Scientific Reports (May 2024)
Conditional disruption of Nr5a1 directed by Sox9-Cre impairs adrenal development
Abstract
Abstract The current study aimed to investigate the effect of Sox9-Cre-directed Nr5a1-conditional knockout (Sox9-Cre;Nr5a1 flox/flox ) on adrenal development. We showed that SOX9 is expressed by adrenocortical cells at E10.5–E11.5 but is extinguished no later than E12.5. The number of adrenocortical cells significantly reduced in Sox9-Cre;Nr5a1 flox/flox mice while the number of cleaved caspase 3-positive cells increased compared to that in the controls at E11.5–E12.5, when the adrenal primordium (AP) is about to expand. This indicated that fetal adrenocortical cells are lost via apoptosis due to Nr5a1 ablation by E12.5. Both medulla formation and encapsulation were perturbed, accompanied by a smaller AP size, in Sox9-Cre;Nr5a1 flox/flox mice during embryonic development. Adult Sox9-Cre;Nr5a1 flox/flox adrenals were hypoplastic and exhibited irregular organization of the medulla with aberrant sex differentiation in the X zone. Additionally, there were histologically eosin-negative vacuolated cells, which were negative for both the X-zone marker 20αHSD and the steroidogenesis marker 3βHSD at the innermost cortex of Sox9-Cre;Nr5a1 flox/flox adrenals. Although Nr5a1 +/− adrenals were hypoplastic, a small number of chromaffin cells were properly located in the center, having normal sex differences in the X-zone. The results collectively provided in-vivo evidence that Nr5a1 plays a critical role in AP expansion and subsequent adrenal development.
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