Tbx1 coordinates addition of posterior second heart field progenitor cells to the arterial and venous poles of the heart.

[22q11.2 deletion syndrome]

Cardiac progenitor cells from the second heart field (SHF ) contribute to rapid growth of the embryonic heart , giving rise to right ventricular and outflow tract (OFT ) myocardium at the arterial pole of the heart , and atrial myocardium at the venous pole . Recent clonal analysis and cell-tracing experiments indicate that a common progenitor pool in the posterior region of the SHF gives rise to both OFT and atrial myocytes . The mechanisms regulating deployment of this progenitor pool remain unknown .To evaluate the role of TBX 1 , the major gene implicated in congenital heart defects in 22 q 11 .2 deletion syndrome patients , in posterior SHF development .Using transcriptome analysis , genetic tracing , and fluorescent dye-labeling experiments , we show that Tbx 1 -dependent OFT myocardium originates in Hox-expressing cells in the posterior SHF . In Tbx 1 null embryos , OFT progenitor cells fail to segregate from this progenitor cell pool , leading to failure to expand the dorsal pericardial wall and altered positioning of the cardiac poles . Unexpectedly , addition of SHF cells to the venous pole of the heart is also impaired , resulting in abnormal development of the dorsal mesenchymal protrusion , and partially penetrant atrioventricular septal defects , including ostium primum defects .Tbx 1 is required for inflow as well as OFT morphogenesis by regulating the segregation and deployment of progenitor cells in the posterior SHF . Our results provide new insights into the pathogenesis of congenital heart defects and 22 q 11 .2 deletion syndrome phenotypes .