Zebrafish Klf11b is Required to Maintain Cell Viability by Inhibiting p53-Mediated Apoptosis

Hee Jeong Kong; Jung Jin Lee; Ju-Won Kim; Julan Kim; Young-Ok Kim; Sang-Yeob Yeo

doi:10.12717/DR.2022.26.2.79

Zebrafish Klf11b is Required to Maintain Cell Viability by Inhibiting p53-Mediated Apoptosis

Dev Reprod. 2022 Jun;26(2):79-90. doi: 10.12717/DR.2022.26.2.79. Epub 2022 Jun 30.

Authors

Hee Jeong Kong¹, Jung Jin Lee², Ju-Won Kim¹, Julan Kim¹, Young-Ok Kim¹, Sang-Yeob Yeo²

Affiliations

¹ Biotechnology Research Division, National Institute of Fisheries Science, Busan 46083, Korea.
² Dept. of Chemical and Biological Engineering, Hanbat National University, Daejeon 34158, Korea.

Abstract

Krüppel-like factor 10 (KLF10) regulates various cellular functions, such as proliferation, differentiation and apoptosis, as well as the homeostasis of several types of tissue. In the present study, we attempted a loss-of-function analysis of zebrafish Klf11a and Klf11b, which constitute human KLF10 homologs. Embryos injected with klf11b-morpholino (MO) showed developmental retardation and cell death, whereas klf11a-MO-injected embryos showed normal development. In klf11b-MO-injected embryos, a dramatic increase in the amount of zebrafish p53 mRNA might be the cause of the increase in that of bax. The degree of apoptosis decreased in the klf11b-MO and p53-MO co-injected embryos. These findings imply that KLF10 is a negative regulator of p53-dependent transcription, suggesting that the KLF10/p53 complex may play an important role in apoptosis for maintenance of tissue homeostasis during embryonic development.

Keywords: Klf11b; Krüppel-like factor 10 (KLF10); Zebrafish; p53.