Graft-versus-Host Disease: Role of Inflammation in the Development of Chromosomal Abnormalities of Keratinocytes

Sloand, Elaine M.; Pfannes, Loretta; Ling, Casey; Feng, Xingmin; Jasek, Monika; Calado, Rodrigo T.; Tucker, Zachary; Hematti, Peiman; Maciejewski, Jaroslaw P.; Dunbar, Cynthia E.; Barrett, John; Young, Neal S.

doi:10.1016/j.bbmt.2010.07.014

Cited by 18 publications

(12 citation statements)

References 46 publications

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“…The rarity of TP53 mutation herein confirms previous findings in three cases of HSCT/SCC showing the absence of TP53 mutation in exons 5-9 (Zhang et al, 2002). Our results in LPLE are also in accordance with an in vitro GVHD model, where keratinocytes showed no mutations in TP53 (Sloand et al, 2010).…”

supporting

confidence: 91%

“…TP53 copy-number alterations, whether TP53 haploinsufficiency or an increased TP53 allele copy number, were found in all LPLE-HSCT/SCC sequences, as described in different malignancies, where TP53 allele deletion can be associated with p53 accumulation without TP53 mutation (Brito-Babapulle et al, 2000;Saeki et al, 2011). These findings are in accordance with the high rate of genomic instability in oral mucosa after HSCT (Khan et al, 2010) and with the common haploinsufficiency for TP53 due to the loss of chromosome 17 in keratinocytes in an in vitro GVHD model (Sloand et al, 2010). Such genomic instability may be due to chronic nitric oxide release and/ or to replication stress.…”

supporting

confidence: 82%

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p53 Phosphorylation and TP53 Copy-Number Alterations in Chronic Graft-Versus-Host Oral Lichen Preceding Squamous Cell Carcinoma

Battistella

Cuccuini

Elbouchtaoui

et al. 2014

Journal of Investigative Dermatology

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knockdown may have altered the immune surveillance milieu in the skin with its complex cytokine patterns and reduced numbers and function of Tregs, thereby leading to the increase of NER mechanisms and subsequent reduction of DNA damage as measured by CPDs (Figure 1c, d, and f). In addition, the CD28 ligands BB-1 and B7 that are expressed in keratinocytes provide an important co-stimulatory signal for CD3mediated proliferation of T lymphocytes, including alloreacting CD4 þ T cells (Koulova et al., 1991; Simon et al., 1994). This raises the possibility that T-cell activation by keratinocytes after UVB exposure may have been inhibited by in vivo CD28 siRNA knockdown. In this regard, it is interesting to note that functional blockade of CD80/CD86 significantly decreased UV-induced tumor development (Loser et al., 2005). In any case, further studies are warranted to determine the precise mechanisms by which CD28 knockdown leads to increased NER and decreased DNA damage and skin alterations.

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supporting

confidence: 91%

supporting

confidence: 82%

p53 Phosphorylation and TP53 Copy-Number Alterations in Chronic Graft-Versus-Host Oral Lichen Preceding Squamous Cell Carcinoma

Battistella

Cuccuini

Elbouchtaoui

et al. 2014

Journal of Investigative Dermatology

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“…In an in vitro mutation analysis system, we found that allostimulated mixed lymphocyte cultures may induce MSI in co-cultured epithelial cells [22]. These results were independently confirmed by subsequent studies from other groups, which reported that the detection of MSI [23] and chromosomal instability [24] in the epithelial tissues of patients after allo-HSCT was correlated to the presence of GvHD inflammation.…”

Section: Introductionsupporting

confidence: 70%

DNA Damage and Repair in Epithelium after Allogeneic Hematopoietic Stem Cell Transplantation

Themeli

Spyridonidis

2012

IJMS

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Allogeneic hematopoietic stem cell transplantation (allo-HSCT) in humans, following hematoablative treatment, results in biological chimeras. In this case, the transplanted hematopoietic, immune cells and their derivatives can be considered the donor genotype, while the other tissues are the recipient genotype. The first sequel, which has been recognized in the development of chimerical organisms after allo-HSCT, is the graft versus host (GvH) reaction, in which the new developed immune cells from the graft recognize the host’s epithelial cells as foreign and mount an inflammatory response to kill them. There is now accumulating evidence that this chronic inflammatory tissue stress may contribute to clinical consequences in the transplant recipient. It has been recently reported that host epithelial tissue acquire genomic alterations and display a mutator phenotype that may be linked to the occurrence of a GvH reaction. The current review discusses existing data on this recently discovered phenomenon and focuses on the possible pathogenesis, clinical significance and therapeutic implications.

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“…34 Surveillance for secondary cutaneous tumors Conditioning regimens and prolonged immunosuppression increases the risk of secondary malignancies of the skin including SCC, basal cell carcinoma, and melanoma. 17,[35][36][37]38 The long-term risk of melanoma in pediatric patients receiving HCT may be associated with a conditioning regimen using high doses of alkylating drugs. 36 Patient age, actinic exposure, skin phototype, and previous ionizing radiation are additional risk factors in the development of nonmelanoma skin cancers after HCT 39,40 (Fig 3).…”

Section: Wound Managementmentioning

confidence: 99%