TCTP and CSN4 control cell cycle progression and development by regulating CULLIN1 neddylation in plants and animals

Translationally Controlled Tumor Protein (TCTP) controls growth by regulating the G1/S transition during cell cycle progression. Our genetic interaction studies show that TCTP fulfills this role by interacting with CSN4, a subunit of the COP9 Signalosome complex, known to influence CULLIN-RING ubiquitin ligases activity by controlling CULLIN (CUL) neddylation status. In agreement with these data, downregulation of CSN4 in Arabidopsis and in tobacco cells leads to delayed G1/S transition comparable to that observed when TCTP is downregulated. Loss-of-function of AtTCTP leads to increased fraction of deneddylated CUL1, suggesting that AtTCTP interferes negatively with COP9 function. Similar defects in cell proliferation and CUL1 neddylation status were observed in Drosophila knockdown for dCSN4 or dTCTP, respectively, demonstrating a conserved mechanism between plants and animals. Together, our data show that CSN4 is the missing factor linking TCTP to the control of cell cycle progression and cell proliferation during organ development and open perspectives towards understanding TCTP’s role in organ development and disorders associated with TCTP miss-expression.

During organism development, the correct implementation of organs with unique shape, size and function, is the result of coordinated cellular processes, such as cell proliferation and expansion. Deregulation of these processes affect human health and can lead to severe diseases. While plants and animals have largely diverged in several aspects, some biological functions, such as cell proliferation, are conserved between these kingdoms. Previously we reported that the Translationally Controlled Tumor Protein (TCTP), a highly-conserved protein among all eukaryotes, positively regulates cell proliferation and this role is conserved between plants and animals. In agreement with these data, animals TCTP was reported to highly accumulate in tumor cells, and thus represents a target for cancer research and therapies. To discover how TCTP regulates cell proliferation, we conducted studies to identify factors acting in the TCTP pathway. Using the model plant Arabidopsis, we identified that TCTP fulfil its role by interacting with CSN4, a subunit of the conserved COP9 complex. TCTP interferes with the role of COP9 to regulate the downstream complex CRL known to control cell proliferation in eukaryotes. We further demonstrate that this role is conserved in the fly Drosophila, thus corroborating the conservation of TCTP pathway between plants and animals. We believe that, the data here will provide exciting perspectives, beyond plant research, that will help understand developmental disorders associated with TCTP misfunction, such as cancer.