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72 research outputs found

Unconventional secretion by autophagosome exocytosis

Author: Anjard
Duran
Itoh
Keller
Kinseth
Kuchler
Manjithaya
McGrath
Nickel
Schotman
Simons
Suzanne R. Pfeffer
Théry
Xie
Publication venue: The Rockefeller University Press
Publication date
Field of study

In this issue, Duran et al. (2010. J. Cell Biol. doi: 10.1083/jcb.200911154) and Manjithaya et al. (2010. J. Cell Biol. doi: 10.1083/jcb.200911149) use yeast genetics to reveal a role for autophagosome intermediates in the unconventional secretion of an acyl coenzyme A (CoA)–binding protein that lacks an endoplasmic reticulum signal sequence. Medium-chain acyl CoAs are also required and may be important for substrate routing to this pathway

Crossref

PubMed Central

α-Synuclein impairs macroautophagy: implications for Parkinson’s disease

Author: Abraham Acevedo-Arozena
Allan
Alvarez
Andrew A. Peden
Ashley R. Winslow
Axe
Bolte
Brinda Ravikumar
Cahir J. O’Kane
Chien-Wen Chen
Cookson
Cooper
Cuervo
David C. Rubinsztein
David E. Gordon
Duran
Dyllick-Brenzinger
Feany
Fiona M. Menzies
Franceschini
Fujita
Furlong
Gidalevitz
Gitler
Hamasaki
Ishihara
Jackson
Kabeya
Kihara
Klionsky
Komatsu
Kuma
Maier
Maike Lichtenberg
Manjithaya
Martinez-Vicente
Massey
McNaught
McNaught
Motley
Ravikumar
Ravikumar
Ravikumar
Ravikumar
Reggiori
Rivera
Ross
Rubinsztein
Ryder
Sara Imarisio
Sarkar
Silvia Corrochano
Snyder
Steve Brown
Suzuki
Tisdale
Tsukamoto
Twig
Yen
Young
Zhang
Zhang
Publication venue: The Rockefeller University Press
Publication date: 20/09/2010
Field of study

α-Synuclein impairs autophagosome formation and mislocalizes Atg9 by inhibiting Rab1a

Crossref

PubMed Central

White Rose Research Online

Pro-autophagic signal induction by bacterial pore-forming toxins

Pore-forming toxins (PFT) comprise a large, structurally heterogeneous group of bacterial protein toxins. Nucleated target cells mount complex responses which allow them to survive moderate membrane damage by PFT. Autophagy has recently been implicated in responses to various PFT, but how this process is triggered is not known, and the significance of the phenomenon is not understood. Here, we show that S. aureus α-toxin, Vibrio cholerae cytolysin, streptolysin O and E. coli haemolysin activate two pathways leading to autophagy. The first pathway is triggered via AMP-activated protein kinase (AMPK). AMPK is a major energy sensor which induces autophagy by inhibiting the target of rapamycin complex 1 (TORC1) in response to a drop of the cellular ATP/AMP-ratio, as is also observed in response to membrane perforation. The second pathway is activated by the conserved eIF2α-kinase GCN2, which causes global translational arrest and promotes autophagy in response to starvation. The latter could be accounted for by impaired amino acid transport into target cells. Notably, PKR, an eIF2α-kinase which has been implicated in autophagy induction during viral infection, was also activated upon membrane perforation, and evidence was obtained that phosphorylation of eIF2α is required for the accumulation of autophagosomes in α-toxin-treated cells. Treatment with 3-methyl-adenine inhibited autophagy and disrupted the ability of cells to recover from sublethal attack by S. aureus α-toxin. We propose that PFT induce pro-autophagic signals through membrane perforation–dependent nutrient and energy depletion, and that an important function of autophagy in this context is to maintain metabolic homoeostasis

Crossref

Springer - Publisher Connector

PubMed Central

Up-regulated expression of LAMP2 and autophagy activity during neuroendocrine differentiation of prostate cancer LNCaP cells

