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84 research outputs found

Targeted metabolomic profiling in rat tissues reveals sex differences

Author: Albano L
Campesi I
Caterino M
Costanzo M
Crisci D
Di Girolamo MG
Franconi F
Milella L
Pecce R
Ruoppolo M
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2018
Field of study

Sex differences affect several diseases and are organ-and parameter-specific. In humans and animals, sex differences also influence the metabolism and homeostasis of amino acids and fatty acids, which are linked to the onset of diseases. Thus, the use of targeted metabolite profiles in tissues represents a powerful approach to examine the intermediary metabolism and evidence for any sex differences. To clarify the sex-specific activities of liver, heart and kidney tissues, we used targeted metabolomics, linear discriminant analysis (LDA), principal component analysis (PCA), cluster analysis and linear correlation models to evaluate sex and organ-specific differences in amino acids, free carnitine and acylcarnitine levels in male and female Sprague-Dawley rats. Several intra-sex differences affect tissues, indicating that metabolite profiles in rat hearts, livers and kidneys are organ-dependent. Amino acids and carnitine levels in rat hearts, livers and kidneys are affected by sex: male and female hearts show the greatest sexual dimorphism, both qualitatively and quantitatively. Finally, multivariate analysis confirmed the influence of sex on the metabolomics profiling. Our data demonstrate that the metabolomics approach together with a multivariate approach can capture the dynamics of physiological and pathological states, which are essential for explaining the basis of the sex differences observed in physiological and pathological conditions

Archivio della ricerca - Università degli studi di Napoli Federico II

New perspective for an old drug: Can naloxone be considered an antioxidant agent?

Author: Acquas E.
Bassareo V.
Campesi I.
Galleri G.
Lostia G.
Migheli R.
Peana A. T.
Rocchitta G.
Serra P. A.
Publication venue
Publication date: 01/01/2023
Field of study

Background: Experimental evidence indicates that Naloxone (NLX) holds antioxidant properties. The present study aims at verifying the hypothesis that NLX could prevent oxidative stress induced by hydrogen peroxide (H2O2) in PC12 cells.Methods: To investigate the antioxidant effect of NLX, initially, we performed electrochemical experiments by means of platinum-based sensors in a cell-free system. Subsequently, NLX was tested in PC12 cells on H2O2induced overproduction of intracellular levels of reactive-oxygen-species (ROS), apoptosis, modification of cells' cycle distribution and damage of cells' plasma membrane.Results: This study reveals that NLX counteracts intracellular ROS production, reduces H2O2-induced apoptosis levels, and prevents the oxidative damage-dependent increases of the percentage of cells in G2/M phase. Likewise, NLX protects PC12 cells from H2O2- induced oxidative damage, by preventing the lactate dehydrogenase (LDH) release. Moreover, electrochemical experiments confirmed the antioxidant properties of NLX.Conclusion: Overall, these findings provide a starting point for studying further the protective effects of NLX on oxidative stress

Archivio istituzionale della ricerca - Università di Cagliari

Epigenetics, stem cells, and autophagy: Exploring a path involving miRNA

Author: Angius A.
Balzano F.
Bellu E.
Campesi I.
Capobianco G.
Cruciani S.
Dessole S.
Garroni G.
Giudici S. D.
Maioli M.
Montella A.
Oggiano A.
Rallo V.
Ventura C.
Publication venue
Publication date: 01/01/2019
Field of study

MiRNAs, a small family of non-coding RNA, are now emerging as regulators of stem cell pluripotency, differentiation, and autophagy, thus controlling stem cell behavior. Stem cells are undifferentiated elements capable to acquire specific phenotype under different kind of stimuli, being a main tool for regenerative medicine. Within this context, we have previously shown that stem cells isolated from Wharton jelly multipotent stem cells (WJ-MSCs) exhibit gender differences in the expression of the stemness related gene OCT4 and the epigenetic modulator gene DNA-Methyltransferase (DNMT1). Here, we further analyze this gender difference, evaluating adipogenic and osteogenic differentiation potential, autophagic process, and expression of miR-145, miR-148a, and miR-185 in WJ-MSCs derived from males and females. These miRNAs were selected since they are involved in OCT4 and DNMT1 gene expression, and in stem cell differentiation. Our results indicate a difference in the regulatory circuit involving miR-148a/DNMT1/OCT4 autophagy in male WJ-MSCs as compared to female cells. Moreover, no difference was detected in the expression of the two-differentiation regulating miRNA (miR-145 and miR-185). Taken together, our results highlight a different behavior of WJ-MSCs from males and females, disclosing the chance to better understand cellular processes as autophagy and stemness, usable for future clinical applications

