Interference of the viral effector proteins pp71 and IE1 with ND10-mediated intrinsic immunity against human cytomegalovirus infections (B03)

Subject Area Virology

Term from 2009 to 2017

Project identifier Deutsche Forschungsgemeinschaft (DFG) - Project number 52732026

Project Description

We have demonstrated that a specific organelle of the cell nucleus, termed PML nuclear body (PML-NB), is modified by viral effector proteins such as the pp71- or IE1-protein of human cytomegalovirus. This correlates with antagonization of a direct repressive function of PML-NB components that act as cellular restriction factors. Recent studies reveal an emerging role of PML-NBs as co-regulatory structures of further innate responses (e.g. IFN pathway). This proposal investigates how IE1 and pp71 are able to evade intrinsic and innate immune responses particularly governed by TRIM factors.

DFG Programme Collaborative Research Centres

Subproject of SFB 796: Reprogramming of Host Cells by Microbial Effectors

Applicant Institution Friedrich-Alexander-Universität Erlangen-Nürnberg

Project Head Professor Dr. Thomas Stamminger

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Interference of the viral effector proteins pp71 and IE1 with ND10-mediated intrinsic immunity against human cytomegalovirus infections (B03)

Additional Information

Servicenavigation

Hauptnavigation

Interference of the viral effector proteins pp71 and IE1 with ND10-mediated intrinsic immunity against human cytomegalovirus infections (B03)

Additional Information

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