Neuroendocrine (NE) prostate cancer (PCa) is a highly aggressive subtype of prostate cancer associated with resistance to androgen ablation therapy. In this study, we used LNCaP prostate cancer cells cultured in a serum-free medium for 6 days as a NE model of prostate cancer. Serum deprivation increased the expression of NE markers such as neuron-specific enolase (NSE) and βIII tubulin (βIII tub) and decreased the expression of the androgen receptor protein in LNCaP cells. Using cDNA microarrays, we compared gene expression profiles of NE cells and non-differentiated LNCaP cells. We identified up-regulation of 155 genes, among them LAMP2, a lysosomal membrane protein involved in lysosomal stability and autophagy. We then confirmed up-regulation of LAMP2 in NE cells by qRT-PCR, Western blot and confocal microscopy assays, showing that mRNA up-regulation correlated with increased levels of LAMP2 protein. Subsequently, we determined autophagy activity in NE cells by assessing the protein levels of SQSTM/p62 and LC3 by Western blot and LC3 and Atg5 mRNAs content by qRT-PCR. The decreased levels of SQSTM/p62 was accompanied by an enhanced expression of LC3 and ATG5, suggesting activation of autophagy in NE cells. Blockage of autophagy with 1μM AKT inhibitor IV, or by silencing Beclin 1 and Atg5, prevented NE cell differentiation, as revealed by decreased levels of the NE markers. In addition, AKT inhibitor IV as well as Beclin1 and Atg5 kwockdown attenuated LAMP2 expression in NE cells. On the other hand, LAMP2 knockdown by siRNA led to a marked blockage of autophagy, prevention of NE differentiation and decrease of cell survival. Taken together, these results suggest that LAMP2 overexpression assists NE differentiation of LNCaP cells induced by serum deprivation and facilitates autophagy activity in order to attain the NE phenotype and cell survival. LAMP2 could thus be a potential biomarker and potential target for NE prostate cancer

Crossref

Directory of Open Access Journals

PubMed Central

University of Dundee Online Publications

FigShare

Guidelines for the use and interpretation of assays for monitoring autophagy (4th edition)

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A. C. Ma
A. K. Au
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Abudu Y. P.
Acevedo-Arozena A.
Adamopoulos I. E.
Adeli K.
Adolph T. E.
Adornetto A.
Aflaki E.
Agam G.
Agarwal A.
Aggarwal B. B.
Agnello M.
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Al-Abd A. M.
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Al-Gharaibeh A.
Alaoui-Jamali M. A.
Alberti S.
Alcocer-Gomez E.
Alessandri C.
Ali M.
Alim Al-Bari M. A.
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Alizadeh J.
Almacellas E.
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Alvarez E. M. C.
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Publication venue: 'Informa UK Limited'
Publication date: 01/01/2021
Field of study

Institutional Research Information System University of Turin

Guidelines for the use and interpretation of assays for monitoring autophagy (4th edition)1.

