Is There an Interplay Between the Functional Domains of IRAP?

Vear, Anika; Gaspari, Tracey; Thompson, Phillip E.; Chai, Siew Yeen

doi:10.3389/fcell.2020.585237

Cited by 6 publications

(5 citation statements)

References 81 publications

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“…Various conformational changes in IRAP induced by ligands are reported [27,28]. Trafficking motifs at the N-terminal domain of IRAP regulate the movement of enzymes within different intracellular compartments [29].…”

Section: Introductionmentioning

confidence: 99%

The Discovery of New Inhibitors of Insulin-Regulated Aminopeptidase by a High-Throughput Screening of 400,000 Drug-like Compounds

Gising,

Honarnejad,

Bras

et al. 2024

IJMS

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With the ambition to identify novel chemical starting points that can be further optimized into small drug-like inhibitors of insulin-regulated aminopeptidase (IRAP) and serve as potential future cognitive enhancers in the clinic, we conducted an ultra-high-throughput screening campaign of a chemically diverse compound library of approximately 400,000 drug-like small molecules. Three biochemical and one biophysical assays were developed to enable large-scale screening and hit triaging. The screening funnel, designed to be compatible with high-density microplates, was established with two enzyme inhibition assays employing either fluorescent or absorbance readouts. As IRAP is a zinc-dependent enzyme, the remaining active compounds were further evaluated in the primary assay, albeit with the addition of zinc ions. Rescreening with zinc confirmed the inhibitory activity for most compounds, emphasizing a zinc-independent mechanism of action. Additionally, target engagement was confirmed using a complementary biophysical thermal shift assay where compounds causing positive/negative thermal shifts were considered genuine binders. Triaging based on biochemical activity, target engagement, and drug-likeness resulted in the selection of 50 qualified hits, of which the IC50 of 32 compounds was below 3.5 µM. Despite hydroxamic acid dominance, diverse chemotypes with biochemical activity and target engagement were discovered, including non-hydroxamic acid compounds. The most potent compound (QHL1) was resynthesized with a confirmed inhibitory IC50 of 320 nM. Amongst these compounds, 20 new compound structure classes were identified, providing many new starting points for the development of unique IRAP inhibitors. Detailed characterization and optimization of lead compounds, considering both hydroxamic acids and other diverse structures, are in progress for further exploration.

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Section: Introductionmentioning

confidence: 99%

The Discovery of New Inhibitors of Insulin-Regulated Aminopeptidase by a High-Throughput Screening of 400,000 Drug-like Compounds

Gising,

Honarnejad,

Bras

et al. 2024

IJMS

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show abstract

“…IRAP instead, thanks to an additional N-terminal cytoplasmic domain, is retained in the endosomal vesicles from where it can traffic to the cell membrane, forming a type II integral membrane glycoprotein [4]. IRAP is a multifaceted protein: it has been shown to be involved in cross-presentation in the endosomes of dendritic cells (DC) and, when in the cell membrane, to catalyze the final step of the angiotensinogen to angiotensin IV (AT4) conversion, being itself a receptor for AT4 [5,6]. In addition, it has been shown to be involved in several other functions, ranging from the insulin metabolic pathway to vesicular trafficking, and has even been present in cognitive processes [7,8].…”

Section: Introductionmentioning

confidence: 99%

A Short ERAP2 That Binds IRAP Is Expressed in Macrophages Independently of Gene Variation

