Mesentsefaalse astrotsüütidest pärineva närvikasvufaktori (MANF) interaktsioonid šaperoniga BiP ning madalmolekulaarsete ühenditega

Üha kasvav hulk teadustulemusi viitavad, et MANF ja tema paraloog CDNF on erinevalt teistest närvikasvufaktoritest lokaliseeritud ER-i. Lisaks on MANF-i ekspressioon ja sekretsioon on reguleeritud UPR-i poolt. Seetõttu võib oletada, et MANF-il on bioloogiliselt oluline funktsioon ER-is. Käesoleva uurimistööga selgitati välja, et šaperon BiP-i ja närvikasvufaktori MANF-i vahel toimub otsene interaktsioon afiinsusega KD= 675 ± 38 nM ning see ei ole Ca2+-sõltuv nagu Glembotski koos oma kaastöötajatega 2012. aasta teadusartiklis arvasid, vaid sõltub ATP-st. Lisaks uuriti MANF-i interaktsioone oluliste ER-i madalmolekulaarsete ühenditega - ADP, ATP, AMP-PNP ning Ca2+ ioonidega. Siinses töös kirjeldatud andmed viitavad esmakordselt, et MANF on võimeline siduma nukleotiide, seevastu interaktsioon Ca2+ ioonidega puudub täielikult

CDNF Interacts with ER Chaperones and Requires UPR Sensors to Promote Neuronal Survival

Cerebral dopamine neurotrophic factor (CDNF) is a neurotrophic factor that has beneficial effects on dopamine neurons in both in vitro and in vivo models of Parkinson’s disease (PD). CDNF was recently tested in phase I-II clinical trials for the treatment of PD, but the mechanisms underlying its neuroprotective properties are still poorly understood, although studies have suggested its role in the regulation of endoplasmic reticulum (ER) homeostasis and the unfolded protein response (UPR). The aim of this study was to investigate the mechanism of action of CDNF through analyzing the involvement of UPR signaling in its anti-apoptotic function. We used tunicamycin to induce ER stress in mice in vivo and used cultured primary neurons and found that CDNF expression is regulated by ER stress in vivo and that the involvement of UPR pathways is important for the neuroprotective function of CDNF. Moreover, we used AP-MS and BiFC to perform the first interactome screening for CDNF and report novel binding partners of CDNF. These findings allowed us to hypothesize that CDNF protects neurons from ER-stress-inducing agents by modulating UPR signaling towards cell survival outcomes

The cytoprotective protein MANF promotes neuronal survival independently from its role as a GRP78 cofactor

Mesencephalic astrocyte-derived neurotrophic factor (MANF) is an endoplasmic reticulum (ER)-stress-regulated protein exhibiting cytoprotective properties through a poorly understood mechanism in various in vitro and in vivo models of neuronal and non-neuronal damage. Although initially characterized as a secreted neurotrophic factor for midbrain dopamine neurons, MANF has recently gained more interest for its intracellular role in regulating the ER homeostasis, including serving as a cofactor of the chaperone glucose-regulated protein 78 (GRP78). We aimed for a better understanding of the neuroprotective mechanisms of MANF. Here we show for the first time that MANF promotes the survival of ER-stressed neurons in vitro as a general unfolded protein response (UPR) regulator, affecting several UPR pathways simultaneously. Interestingly, MANF does not affect naive neurons. We hypothesize that MANF regulates UPR signaling toward a mode more compatible with neuronal survival. Screening of MANF interacting proteins from two mammalian cell lines revealed a conserved interactome of 15 proteins including several ER chaperones such as GRP78, GRP170, protein disulfide isomerase family A member 1, and protein disulfide isomerase family A member 6. Further characterization confirmed previously published finding that MANF is a cofactor of GRP78 interacting with its nucleotide binding domain. Using microscale thermophoresis and nuclear magnetic resonance spectroscopy, we discovered that MANF is an ATP binding protein and that ATP blocks the MANF-GRP78 interaction. Interestingly, functional analysis of the antiapoptotic properties of MANF mutants in cultured neurons revealed divergent roles of MANF as a GRP78 cofactor and as an antiapoptotic regulator of UPR. We conclude that the co-factor type interaction with GRP78 is dispensable for the survival-promoting activity of MANF in neurons.Peer reviewe