MAPPIT: a versatile tool to study cytokine receptor signalling

Lemmens, Irma; Lievens, Sam; Tavernier, Jan

doi:10.1042/bst0361448

Cited by 4 publications

(1 citation statement)

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“…In addition, several new approaches have emerged as powerful tools to map PPIs, including MAPPIT, luminescencebased mammalian interactome and protein-fragment complementation assay. These technologies allow discovering true interactions with true biological meaning in true physiological context, such as modification-independent and phosphorylation-dependent interactions, induced and constitutive PPIs in mammalian cells [127]. These emerging technologies combined with modern bioinformatics will be utilized to establish HBx-interactome and search therapeutic blockers of abnormal PPIs.…”

Section: Five-year Viewmentioning

confidence: 99%

Using proteomics to identify the HBx interactome in hepatitis B virus: how can this inform the clinic?

Xie

Chen

Zhang

et al. 2013

Expert Review of Proteomics

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Hepatitis B virus (HBV) is a small and enveloped DNA virus, of which chronic infection is the main risk factor of liver cirrhosis and hepatocellular carcinoma. Hepatitis B virus X protein (HBx) is a multifunctional protein encoded by HBV genome, which have significant effects on HBV replication and pathogenesis. Through directly interacting with cellular proteins, HBx is capable to promote HBV replication, regulate transcription of host genes, disrupt protein degradation, modulate signaling pathway, manipulate cell death and deregulate cell cycle. In this review, we briefly discuss the diversified effects of HBx-interactome and their potential clinical significances.

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Section: Five-year Viewmentioning

confidence: 99%

Using proteomics to identify the HBx interactome in hepatitis B virus: how can this inform the clinic?

Xie

Chen

Zhang

et al. 2013

Expert Review of Proteomics

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MAPPIT, a Mammalian Two-Hybrid Method for In-Cell Detection of Protein-Protein Interactions

Lemmens

Lievens

Tavernier

2015

Methods in Molecular Biology

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MAPPIT (MAmmalian Protein-Protein Interaction Trap) is a two-hybrid technology that facilitates the detection and analysis of interactions between proteins in living mammalian cells. The system is based on type 1 cytokine receptor signaling. The bait protein of interest is fused to a chimeric signaling-deficient cytokine receptor, the signaling competence of which is restored upon recruitment of a prey protein that is coupled to a functional cytokine receptor domain. MAPPIT exhibits an excellent signal-to-noise ratio, detects a wide variety of protein-protein interactions (PPIs) including transient and indirect interactions, and has been shown to be highly complementary to other two-hybrid methods with respect to the interactions it can detect. Variants of the method were developed to allow large-scale PPI screening, mapping of protein interaction interfaces, PPI inhibitor screening and drug profiling. This chapter describes a basic 4-day MAPPIT protocol for the analysis of interaction between two designated proteins.

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