Small molecule inhibitors and a kinase-dead expressing mouse model demonstrate that the kinase activity of Chk1 is essential for mouse embryos and cancer cells

Abstract: Chk1 kinase is downstream of the ATR kinase in the sensing of improper replication. Previous cell culture studies have demonstrated that Chk1 is essential for replication and Chk1 inhibitors are efficacious against tumors with high-level replication stress such as Myc-induced lymphoma cells. Treatment with Chk1 inhibitors also combines well with certain chemotherapeutic drugs and effects associates with induction of DNA damage and reduction of Chk1 protein levels. Most studies of Chk1 function has relied on th… Show more

“…CHK1 inhibition causes premature mitosis in both mouse (Ju et al, 2020) and human (Palmerola et al, 2022) zygotes. CHK1 kinase activity itself is necessary for early embryos (Muralidharan et al, 2020). It is also consistent with more other studies in mice and (Fishler et al, 2010; Lam et al, 2004; Niida et al, 2005; Peddibhotla et al, 2009; Ruth et al, 2021), humans (Branigan et al, 2021; Durkin et al, 2006; Niida et al, 2005; Syljuåsen et al, 2005) and other species (Zachos et al, 2007, 2003, 2005).…”

“…CHK1 is activated after replication stress in somatic cells and early embryos (González Besteiro & Gottifredi 2015; Lam et al, 2004; Lebrec et al, 2022; Lemmens et al, 2018; Michelena et al, 2019; Moiseeva et al, 2019; Muralidharan et al, 2020; Palmerola et al, 2022; Syljuåsen et al, 2005; Zachos et al, 2005). Replication stress signalling is usually orchestrated by ATR kinase (Eykelenboom et al, 2013; Saldivar et al, 2018).…”

“…This finding is consistent with other studies (Branigan et al, 2021;Lam et al, 2004), where Chk1 depletion or inhibition causes premature mitosis in cells with only mildly, but not severely, under-replicated DNA. CHK1 is activated after replication stress in somatic cells and early embryos (González Besteiro & Gottifredi 2015;Lam et al, 2004;Lebrec et al, 2022;Lemmens et al, 2018;Michelena et al, 2019;Moiseeva et al, 2019;Muralidharan et al, 2020;Palmerola et al, 2022;Syljuåsen et al, 2005;Zachos et al, 2005). Replication stress signalling is usually orchestrated by ATR kinase (Eykelenboom et al, 2013;Saldivar et al, 2018).…”

“…CHK1 also regulates cell cycle progression during embryonic development in zebrafish (Dalle Nogare et al, 2009; Zhang et al, 2014), Drosophila (Deneke et al, 2016) and Xenopus (Petrus et al, 2004; Shimuta et al, 2002). Moreover, CHK1 inhibition or depletion in human (Palmerola et al, 2022) and mouse embryos (Ju et al, 2020; Liu et al, 2000; Muralidharan et al, 2020; Takai et al, 2000) exacerbates the incidence of aneuploidy and induces genome fragmentation.…”

“…CHK1 also regulates cell cycle progression during embryonic development in zebrafish (Dalle Nogare et al, 2009;Zhang et al, 2014), Drosophila (Deneke et al, 2016) and Xenopus (Petrus et al, 2004;Shimuta et al, 2002). Moreover, CHK1 inhibition or depletion in human (Palmerola et al, 2022) and mouse embryos (Ju et al, 2020;Liu et al, 2000;Muralidharan et al, 2020;Takai et al, 2000) exacerbates the incidence of aneuploidy and induces genome fragmentation. Although the mechanism underlying the role of CHK1 in cell cycle checkpoint signaling is well understood in somatic cells, little is known regarding the function of CHK1 signaling in regulating embryonic cell division and genome integrity in early mammalian embryos.…”

CHK1-CDC25A-CDK1 regulate cell cycle progression in early mouse embryos to protect genome integrity

“…CHK1 inhibition causes premature mitosis in both mouse (Ju et al, 2020) and human (Palmerola et al, 2022) zygotes. CHK1 kinase activity itself is necessary for early embryos (Muralidharan et al, 2020). It is also consistent with more other studies in mice and (Fishler et al, 2010; Lam et al, 2004; Niida et al, 2005; Peddibhotla et al, 2009; Ruth et al, 2021), humans (Branigan et al, 2021; Durkin et al, 2006; Niida et al, 2005; Syljuåsen et al, 2005) and other species (Zachos et al, 2007, 2003, 2005).…”

“…CHK1 is activated after replication stress in somatic cells and early embryos (González Besteiro & Gottifredi 2015; Lam et al, 2004; Lebrec et al, 2022; Lemmens et al, 2018; Michelena et al, 2019; Moiseeva et al, 2019; Muralidharan et al, 2020; Palmerola et al, 2022; Syljuåsen et al, 2005; Zachos et al, 2005). Replication stress signalling is usually orchestrated by ATR kinase (Eykelenboom et al, 2013; Saldivar et al, 2018).…”

“…This finding is consistent with other studies (Branigan et al, 2021;Lam et al, 2004), where Chk1 depletion or inhibition causes premature mitosis in cells with only mildly, but not severely, under-replicated DNA. CHK1 is activated after replication stress in somatic cells and early embryos (González Besteiro & Gottifredi 2015;Lam et al, 2004;Lebrec et al, 2022;Lemmens et al, 2018;Michelena et al, 2019;Moiseeva et al, 2019;Muralidharan et al, 2020;Palmerola et al, 2022;Syljuåsen et al, 2005;Zachos et al, 2005). Replication stress signalling is usually orchestrated by ATR kinase (Eykelenboom et al, 2013;Saldivar et al, 2018).…”

“…CHK1 also regulates cell cycle progression during embryonic development in zebrafish (Dalle Nogare et al, 2009; Zhang et al, 2014), Drosophila (Deneke et al, 2016) and Xenopus (Petrus et al, 2004; Shimuta et al, 2002). Moreover, CHK1 inhibition or depletion in human (Palmerola et al, 2022) and mouse embryos (Ju et al, 2020; Liu et al, 2000; Muralidharan et al, 2020; Takai et al, 2000) exacerbates the incidence of aneuploidy and induces genome fragmentation.…”

“…CHK1 also regulates cell cycle progression during embryonic development in zebrafish (Dalle Nogare et al, 2009;Zhang et al, 2014), Drosophila (Deneke et al, 2016) and Xenopus (Petrus et al, 2004;Shimuta et al, 2002). Moreover, CHK1 inhibition or depletion in human (Palmerola et al, 2022) and mouse embryos (Ju et al, 2020;Liu et al, 2000;Muralidharan et al, 2020;Takai et al, 2000) exacerbates the incidence of aneuploidy and induces genome fragmentation. Although the mechanism underlying the role of CHK1 in cell cycle checkpoint signaling is well understood in somatic cells, little is known regarding the function of CHK1 signaling in regulating embryonic cell division and genome integrity in early mammalian embryos.…”

CHK1-CDC25A-CDK1 regulate cell cycle progression in early mouse embryos to protect genome integrity