Author: Abdel-Aziz AK
Abdelfatah S
Abdellatif M
Abdoli A
Abel S
Abeliovich H
Abildgaard MH
Abudu YP
Acevedo-Arozena A
Adamopoulos IE
Adeli K
Adolph TE
Adornetto A
Aflaki E
Agam G
Agarwal A
Aggarwal BB
Agnello M
Agostinis P
Agrewala JN
Agrotis A
Aguilar PV
Ahmad ST
Ahmed ZM
Ahumada-Castro U
Aits S
Aizawa S
Akkoc Y
Akoumianaki T
Akpinar HA
Al-Abd AM
Al-Akra L
Al-Gharaibeh A
Alaoui-Jamali MA
Alberti S
Alcocer-Gómez E
Alessandri C
Ali M
Alim Al-Bari MA
Aliwaini S
Alizadeh J
Almacellas E
Almasan A
Alonso A
Alonso GD
Altan-Bonnet N
Altieri DC
Alves da Costa C
Alves S
Alzaharna MM
Amadio M
Amantini C
Amaral C
Ambrosio S
Amer AO
Ammanathan V
An Z
Andersen SU
Andrabi SA
Andrade-Silva M
Andres AM
Angelini S
Ann D
Anozie UC
Ansari MY
Antas P
Antebi A
Antón Z
Anwar T
Apetoh L
Apostolova N
Araki T
Araki Y
Arasaki K
Araya J
Araújo WL
Arden C
Arguelles S
Arias E
Arikkath J
Arimoto H
Ariosa AR
Armstrong-James D
Arnauné-Pelloquin L
Aroca A
Arroyo DS
Arsov I
Artero R
Arévalo M-A
Asaro DML
Aschner M
Ashrafizadeh M
Ashur-Fabian O
Atanasov AG
Au AK
Auberger P
Auner HW
Aurelian L
Autelli R
Avagliano L
Aveic S
Aveleira CA
Avin-Wittenberg T
Aydin Y
Ayton S
Ayyadevara S
Azzopardi M
Baba M
Backer JM
Backues SK
Bae D-H
Bae O-N
Bae SH
Baehrecke EH
Baek A
Baek S-H
Baek SH
Bagetta G
Bagniewska-Zadworna A
Bai H
Bai J
Bai X
Bai Y
Bairagi N
Baksi S
Balazadeh S
Balbi T
Baldari CT
Balduini W
Ballabio A
Ballester M
Balzan R
Bandopadhyay R
Banerjee S
Banerjee S
Bao Y
Baptista MS
Baracca A
Barbati C
Bargiela A
Barilà D
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Brackney DE
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Bravo-San Pedro JM
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Campbell-Valois F-X
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Camuzard O
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Candido de Almeida D
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Caniggia I
Canonico B
Cantí C
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Caraglia M
Caramés B
Carchman EH
Cardenal-Muñoz E
Cardenas C
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Carew JS
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Carmona-Gutierrez D
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Castro-Obregon S
Catz SD
Cavadas C
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Cavinato M
Cayuela ML
Cebollada Rica P
Cecarini V
Cecconi F
Cechowska-Pasko M
Cenci S
Ceperuelo-Mallafré V
Cerqueira JJ
Cerutti JM
Cervia D
Cetintas VB
Cetrullo S
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Chan DW
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Chan EYW
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Chan MTV
Chan YS
Chandra PK
Chang C
Chang C-P
Chang H-C
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Chao J
Chapman T
Charlet-Berguerand N
Chatterjee S
Chaube SK
Chaudhary A
Chauhan S
Chaum E
Checler F
Cheetham ME
Chen C-S
Chen G-C
Chen J-F
Chen L
Chen L
Chen LL
Chen M
Chen M-K
Chen N
Chen Q
Chen R-H
Chen S
Chen W
Chen W
Chen X
Chen X-M
Chen X-W
Chen Y
Chen Y
Chen Y
Chen Y-G
Chen Y-J
Chen Y-Q
Chen Z
Chen Z
Chen Z
Chen Z-H
Chen ZJ
Chen ZS
Cheng H
Cheng J
Cheng S-Y
Cheng W
Cheng X
Cheng X-T
Cheng Y
Cheng Z
Cheong H
Cheong JK
Chernyak BV
Cherry S
Cheung CFR
Cheung CHA
Cheung K-H
Chevet E
Chi RJ
Chiang AKS
Chiaradonna F
Chiarelli R
Chiariello M
Chica N
Chiocca S
Chiong M
Chiou S-H
Chiramel AI
Chiurchiù V
Cho D-H
Choe S-K
Choi AMK
Choi ME
Choudhury KR
Chow NS
Chu CT
Chua JJE
Chua JP
Chung H
Chung KP
Chung S
Chung S-H
Chung Y-L
Cianfanelli V
Ciechomska IA
Cifuentes M
Cinque L
Cirak S
Cirone M
Clague MJ
Clarke R
Clementi E
Coccia EM
Codogno P
Cohen E
Cohen MM
Colasanti T
Colasuonno F
Colbert RA
Colell A
Coll NS
Collins MO
Colombo MI
Colón-Ramos DA
Combaret L
Comincini S
Cominetti MR
Consiglio A
Conte A
Conti F
Contu VR
Cookson MR
Coombs KM
Coppens I
Corasaniti MT
Cordes N
Corkery DP
Cortese K
Costa MDC
Costantino S
Costelli P
Coto-Montes A
Crack PJ
Crespo JL
Criollo A
Crippa V
Cristofani R
Csizmadia T
Cuadrado A
Cui B
Cui J
Cui Y
Cui Y
Culetto E
Cumino AC
Cybulsky AV
Czaja MJ
Czuczwar SJ
D'Adamo S
D'Amelio M
D'Arcangelo D
D'Lugos AC
D'Orazi G
da Silva JA
Dafsari HS
Dagda RK
Dagdas Y
Daglia M
Dai X
Dai Y
Dai Y
Dal Col J
Dalhaimer P
Dalla Valle L
Dallenga T
Dalmasso G
Damme M
Dando I
Dantuma NP
Darling AL
Das H
Dasarathy S
Dasari SK
Dash S
Daumke O
Dauphinee AN
Davies JS
Davis RJ
Davis T
Dayalan Naidu S
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De Felice F
De Franceschi L
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de Mattos Barbosa MG
De Meyer GRY
De Milito A
De Nunzio C
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De Zio D
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DeBosch BJ
Decuypere J-P
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DeGregori J
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Delaney JR
Delbridge LMD
Delorme-Axford E
Delpino MV
Demarchi F
Dembitz V
Demers ND
Deng H
Deng Z
Dengjel J
Dent P
Denton D
DePamphilis ML
Der CJ
Deretic V
Descoteaux A
Devis L
Devkota S
Devuyst O
Dewson G
Dharmasivam M
Dhiman R
di Bernardo D
Di Cristina M
Di Domenico F
Di Fazio P
Di Fonzo A
Di Guardo G
Di Guglielmo GM
Di Leo L
Di Malta C
Di Nardo A
Di Rienzo M
Di Sano F
Diallinas G
Diao J
Diaz-Araya G
Dickinson JM
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Dieudé M
Dikic I
Ding S
Ding W-X
Dini L
Dinic M
Dinić J
Dinkova-Kostova AT
Dionne MS
Distler JHW
Diwan A
Dixon IMC
Djavaheri-Mergny M
Dobrinski I
Dobrovinskaya O
Dobrowolski R
Dobson RCJ
Dokmeci Emre S
Donadelli M
Dong B
Dong X
Dong XC
Dong Z
Dorn Ii GW
Dotsch V
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Dridi S
Drucker L
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Du A
Du C
Du G
Du H-N
Du L-L
Duan S-B
Duan X
Duarte SP
Dubrovska A
Dunlop EA
Dupont N
Durán RV
Dwarakanath BS
Dyshlovoy SA
Dávila VA
Díaz-Laviada I
Ebrahimi-Fakhari D
Eckhart L
Edelstein CL
Efferth T
Eftekharpour E
Eichinger L
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Eisenberg T
Eissa NT
Eissa S
Ejarque M
El Andaloussi A
El-Hage N
El-Naggar S
El-Shafey ES
Eleuteri AM
Elgendy M
Eliopoulos AG
Elizalde MM
Elks PM
Elsasser H-P
Elsherbiny ES
Emerling BM
Emre NCT
Eng CH
Engedal N
Engelbrecht A-M
Engelsen AST
Enserink JM
Escalante R
Esclatine A
Escobar-Henriques M
Eskelinen E-L
Espert L
Eusebio M-O
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Fabrizi C
Facchiano A
Facchiano F
Fadeel B
Fader C
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Fairlie WD
Falcó A
Falkenburger BH
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Fan Y
Fang EF
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Farfel-Becker T
Faure M
Fazeli G
Fedele AO
Feldman AM
Feng D
Feng J
Feng L
Feng W
Feng Y
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Fenz Araujo T
Ferguson TA
Fernandez-Checa JC
Fernie AR
Fernández ÁF
Fernández-Veledo S
Ferrante AW
Ferraresi A
Ferrari MF
Ferreira JCB
Ferro-Novick S
Figueras A
Filadi R
Filigheddu N
Filippi-Chiela E
Filomeni G
