Targeting Toll-like receptor-driven systemic inflammation by engineering an innate structural fold into drugs.
Ganna PetrukManoj PuthiaFirdaus SamsudinJitka PetrlovaFranziska OlmMargareta MittendorferSnejana HyllénDag EdströmAnn-Charlotte StrömdahlCarl DiehlSimon EkströmBjörn WalseSven KjellströmPeter John BondSandra LindstedtArtur SchmidtchenPublished in: Nature communications (2023)
There is a clinical need for conceptually new treatments that target the excessive activation of inflammatory pathways during systemic infection. Thrombin-derived C-terminal peptides (TCPs) are endogenous anti-infective immunomodulators interfering with CD14-mediated TLR-dependent immune responses. Here we describe the development of a peptide-based compound for systemic use, sHVF18, expressing the evolutionarily conserved innate structural fold of natural TCPs. Using a combination of structure- and in silico-based design, nuclear magnetic resonance spectroscopy, biophysics, mass spectrometry, cellular, and in vivo studies, we here elucidate the structure, CD14 interactions, protease stability, transcriptome profiling, and therapeutic efficacy of sHVF18. The designed peptide displays a conformationally stabilized, protease resistant active innate fold and targets the LPS-binding groove of CD14. In vivo, it shows therapeutic efficacy in experimental models of endotoxin shock in mice and pigs and increases survival in mouse models of systemic polymicrobial infection. The results provide a drug class based on Nature´s own anti-infective principles.
Keyphrases
- immune response
- toll like receptor
- inflammatory response
- nuclear factor
- mass spectrometry
- dendritic cells
- nk cells
- mouse model
- single cell
- transcription factor
- oxidative stress
- drug induced
- cancer therapy
- emergency department
- rna seq
- gene expression
- weight gain
- genome wide
- body mass index
- anti inflammatory
- adipose tissue
- high performance liquid chromatography
- drug delivery
- dna methylation
- ms ms
- weight loss