The thymus is the primary organ able to support T cell ontogeny, abrogated in FOXN1(-/-) human athymia. Although evidence indicates that in animal models T lymphocytes may differentiate at extrathymic sites, whether this process is really thymus-independent has still to be clarified. In an athymic FOXN1(-/-) fetus, in which we previously described a total blockage of CD4(+) and partial blockage of CD8(+) cell development, we investigated whether intestine could play a role as extrathymic site of T-lymphopoiesis in humans. We document the presence of few extrathymically developed T lymphocytes and the presence in the intestine of CD3(+) and CD8(+), but not of CD4(+) cells, a few of them exhibiting a CD45RA(+) naïve phenotype. The expression of CD3εεpTα, RAG1 and RAG2 transcripts in the intestine and TCR gene rearrangement was also documented, thus indicating that in humans the partial T cell ontogeny occurring at extrathymic sites is a thymus- and FOXN1-independent process.
Molecular evidence for a thymus-independent partial T cell development in a FOXN1-/- athymic human fetus / Fusco, Anna; Panico, L.; Gorrese, M.; Bianchino, G.; Barone, MARIA VITTORIA; Grieco, V.; Vitiello, L.; D’Assante, R.; Romano, Rosa; Palamaro, Loredana; Scalia, G.; DEL VECCHIO, Luigi; Pignata, Claudio. - In: PLOS ONE. - ISSN 1932-6203. - 8:12(2013), p. e81786. [10.1371/journal.pone.0081786]
Molecular evidence for a thymus-independent partial T cell development in a FOXN1-/- athymic human fetus
FUSCO, ANNA;BARONE, MARIA VITTORIA;D’Assante R.;ROMANO, ROSA;PALAMARO, LOREDANA;DEL VECCHIO, LUIGI;PIGNATA, CLAUDIO
2013
Abstract
The thymus is the primary organ able to support T cell ontogeny, abrogated in FOXN1(-/-) human athymia. Although evidence indicates that in animal models T lymphocytes may differentiate at extrathymic sites, whether this process is really thymus-independent has still to be clarified. In an athymic FOXN1(-/-) fetus, in which we previously described a total blockage of CD4(+) and partial blockage of CD8(+) cell development, we investigated whether intestine could play a role as extrathymic site of T-lymphopoiesis in humans. We document the presence of few extrathymically developed T lymphocytes and the presence in the intestine of CD3(+) and CD8(+), but not of CD4(+) cells, a few of them exhibiting a CD45RA(+) naïve phenotype. The expression of CD3εεpTα, RAG1 and RAG2 transcripts in the intestine and TCR gene rearrangement was also documented, thus indicating that in humans the partial T cell ontogeny occurring at extrathymic sites is a thymus- and FOXN1-independent process.I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.
