Acidic chitinase primes the protective immune response to gastrointestinal nematodes

Vannella, Kevin M.; Ramalingam, Thirumalai R.; Hart, Kevin M.; Prado, Rafael de Queiroz; Sciurba, Joshua; Barron, Luke; Borthwick, Lee A.; Smith, Allen; Mentink‐Kane, Margaret M.; White, Sandra; Thompson, Robert W.; Cheever, Allen W.; Bock, Kevin W.; Moore, Ian N.; Fitz, Lori; Urban, Joseph F.; Wynn, Thomas A.

doi:10.1038/ni.3417

Cited by 53 publications

(53 citation statements)

References 32 publications

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“…These findings are in contrast to another report demonstrating a lack of effect in AMCase KO mice in the allergic phenotype in either acute or chronic model of dust mite exposure [12]. The mechanism behind these differences are unclear but may involve the fact that one study used an intact but enzymatically inactive AMCase that can still bind chitin [8], versus one in which AMCase protein expression was abolished [12], thus suggesting that while AMCase’s best-known function is to cleave chitin, it may play other roles in chitin biology. Moreover, it is possible that the other active chitinase, chitotriosidase ( CHIT1 ), has a redundant role in the absence of AMCase; its expression was reportedly detected in the lungs of AMCase KO mice [12] but not in AMCase-ED mice [11•].…”

Section: Introductioncontrasting

confidence: 99%

“…The authors claimed that chitin or chitin-containing dust mite extracts activates caspase-1 which in turn activates caspase-7 which then cleaves and inactivates IL-33 thus leading to resolution of type 2 inflammation [11•]. These findings are in contrast to another report demonstrating a lack of effect in AMCase KO mice in the allergic phenotype in either acute or chronic model of dust mite exposure [12]. The mechanism behind these differences are unclear but may involve the fact that one study used an intact but enzymatically inactive AMCase that can still bind chitin [8], versus one in which AMCase protein expression was abolished [12], thus suggesting that while AMCase’s best-known function is to cleave chitin, it may play other roles in chitin biology.…”

Section: Introductionmentioning

confidence: 99%

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Epithelial Cell Regulation of Allergic Diseases

Gour

Lajoie

2016

Curr Allergy Asthma Rep

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Allergic diseases, which have escalated in prevalence in recent years, arise as a result of maladaptive immune responses to ubiquitous environmental stimuli. Why only certain individuals mount inappropriate type 2 immune responses to these otherwise harmless allergens has remained an unanswered question. Mounting evidence suggests that the epithelium, by sensing its environment, is the central regulator of allergic diseases. Once considered to be a passive barrier to allergens, epithelial cells at mucosal surfaces are now considered to be the cornerstone of the allergic diathesis. Beyond their function as maintaining barrier at mucosal surfaces, mucosal epithelial cells through the secretion of mediators like IL-25, IL-33, and TSLP control the fate of downstream allergic immune responses. In this review, we will discuss the advances in recent years regarding the process of allergen recognition and secretion of soluble mediators by epithelial cells that shape the development of the allergic response.

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Section: Introductioncontrasting

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Epithelial Cell Regulation of Allergic Diseases

Gour

Lajoie

2016

Curr Allergy Asthma Rep

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“…Recently, AMCase has been shown to have a critical role in initiating type 2 immunity against the chitin-containing nematode18. Thus, AMCase can function as not only a digestive enzyme but also a part of the host defense against chitin-containing pathogens in the mouse GIT.…”

Section: Discussionmentioning

confidence: 99%

“…AMCase is an important downstream effector of interleukin-13 stimulation in T Helper-2 (Th2) cell-mediated immune responses to ovalbumin, pathogens and parasites917. AMCase also functions as a critical initiator of protective type 2 responses to intestinal nematodes18. In addition, several genetic variants of AMCase are associated with bronchial asthma in humans19202122.…”

mentioning

confidence: 99%

Acidic mammalian chitinase is a proteases-resistant glycosidase in mouse digestive system

Ohno

Kimura

Miyazaki

et al. 2016

Sci Rep

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Chitinases are enzymes that hydrolyze chitin, a polymer of β-1, 4-linked N-acetyl-D-glucosamine (GlcNAc). Chitin has long been considered as a source of dietary fiber that is not digested in the mammalian digestive system. Here, we provide evidence that acidic mammalian chitinase (AMCase) can function as a major digestive enzyme that constitutively degrades chitin substrates and produces (GlcNAc)2 fragments in the mouse gastrointestinal environment. AMCase was resistant to endogenous pepsin C digestion and remained active in the mouse stomach extract at pH 2.0. The AMCase mRNA levels were much higher than those of four major gastric proteins and two housekeeping genes and comparable to the level of pepsinogen C in the mouse stomach tissues. Furthermore, AMCase was expressed in the gastric pepsinogen-synthesizing chief cells. The enzyme was also stable and active in the presence of trypsin and chymotrypsin at pH 7.6, where pepsin C was completely degraded. Mouse AMCase degraded polymeric colloidal and crystalline chitin substrates in the gastrointestinal environments in presence of the proteolytic enzymes. Thus, AMCase can function as a protease-resistant major glycosidase under the conditions of stomach and intestine and degrade chitin substrates to produce (GlcNAc)2, a source of carbon, nitrogen and energy.

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“…Chitin elicits strong type 2 immunity in the lung mucosa, 18,19 and acidic mammalian chitinase, which is predominantly expressed by certain pulmonary 20 and gastrointestinal 21 epithelial cells, is required for optimal protection against both N. brasiliensis and H. polygyrus infections. 22 However, as chitin is also a major part of the fungal cell wall, it alone is an insufficient explanation for the induction of antiparasitic immunity. Given that intestinal nematodes tend to cause more tissue destruction than other pathogens (because of their sheer size and invasiveness), it is perhaps more plausible that type 2 immunity results from combined recognition of both endogenous damage-associated alarmins and worm-derived molecules that become available for uptake after larval molting (including chitin), as well as parasite-derived antigens that are continuously secreted throughout infection.…”

Section: Detectionmentioning

confidence: 99%