Fimia GM
Fineschi V
Finetti F
Finkbeiner S
Fisher EA
Fisher PB
Flamigni F
Fliesler SJ
Flo TH
Florance I
Florey O
Florio T
Fodor E
Follo C
Fon EA
Forlino A
Fornai F
Fortini P
Fracassi A
Fraldi A
Franco B
Franco R
Franconi F
Frankel LB
Friedman SL
Fröhlich LF
Frühbeck G
Fuentes JM
Fujiki Y
Fujita N
Fujiwara Y
Fukuda M
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Galadari S
Galasso A
Galindo MF
Gallolu Kankanamalage S
Galluzzi L
Galy V
Gammoh N
Gan B
Ganley IG
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Gao M
Gao P
Gao S-J
Gao W
Gao X
Garcera A
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Garcia VE
Garcia-Escudero V
Garcia-Garcia A
Garcia-Macia M
Garcia-Ruiz C
García-Del Portillo F
García-Moreno D
García-Sanz P
Garg AD
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Garofalo T
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Geiss-Friedlander R
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Ghigo A
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Giamas G
Giampietri C
Giatromanolaki A
Gibson GE
Gibson SB
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Girao H
Girardin SE
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Giulivi C
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Goldstone DC
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Gonzalez-Polo RA
Gonzalez-Reyes JA
González-Gallego J
González-Rodríguez P
Goping IS
Gorbatyuk MS
Gorbunov NV
Gorojod RM
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Goruppi S
Gotor C
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Gozuacik D
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Granatiero V
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Guan J-L
Guardia CM
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Helgason GV
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Hoet PHM
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Hooper LV
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Huber TB
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Izquierdo JM
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Johansen T
Johnson GVW
Johnston SA
Jokitalo E
Jolly MK
Joosten LAB
Jordan J
Joseph B
Ju D
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Judith D
Juhász G
Jun Y
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Kapuy O
Karamouzis MV
Karim MR
Karmakar P
Katare RG
Kato M
Kaufmann SHE
Kauppinen A
Kaushal GP
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Kazan K
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Keating DJ
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Kehrl JH
Keller CW
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Kemper JK
Kenchappa CS
Kenific CM
Kepp O
Kermorgant S
Kern A
Ketteler R
Keulers TG
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Khalil H
Khambu B
Khan SY
Khandelwal VKM
Khandia R
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Khobrekar NV
Khuansuwan S
Khundadze M
Killackey SA
Kim D
Kim D-E
Kim D-H
Kim DR
Kim E-K
Kim EY
Kim H-R
Kim H-S
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Kim JH
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Kim JK
Kim KI
Kim PK
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Kimball SR
Kimchi A
Kimmelman AC
Kimura T
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Kinghorn KJ
Kinsey CG
Kirkin V
Kirshenbaum LA
Kiselev SL
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Kitaoka Y
Kitazato K
Kitsis RN
Kittler JT
Kjaerulff O
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Koh YH
Kohlwein SD
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Korcsmaros T
Korkmaz G
Korolchuk VI
Korsnes MS
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Kota J
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Kotler ML
Kou Y
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Kovacs AL
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Krasnodembskaya AD
Kretz-Remy C
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Laface I
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Lagace DC
Lahiri V
Lai Z
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Lane DJR
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Lau WCY
Laurie GW
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Leck LYW
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Lee J-A
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Lee M
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Lima TRR
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Lin C
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Lin D-S
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Lin K-H
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Lin L-T
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Lin W
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Ling S-C
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Liu C
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Liu H-F
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Lünemann JD
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Madrigal-Matute J
Maeda A
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Martín-Segura A
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Masclaux-Daubresse C
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Mora AL
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Moratalla R
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Mulcahy Levy JM
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Nawrocki ST
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Netea MG
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Ortega-Villaizan MDM
Ortiz-Gonzalez XR
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Pajvani UB
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Palumbo C
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Pan X
Panasyuk G
Pandey R
Pandey UB
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Paneni F
Pang SY
Panzarini E
Papademetrio DL
Papaleo E
Papinski D
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Park HT
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Park J-I
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Park JT
Park S-Y
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Pimentel-Muiños FX
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Promponas VJ
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Pulinilkunnil T
Puri D
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Zhang X-W
Zhang XD
Zhang Y
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Zhang Y-D
Zhang Y-Y
Zhang Z
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Zhao X-F
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Zhou Y
Zhou Y
Zhou Y
Zhou Z
Zhou Z-Y
Zhu B
Zhu C
Zhu G-Q
Zhu H
Zhu H
Zhu H
Zhu W-G
Zhu Y
Zhu Y
Zhuang H
Zhuang X
Zientara-Rytter K
Zimmermann CM
Ziviani E
Zoladek T
Zong W-X
Zorov DB
Zorzano A
Zou W
Zou Z
Zou Z
Zuryn S
Zwerschke W
Álvarez ÉMC
Ávalos Y
Önal G
Üstün S
Čolić M
Đokić J
Žerovnik E
Publication venue: 'Informa UK Limited'
Publication date: 01/01/2021
Field of study

