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Insertion Sites in Engrafted Cells Cluster Within a Limited Repertoire of Genomic Areas After Gammaretroviral Vector Gene Therapy

Articolo
Data di Pubblicazione:
2011
Abstract:
Vector-associated side effects in clinical gene therapy have provided insights into the molecular mechanisms of hematopoietic regulation in vivo. Surprisingly, many retrovirus insertion sites (RIS) present in engrafted cells have been found to cluster nonrandomly in close association with specific genes. Our data demonstrate that these genes directly influence the in vivo fate of hematopoietic cell clones. Analysis of insertions thus far has been limited to individual clinical studies. Here, we studied >7,000 insertions retrieved from various studies. More than 40% of all insertions found in engrafted gene-modified cells were clustered in the same genomic areas covering only 0.36% of the genome. Gene classification analyses displayed significant overrepresentation of genes associated with hematopoietic functions and relevance for cell growth and survival in vivo. The similarity of insertion distributions indicates that vector insertions in repopulating cells cluster in predictable patterns. Thus, insertion analyses of preclinical in vitro and murine in vivo studies as well as vector insertion repertoires in clinical trials yielded concerted results and mark a small number of interesting genomic loci and genes that warrants further investigation of the biological consequences of vector insertions.
Tipologia CRIS:
1.1 Articolo in rivista
Elenco autori:
Deichmann, A; Brugman, Mh; Bartholomae, Cc; Schwarzwaelder, K; Verstegen, Mm; Howe, Sj; Arens, A; Ott, Mg; Hoelzer, D; Seger, R; Grez, M; Hacein Bey Abina, S; Cavazzana Calvo, M; Fischer, A; Paruzynski, A; Gabriel, R; Glimm, H; Abel, U; Cattoglio, C; Mavilio, F; Cassani, B; Aiuti, Alessandro; Dunbar, Ce; Baum, C; Gaspar, Hb; Thrasher, Aj; von Kalle, C; Schmidt, M; Wagemaker, G.
Autori di Ateneo:
AIUTI ALESSANDRO
Link alla scheda completa:
https://iris.unisr.it/handle/20.500.11768/11664
Pubblicato in:
MOLECULAR THERAPY
Journal
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