Crohn’s disease as an immunodeficiency

Hayee, Bu’Hussain; Rahman, Farooq; Sewell, Gavin W.; Smith, Andrew M.; Segal, Anthony W.

doi:10.1586/eci.10.32

Cited by 21 publications

(20 citation statements)

References 138 publications

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“…Mechanisms to both eliminate microbes and resolve infection by returning the immune system to basal activity are necessary to maintain an adequate and balanced immune response [1,2]. Alterations in these responses can lead to immune deficiency or auto-inflammation [3–5]. Yet, to date, how these mechanisms are coordinated upon infection remains unclear.…”

Section: Introductionmentioning

confidence: 99%

The Drosophila CD36 Homologue croquemort Is Required to Maintain Immune and Gut Homeostasis during Development and Aging

et al. 2016

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Phagocytosis is an ancient mechanism central to both tissue homeostasis and immune defense. Both the identity of the receptors that mediate bacterial phagocytosis and the nature of the interactions between phagocytosis and other defense mechanisms remain elusive. Here, we report that Croquemort (Crq), a Drosophila member of the CD36 family of scavenger receptors, is required for microbial phagocytosis and efficient bacterial clearance. Flies mutant for crq are susceptible to environmental microbes during development and succumb to a variety of microbial infections as adults. Crq acts parallel to the Toll and Imd pathways to eliminate bacteria via phagocytosis. crq mutant flies exhibit enhanced and prolonged immune and cytokine induction accompanied by premature gut dysplasia and decreased lifespan. The chronic state of immune activation in crq mutant flies is further regulated by negative regulators of the Imd pathway. Altogether, our data demonstrate that Crq plays a key role in maintaining immune and organismal homeostasis.

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Section: Introductionmentioning

confidence: 99%

The Drosophila CD36 Homologue croquemort Is Required to Maintain Immune and Gut Homeostasis during Development and Aging

et al. 2016

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“…The lack of an initial acute inflammation with the reduced elimination of foreign material and bacteria may result in a chronic inflammation with T cell mediated granuloma formation, which are supposed to confine hazardous material and protect the intestine from bacterial spreading [25,26]. The development of a Chronlike enterocolitis in CGD supports the theory that also the classical form of IBD, as Chron's disease, may be an immunodeficiency due to malfunction of macrophages and impaired pro-inflammatory responses [27]. The continuous secretion of pro-inflammatory cytokines by cells like macrophages that form the granuloma, sustains the chronic inflammation and finally results in extensive tissue damage.…”

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confidence: 76%

New frontiers in primary immunodeficiency disorders: immunology and beyond…

Gambineri

2011

Cell. Mol. Life Sci.

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“…These findings may make miltefosine an attractive candidate for the treatment of IBD. Although the cause of IBD remains unclear, there are many indications that suggest that a reduced function of the innate immune system predisposes to an excessive response of the adaptive immune response to intestinal microbiota (Marks et al, 2006;Hayee et al, 2010;Uhlig, 2013). Given the results discussed above, miltefosine may have a dual therapeutic effect in IBD by both stimulating macrophagemediated innate immunity and reducing excessive activation of T cell-mediated adaptive immunity.…”

Section: Inhibitory Effects On the Adaptive Immune Responsementioning

confidence: 99%

Repurposing Miltefosine for the Treatment of Immune-Mediated Disease?

Verhaar

Wildenberg

Peppelenbosch

et al. 2014

J Pharmacol Exp Ther

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Miltefosine is an ether lipid that was initially developed for cancer treatment in the early 1980s. Miltefosine largely failed development for oncology, although it was approved for the topical treatment of breast cancer metastasis. It was subsequently discovered that miltefosine is a highly effective treatment of visceral Leishmaniasis, a parasitic disease that affects millions worldwide and causes an estimated 30,000 fatalities each year. Oral treatment with miltefosine is generally well tolerated and has relatively few adverse effects. The exact mechanism of action of miltefosine treatment is still under investigation. Its close resemblance to phospholipids allows it to be quickly taken up by cell membranes and affect related processes, such as lipid metabolism and signaling through lipid rafts. These processes play an important role in the immune response and it comes as no surprise that miltefosine has been successfully tested for the treatment of a number of immune-mediated diseases in preclinical models of disease. Drug repurposing of miltefosine for immunemediated diseases may provide an opportunity to expand the limited number of drugs that are currently available for therapeutic use.

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Crohn’s disease as an immunodeficiency

Cited by 21 publications

References 138 publications

The Drosophila CD36 Homologue croquemort Is Required to Maintain Immune and Gut Homeostasis during Development and Aging

The Drosophila CD36 Homologue croquemort Is Required to Maintain Immune and Gut Homeostasis during Development and Aging

New frontiers in primary immunodeficiency disorders: immunology and beyond…

Repurposing Miltefosine for the Treatment of Immune-Mediated Disease?

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