In 2008, we published the first set of guidelines for standardizing research in autophagy. Since then, this topic has received increasing attention, and many scientists have entered the field. Our knowledge base and relevant new technologies have also been expanding. Thus, it is important to formulate on a regular basis updated guidelines for monitoring autophagy in different organisms. Despite numerous reviews, there continues to be confusion regarding acceptable methods to evaluate autophagy, especially in multicellular eukaryotes. Here, we present a set of guidelines for investigators to select and interpret methods to examine autophagy and related processes, and for reviewers to provide realistic and reasonable critiques of reports that are focused on these processes. These guidelines are not meant to be a dogmatic set of rules, because the appropriateness of any assay largely depends on the question being asked and the system being used. Moreover, no individual assay is perfect for every situation, calling for the use of multiple techniques to properly monitor autophagy in each experimental setting. Finally, several core components of the autophagy machinery have been implicated in distinct autophagic processes (canonical and noncanonical autophagy), implying that genetic approaches to block autophagy should rely on targeting two or more autophagy-related genes that ideally participate in distinct steps of the pathway. Along similar lines, because multiple proteins involved in autophagy also regulate other cellular pathways including apoptosis, not all of them can be used as a specific marker for bona fide autophagic responses. Here, we critically discuss current methods of assessing autophagy and the information they can, or cannot, provide. Our ultimate goal is to encourage intellectual and technical innovation in the field

