Investigating intestinal mast cell dynamics during acute heat stress in growing pigs.
J Anim Sci
; 1022024 Jan 03.
Article
em En
| MEDLINE
| ID: mdl-38290531
ABSTRACT
Objectives were to examine the temporal pattern of intestinal mast cell dynamics and the effects of a mast cell stabilizer (ketotifen [Ket]) during acute heat stress (HS) in growing pigs. Crossbred barrows (nâ
=â
42; 32.3â
±â
1.9 kg body weight [BW]) were randomly assigned to 1 of 7 environmental-therapeutic treatments (1) thermoneutral (TN) control (TNCon; nâ
=â
6), (2) 2 h HS control (2 h HSCon; nâ
=â
6), (3) 2 h HSâ
+â
Ket (2 h HSKet; nâ
=â
6); (4) 6 h HSCon (nâ
=â
6), (5) 6 h HSKet (nâ
=â
6), (6) 12 h HSCon (nâ
=â
6), or (7) 12 h HSKet (nâ
=â
6). Following 5 d of acclimation to individual pens, pigs were enrolled in two experimental periods (P). During P1 (3 d), pigs were housed in TN conditions (21.5â
±â
0.8 °C) for the collection of baseline measurements. During P2, TNCon pigs remained in TN conditions for 12 h, while HS pigs were exposed to constant HS (38.1â
±â
0.2 °C) for either 2, 6, or 12 h. Pigs were euthanized at the end of P2, and blood and tissue samples were collected. Regardless of time or therapeutic treatment, pigs exposed to HS had increased rectal temperature, skin temperature, and respiration rate compared to their TNCon counterparts (1.9 °C, 6.9° C, and 119 breaths/min; Pâ
<â
0.01). As expected, feed intake and BW gain markedly decreased in HS pigs relative to their TNCon counterparts (Pâ
<â
0.01). Irrespective of therapeutic treatment, circulating corticotropin-releasing factor decreased from 2 to 12 h of HS relative to TNCon pigs (Pâ
<â
0.01). Blood cortisol increased at 2 h of HS (2-fold; Pâ
=â
0.04) and returned to baseline by 6 h. Plasma histamine (a proxy of mast cell activation) remained similar across thermal treatments and was not affected by Ket administration (Pâ
>â
0.54). Independent of Ket or time, HS increased mast cell numbers in the jejunum (94%; Pâ
<â
0.01); however, no effects of HS on mast cell numbers were detected in the ileum or colon. Jejunum and ileum myeloperoxidase area remained similar among treatments (Pâ
>â
0.58) but it tended to increase (12%; Pâ
=â
0.08) in the colon in HSCon relative to TNCon pigs. Circulating lymphocytes and basophils decreased in HSKet relative to TN and HSCon pigs (Pâ
≤â
0.06). Blood monocytes and eosinophils were reduced in HS pigs relative to their TNCon counterparts (Pâ
<â
0.01). In summary, HS increased jejunum mast cell numbers and altered leukocyte dynamics and proinflammatory biomarkers. However, Ket administration had no effects on mast cell dynamics measured herein.
Heat stress (HS) affects various physiological, metabolic, and endocrine parameters, ostensibly due to reduced intestinal barrier integrity and the ensuing immune response. Evidence indicates that generalized "stress" may be a critical component of HS-induced leaky gut, a mechanism likely mediated by mast cells. Mast cell activation has been extensively associated with various stress-related intestinal inflammatory conditions; however, its contribution to intestinal barrier dysfunction during HS remains unclear. Thus, this study was designed to evaluate mast cell dynamics during an acute HS challenge and to assess the effects a mast cell stabilizer on biomarkers of intestinal inflammation. Herein, HS induced a rapid increase in circulating cortisol, increased jejunum mast cell numbers, and altered metabolism, leukocyte dynamics, and proinflammatory biomarkers. Contrary to our hypothesis, HS did not alter circulating histamine (a biomarker of mast cell activation), and mast cell stabilization did not affect mast cell numbers nor altered histamine concentrations. Altogether, our observations support a connection between HS and intestinal mast cell infiltration that may contribute to the pathophysiology of intestinal dysfunction during a heat load.
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Base de dados:
MEDLINE
Assunto principal:
Doenças dos Suínos
/
Transtornos de Estresse por Calor
Limite:
Animals
Idioma:
En
Ano de publicação:
2024
Tipo de documento:
Article