Abstract 2221

Poster Board II-198

Background:

Acute graft-versus-host disease (GVHD) was known to be involved in the Th1 cytokine activation and alloreactive T-cell cytotoxicity, while the pathogenesis of chronic GVHD is yet revealed fully although in which Th2 cytokine activation or transforming growth factor (TGF) mediated pathway was suggested to be involved. The current study is a hypothesis generating study in order to identify potential predictive surrogate associated with the risk of acute or chronic GVHD in addition with transplant outcomes after allogeneic hematopoietic stem cell transplantation (HSCT).

Methods:

The current study was performed to identify genetic surrogates predicting the risk of acute / chronic GVHD, relapse free survival, non-relapse mortality and overall survival in 394 pairs transplanted at the Princess Margaret Hospital, Toronto, ON, Canada. In addition, the predictive markers for organ specific incidence of acute / chronic GVHD were also evaluated (i.e. for skin/liver/gut acute GVHD or skin, eye, oral, lung or liver chronic GVHD). Total of 261 single nucleotide polymorphisms (SNPs) in 56 genes were determined for donor/recipients' genotypes using MALDI-TOF based platform, involving in the pathways of 1) cytokines (i.e. IL1A, IL1B and its receptor, IL1R1, IL2 & IL2RA, IL4 & IL4R, IL6 & IL6R, IL8, IL10 & IL10RA, RB, IL12A/BandIL12RB1, IFNG & IFNGR1/2, TNFTI/II/II), 2) NFKB (NFKB1/2/A, NFKBIA/B, IKB, IKK1, IKBKB, RelB), 3) apoptosis (FAS, TRAIL & TRAILR1), 4) endothelium nitric oxide regulation (EDN1, NOS1/2A/3), 5) PDGF (PDGFB/C/D & PDGFRA/B), 6) TGF-β (TGFB1/2 & TGFBR1/2/3, TGFRB1), 7) Toll-like receptor (TLR4/5), 8) NOD2/CARD15 and 9) prostaglandin-endoperoxide synthase (PTGS1/2). The candidate genotypes have been selected by choosing the SNPs in non-synonymous SNPs in exon region with minor allele frequency of > 0.05 to 0.1.

Results:

Followings are the lists of recipients' and donors' genotypes with p-value<0.05 thus associating with clinical outcomes following allogeneic HSCT:

Clinical outcomesRecipients' genotypeDonors' genotype
Acute GVHD FAS, EDN, TGFB1, TNFRI, NFKBIA TNFRI 
Chronic GVHD IL1R, FCRG2A 
Chronic GVHD, skin PDGFC NFKBA, PDGFC 
Chronic GVHD, eye IL6R, PDGFR TGFBR1 
Chronic GVHD, oral IL12R FCRG2A 
Chronic GVHD, lung TGFB1, FAS, RelB IL4R, FAS, TGFB1, IL12B3 
Relapse free survival IL6R NOD2/CARD15, IL6R 
Non-relapse mortality IL2 NOS2, TGFB2 
Overall survival IL2 NOS2, TGFB2, IL1B 
Steroid responsiveness IL4R, PDGFR  
Clinical outcomesRecipients' genotypeDonors' genotype
Acute GVHD FAS, EDN, TGFB1, TNFRI, NFKBIA TNFRI 
Chronic GVHD IL1R, FCRG2A 
Chronic GVHD, skin PDGFC NFKBA, PDGFC 
Chronic GVHD, eye IL6R, PDGFR TGFBR1 
Chronic GVHD, oral IL12R FCRG2A 
Chronic GVHD, lung TGFB1, FAS, RelB IL4R, FAS, TGFB1, IL12B3 
Relapse free survival IL6R NOD2/CARD15, IL6R 
Non-relapse mortality IL2 NOS2, TGFB2 
Overall survival IL2 NOS2, TGFB2, IL1B 
Steroid responsiveness IL4R, PDGFR  

In summary, the risk of chronic GVHD was significantly associated with SNP of the genes involved in the pathway of NFKB, PDGF, TGF-β, and some of cytokines (esp. type II, IL6 & IL4), while that of acute GVHD associates with the genotypes in the pathway of TNF and apoptosis. In addition, survival after allogeneic transplantation was associated with the genotypes in NOS (nitric oxide synthase, endothelial nitric oxide synthesis pathway), IL-2 and TGF pathway.

Conclusion:

Because of complex nature of GVHD pathogenesis, multiple candidate pathway SNPs has been explored targeting SNPs in the pathway of cytokines, NFKB, apoptosis, endothelium nitric oxide regulation, NOD2/CARD15, PDGF, PTGS1/2, TGF-β and TLR. Different involvements were noted of TGF-β, PDGF or NFKB with chronic GVHD versus TNF and apoptosis-associated SNPs with acute GVHD. Further study will help us to reach more clear conclusion which genotype is the predictor of the risk of GVHD.

Disclosures:

No relevant conflicts of interest to declare.

Author notes

*

Asterisk with author names denotes non-ASH members.

Sign in via your Institution