Plymouth Electronic Archive and Research Library

Vps34 and PLD1 take center stage in nutrient signaling: their dual roles in regulating autophagy

Author: B Ravikumar
C Dall'Armi
C He
CA Lamb
DW Hailey
E Itakura
EF Blommaart
EJ Bae
EL Axe
H Nakanishi
HX Yuan
IG Ganley
J Geng
J Kim
J Kim
JL Jewell
K Inoki
K Matsunaga
K Moreau
K Suzuki
L Bar-Peled
L Shang
L Xu
M Bjorklund
M Hayashi-Nishino
Mee-Sup Yoon
MG Roth
MP Byfield
MS Yoon
MS Yoon
N Fujita
N Gammoh
N Jaber
N Mizushima
N Mizushima
N Mizushima
N Mizushima
N Mizushima
NM Mazure
P Gulati
P Yla-Anttila
PM Wong
PV Schu
R Manjithaya
R Zoncu
RC Russell
RC Russell
RK Amaravadi
SA Tooze
T Nishimura
T Nobukuni
T Proikas-Cezanne
X Qu
X Zhou
Y Fang
Y Kabeya
Y Sancak
Y Sancak
Y Sun
Y Yan
Y Yan
YH Jang
Z Xie
Z Yue
Publication venue: 'Springer Science and Business Media LLC'
Publication date
Field of study

