MCL1 binding to the reverse BH3 motif of P18INK4C couples cell survival to cell proliferation

Abstract: Commitment to cell cycle entry and cellular duplication is a tightly coordinated and regulated process. Once initiated, a series of multiple checkpoints ensure both accurate genomic replication and chromosomal separation. In the event of unsuccessful cell division, parallel pathways exist that induce the cell to undergo programmed cell death, or apoptosis. At the center of such stress-induced, intrinsic apoptotic regulation lies the BCL2 family of pro-and antiapoptotic regulatory proteins. In a proliferative s… Show more

“…Here, we establish a unique function of MCL1 in transcriptional regulation that has never been previously described. As this is the second account of an rBH3-mediated interaction with MCL1, our work provides further validation that the rBH3 motif is a biologically relevant and available mechanism for mediating interactions between the Bcl-2 family and other protein signaling networks 11,12 . By characterizing these rBH3-mediated interactions, we gain a better understanding of the core homeostatic mechanisms regulating MCL1.…”

“…These findings support and expand on the role that the rBH3 motif plays in extending MCL1 function in cells. Recently, we published a study showing that MCL1 directly modulates protein stability of the cell cycle regulator P18 through a homologous rBH3-mediated interaction 12 . Our work here provides further evidence that the rBH3 motif is capable of mediating interactions with MCL1 and implies other rBH3-containing proteins should be explored.…”

“…In addition to several DNA damage response studies, nuclear MCL1 has also been implicated in cell cycle regulation 12 , 37 , 59 . In 2000, Fujise and colleagues identified that MCL1 interacts with proliferating cell nuclear antigen (PCNA) in the nucleus to regulate cell cycle progression through S-phase.…”

“…To study the p73 TD , we synthesized a corresponding 23 amino acid peptide (p73 23mer ) that parallels the homologous BH3 peptides used for other Bcl-2 family binding studies 12,25,26 (Table 2). Through an N-terminally labeled FITC-p73 23mer peptide, we determined that p73 binds MCL1 with a K D that is ≤5 nM (limit of detection for our probe) (Fig.…”

“…Therefore, we refer to these sequences as having a reverse-BH3 or rBH3 motif. Using BLAST sequence analysis of the human proteome, we identified a series of native proteins that contain rBH3-like sequences, thereby establishing a pool of potential novel MCL1-binding partners 11,12 .…”

MCL1 binds and negatively regulates the transcriptional function of tumor suppressor p73

“…Here, we establish a unique function of MCL1 in transcriptional regulation that has never been previously described. As this is the second account of an rBH3-mediated interaction with MCL1, our work provides further validation that the rBH3 motif is a biologically relevant and available mechanism for mediating interactions between the Bcl-2 family and other protein signaling networks 11,12 . By characterizing these rBH3-mediated interactions, we gain a better understanding of the core homeostatic mechanisms regulating MCL1.…”

“…These findings support and expand on the role that the rBH3 motif plays in extending MCL1 function in cells. Recently, we published a study showing that MCL1 directly modulates protein stability of the cell cycle regulator P18 through a homologous rBH3-mediated interaction 12 . Our work here provides further evidence that the rBH3 motif is capable of mediating interactions with MCL1 and implies other rBH3-containing proteins should be explored.…”

“…In addition to several DNA damage response studies, nuclear MCL1 has also been implicated in cell cycle regulation 12 , 37 , 59 . In 2000, Fujise and colleagues identified that MCL1 interacts with proliferating cell nuclear antigen (PCNA) in the nucleus to regulate cell cycle progression through S-phase.…”

“…To study the p73 TD , we synthesized a corresponding 23 amino acid peptide (p73 23mer ) that parallels the homologous BH3 peptides used for other Bcl-2 family binding studies 12,25,26 (Table 2). Through an N-terminally labeled FITC-p73 23mer peptide, we determined that p73 binds MCL1 with a K D that is ≤5 nM (limit of detection for our probe) (Fig.…”

“…Therefore, we refer to these sequences as having a reverse-BH3 or rBH3 motif. Using BLAST sequence analysis of the human proteome, we identified a series of native proteins that contain rBH3-like sequences, thereby establishing a pool of potential novel MCL1-binding partners 11,12 .…”

MCL1 binds and negatively regulates the transcriptional function of tumor suppressor p73

MCL1 alternative polyadenylation is essential for cell survival and mitochondria morphology

FOXO1 represses MCL1 transcription to regulate the function of vascular smooth muscle cells in intracranial aneurysm