Mattorre

Caristi

Donato

et al. 2022

IJMS

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The M1 zinc metalloproteases ERAP1, ERAP2, and IRAP play a role in HLA-I antigen presentation by refining the peptidome either in the ER (ERAP1 and ERAP2) or in the endosomes (IRAP). They have also been entrusted with other, although less defined, functions such as the regulation of the angiotensin system and blood pressure. In humans, ERAP1 and IRAP are commonly expressed. ERAP2 instead has evolved under balancing selection that maintains two haplotypes, one of which undergoing RNA splicing leading to nonsense-mediated decay and loss of protein. Hence, likewise in rodents, wherein the ERAP2 gene is missing, about a quarter of the human population does not express ERAP2. We report here that macrophages, but not monocytes or other mononuclear blood cells, express and secrete an ERAP2 shorter form independent of the haplotype. The generation of this “short” ERAP2 is due to an autocatalytic cleavage within a distinctive structural motif and requires an acidic micro-environment. Remarkably, ERAP2 “short” binds IRAP and the two molecules are co-expressed in the endosomes as well as in the cell membrane. Of note, the same phenomenon could be observed in some cancer cells. These data prompt us to reconsider the role of ERAP2, which might have been maintained in humans due to fulfilling a relevant function in its “short” form.

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“…IRAP instead, thanks to an additional N-terminal cytoplasmic domain, is retained in the endosomal vesicles from where it can traffic to the cell membrane forming a type II integral membrane glycoprotein (4). IRAP is a multifaceted protein: it has been shown to be involved in cross-presentation in the endosomes of dendritic cells (DC) and, when in the cell membrane, to catalyze the final step of the angiotensinogen to angiotensin IV (AT4) conversion being itself a receptor for AT4 (5,6). In addition, it has been shown to be involved in several other functions, ranging from the insulin metabolic pathway to vesicular trafficking and even in cognitive processes (7,8).…”

Section: Introductionmentioning

confidence: 99%

“…6 cells/ml) in Roswell Park Memorial Institute medium (RPMI 1640, Invitrogen) containing 10% of heat inactivated fetal bovine serum (FBS, Invitrogen) and supplemented with 10 mM Hepes (Gibco, #15630-056), 1 mM pyruvate (Gibco, #11360-039), 2.5 g/l D-glucose (Merck). U937 cells were differentiated to macrophages by 24 h incubation with 20 nM phorbol 12-myristate 13-acetate (PMA, Sigma, P8139) followed by 24 h incubation in RPMI medium.…”

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confidence: 99%

A short ERAP2 that binds IRAP is expressed in macrophages independently from gene variation

Mattorre

Caristi

Donato

et al. 2022

Preprint

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The M1 zinc metalloproteases ERAP1, ERAP2 and IRAP play a role in HLA-I antigen presentation by refining the peptidome either in the ER (ERAP1 and ERAP2) or in the endosomes (IRAP). They have been also entrusted with other, although less defined, functions such as the regulation of the angiotensin system and blood pressure. In humans, ERAP1 and IRAP are commonly expressed. ERAP2 instead has evolved under balancing selection that maintains two haplotypes one of which undergoing RNA splicing leading to nonsense-mediated decay and loss of protein. Hence, likewise in rodents in which the ERAP2 gene is missing, about a quarter of the human population does not express ERAP2. We report here that macrophages, but not monocytes or other mononuclear blood cells, express and secrete an ERAP2 shorter form independently from the haplotype. The generation of this short ERAP2 is due to an autocatalytic cleavage within a distinctive structural motif and requires an acidic microenvironment. Remarkably, this short ERAP2 binds IRAP and the two molecules are co-expressed in the endosomes as well as in the cell membrane. Of note, the same phenomenon could be observed in some cancer cells. These data prompt to reconsider the role of ERAP2 which might have been maintained in humans because fulfilling a relevant function as short form in specialized cells.

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Is There an Interplay Between the Functional Domains of IRAP?

Cited by 6 publications

References 81 publications

The Discovery of New Inhibitors of Insulin-Regulated Aminopeptidase by a High-Throughput Screening of 400,000 Drug-like Compounds

The Discovery of New Inhibitors of Insulin-Regulated Aminopeptidase by a High-Throughput Screening of 400,000 Drug-like Compounds

A Short ERAP2 That Binds IRAP Is Expressed in Macrophages Independently of Gene Variation

A short ERAP2 that binds IRAP is expressed in macrophages independently from gene variation

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