Crossref

A molecular genetic toolbox for Yarrowia lipolytica

Author: A Beopoulos
A Kretzschmar
A Martinez-Vazquez
AE Carpenter
AFJ Ram
AM Ansari
Anne M Carroll
AS Ivessa
B Dujon
B Langmead
C Ketel
C Madzak
C Ratledge
C Trapnell
CA Schneider
CH Calvey
Christopher T Evans
CM Gaillardin
CR Raetz
D Fennessy
D Sorger
D Zweytick
DC Hess
DG Gibson
DP Delmer
E Naumova
Eduard J. Kerkhoven
EJ Kerkhoven
EN Biryukova
Erin L. Bredeweg
F Matthaus
F Pascual
FM Kawasse
GA Eitzen
GM Carman
GM Carman
H Orozco
H Wolinski
H Wolinski
H-S Choi
HB Van Den Hazel
HJ Ham
HV Colot
I Vlaardingerbroek
J Blazeck
J Cescut
J Chang
J Reinders
J Schindelin
J Spencer
J Verbeke
J Yang
J-D Pédelacq
J-M Nicaud
Jens Nielsen
JJ Smith
JK Hane
JL Gordon
K Athenstaedt
K Athenstaedt
K Athenstaedt
K Gulshan
K Qiao
KR Pomraning
KR Pomraning
Kyle R. Pomraning
L Gritz
L Liu
L Ruiz-Pavón
LJ Wickerham
M Aguedo
M Benghezal
M Breker
M Chalfie
M Holsters
M Lopes
M Mekouar
M Tai
MC Jonikas
MG Murray
MJA de Groot
MT Le Dall
MU Hutchins
MW Foster
N Dean
N Morin
N-J Hung
N-J Hung
O Tehlivets
P Fickers
P Fickers
P Fournier
P Kabran
P Oelkers
P Pan
PJ Punt
R Cordero Otero
R Dulermo
R Manjithaya
RA Jefferson
RD Gietz
RD Gietz
RK Szilard
S Ayciriex
S Ghaemmaghami
S Götz
S Jain
S-K Chung
SA Henry
SC Ushinsky
Scott E. Baker
SD Kohlwein
SJ Gould
SJ Kolodziej
T Dulermo
T Dulermo
T Dulermo
T Liu
T Nazarko
T Wriessnegger
Tenagy
U Hoja
V Fotopoulos
VI Titorenko
VI Titorenko
W Handee
W-K Huh
W-M Su
W-M Su
WJ Kent
WL Chaffin
WS Park
Y Elgersma
Z Xue
Z-P Wang
Ziyu Dai
Publication venue: 'Springer Science and Business Media LLC'
Publication date
Field of study

Crossref

The 3' Untranslated Region of Bovine Follicle-Stimulating Hormone $\beta$ Messenger RNA Downregulates Reporter Expression: Involvement of AU-Rich Elements and Transfactors

Author: Dighe Rajan R
Manjithaya Ravi R
Publication venue: Society for the Study of Reproduction
Publication date
Field of study

FSH

\beta

mRNA has a unique 3' untranslated region (3'UTR) that is highly conserved across the species. Sequence analyses of the mouse, rat, human, bovine, and ovine 3'UTRs revealed the presence of elements implicated in mRNA instability and translational control such as AU-Rich Element (ARE) and lipoxygenase differentiation control elements. Bovine FSH

\beta

3'UTR down-regulated reporter expression in aT3-1 and NIH3T3 cells, but not in HEK 293 cells, suggesting the involvement of a cellspecific factor or mechanism. The presence of a 3'UTR did not influence reporter mRNA stability, but it did decrease its association with polysomes, indicating that the downregulatory effect may be exerted at the translational level. The segment spanning 601–800 bases (U4) of the bovine FSH

\beta

3'UTR was found to be the most effective downregulating segment, its effect being equal to that of the full-length 3'UTR. RNA electrophoretic mobility shift assay with U4 showed the presence of specific transfactors in the cytosolic preparations of bovine pituitary and the cell lines. U4 contained an ARE that appeared to be functional, because the mutated U4 ARE was ineffective in downregulating the reporter expression and inhibiting [32P]-labeled U4-transfactor complex formation. Downregulation of reporter activity by the full-length 3'UTR and U4 could be overcome by overexpression of HuR, a protein known to stabilize ARE-containing mRNAs in NIH3T3 cells, but not in the aT3-1 cells, once again indicating that factors other than HuR may also be involved in the regulation of FSH

\beta

in the pituitary

Open Access Repository of IISc Research Publications