely the lack of insulinotropic and insulinomimetic signaling of gut‐originating incretins as well as the potentially toxicity of phytosterols and pro‐inflammatory fatty acids mainly released from soybean oil‐based lipid emulsions, are discussed. Finally, novel approaches in the design of next generation lipid delivery systems are proposed. Propositions include modifying the physicochemical properties of lipid emulsions, the use of lipid emulsions generated from sustainable oils with favorable ratios of anti‐inflammatory n‐3 to pro‐inflammatory n‐6 fatty acids, beneficial adjuncts to TPN, and concomitant pharmacotherapies to mitigate TPN‐associated adverse effects.

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Novel Long‐Acting GLP‐2 Analogue, FE 203799 (Apraglutide), Enhances Adaptation and Linear Intestinal Growth in a Neonatal Piglet Model of Short Bowel Syndrome with Total Resection of the Ileum

Cited by 35 publications

References 30 publications

Comparing the Intestinotrophic Effects of 2 Glucagon‐Like Peptide‐2 Analogues in the Treatment of Short‐Bowel Syndrome in Neonatal Piglets

Comparing the Intestinotrophic Effects of 2 Glucagon‐Like Peptide‐2 Analogues in the Treatment of Short‐Bowel Syndrome in Neonatal Piglets

Site-Specific and Temporal Effects of Apraglutide, a Novel Long-Acting Glucagon-Like Peptide-2 Receptor Agonist, on Intestinal Growth in Mice

Novel Strategies to Prevent Total Parenteral Nutrition‐Induced Gut and Liver Inflammation, and Adverse Metabolic Outcomes

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