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Sequence-specific activation of the DNA sensor cGAS by Y-form DNA structures as found in primary HIV-1 cDNA

Authors :
Cristina Amparo Hagmann
Janos Ludwig
Tsan Sam Xiao
Thomas Gramberg
Veit Hornung
Damian Ackermann
Sabine Wittmann
Marion Goldeck
Thomas Zillinger
Liudmila Andreeva
Martin Schlee
Anna-Maria Herzner
Christoph Coch
Kirsten Kübler
Karl-Peter Hopfner
Tengchuan Jin
Winfried Barchet
Eva Bartok
Steven Wolter
Christina Mertens
Gunther Hartmann
Source :
Nature immunology. 16(10)
Publication Year :
2014

Abstract

Cytosolic DNA that emerges during infection with a retrovirus or DNA virus triggers antiviral type I interferon responses. So far, only double-stranded DNA (dsDNA) over 40 base pairs (bp) in length has been considered immunostimulatory. Here we found that unpaired DNA nucleotides flanking short base-paired DNA stretches, as in stem-loop structures of single-stranded DNA (ssDNA) derived from human immunodeficiency virus type 1 (HIV-1), activated the type I interferon-inducing DNA sensor cGAS in a sequence-dependent manner. DNA structures containing unpaired guanosines flanking short (12- to 20-bp) dsDNA (Y-form DNA) were highly stimulatory and specifically enhanced the enzymatic activity of cGAS. Furthermore, we found that primary HIV-1 reverse transcripts represented the predominant viral cytosolic DNA species during early infection of macrophages and that these ssDNAs were highly immunostimulatory. Collectively, our study identifies unpaired guanosines in Y-form DNA as a highly active, minimal cGAS recognition motif that enables detection of HIV-1 ssDNA.

Details

ISSN :
15292916
Volume :
16
Issue :
10
Database :
OpenAIRE
Journal :
Nature immunology
Accession number :
edsair.doi.dedup.....a4b56157151d7ded797019c9ce471caa