Archivio istituzionale della ricerca - Alma Mater Studiorum Università di Bologna

Human umbilical endothelial cells (HUVECs) have a sex: characterisation of the phenotype of male and female cells

Author: AK Death
B Toth
C Chen
CM Sena
CN Hales
CV Sapan
D Onat
DB Cines
E Bertino
E Cuestas
E Greaves
E Lyros
E Straface
ER Prossnitz
F Schatz
F Wang
G Annibalini
G Balconi
HJM de Jonge
I Campesi
IC Villar
J Lee
J Vandesompele
JD Rabinowitz
JF Reckelhoff
JJM de Llano
K Kublickiene
K Kublickiene
K McGrath
K Shah
KE Kypreos
KE Taylor
L Du
L Murrow
L Xiao
M Pellegrini
M Simard
M Wang
MAJ Hervé
MG Cattaneo
MH Laughlin
MJ Evans
MJ Legato
MW Pfaffl
NA Papakonstantinou
NC Gupta
P Matarrese
PJ Oviedo
Q Wu
R Dai
RI Handin
RO Batres
S Bae
S Kim-Schulze
SB Ogueta
SP Crampton
TYL Le
V Regitz-Zagrosek
W Malorni
XH Ma
Y Zhang
Publication venue: 'Springer Science and Business Media LLC'
Publication date
Field of study

Crossref

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

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A. C. Ma
A. K. Au
Abdel-Aziz A. K.
Abdelfatah S.
Abdellatif M.
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Abeliovich H.
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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.
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Ahumada-Castro U.
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Al-Abd A. M.
Al-Akra L.
Al-Gharaibeh A.
Alaoui-Jamali M. A.
Alberti S.
Alcocer-Gomez E.
Alessandri C.
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Alim Al-Bari M. A.
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Alizadeh J.
Almacellas E.
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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
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Bao Y
Baptista MS
Baracca A
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Bargiela A
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Bhuiyan MS
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Brackney DE
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Bravo-San Pedro JM
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Broaddus VC
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Brodsky JL
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Bronstein JM
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Brumell JH
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Bruno D
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Buitrago-Molina LE
Bultynck G
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Camara NO
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Campbell EM
Campbell-Valois F-X
Campello S
Campesi I
Campos JC
Camuzard O
Cancino J
Candido de Almeida D
Canesi L
Caniggia I
Canonico B
Cantí C
Cao B
Caraglia M
Caramés B
Carchman EH
Cardenal-Muñoz E
Cardenas C
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Cardoso SM
Carew JS
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Carloni S
Carmona-Gutierrez D
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Carosi JM
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Castro-Caldas M
Castro-Hernandez J
Castro-Obregon S
Catz SD
Cavadas C
Cavaliere F
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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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Chakraborty T
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Chamilos G
Chan DW
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Chan EYW
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Chan HYE
Chan MTV
Chan YS
Chandra PK
Chang C
Chang C-P
Chang H-C
Chang K
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 Bosscher K
De Felice F
De Franceschi L
De Leonibus C
de Mattos Barbosa MG
De Meyer GRY
De Milito A
De Nunzio C
De Palma C
De Santi M
De Virgilio C
De Zio D
Debnath J
DeBosch BJ
Decuypere J-P
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Deflorian G
DeGregori J
Dehay B
Del Rio G
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
Diederich M
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
Dou H
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Dowaidar M
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
Eid N
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
Fabrias G
Fabrizi C
Facchiano A
Facchiano F
Fadeel B
Fader C
Faesen AC
Fairlie WD
Falcó A
Falkenburger BH
Fan D
Fan J
Fan Y
Fang EF
Fang Y
Fang Y
Fanto M
Farfel-Becker T
Faure M
Fazeli G
Fedele AO
Feldman AM
Feng D
Feng J
Feng L
Feng W
Feng Y
Feng Y
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
Fulda S
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Furuya N
Fusco C
Gack MU
Gaffke L
Galadari S
Galasso A
Galindo MF
Gallolu Kankanamalage S
Galluzzi L
Galy V
Gammoh N
Gan B
Ganley IG
Gao F
Gao H
Gao M
Gao P
Gao S-J
Gao W
Gao X
Garcera A
Garcia MN
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
Gargini R
Garofalo T
Garry RF
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Gatica D
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Geiss-Friedlander R
Gelfi C
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Gentle IE
Gerbino V
Gerhardt C
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Gewirtz DA
Ghasemipour Afshar E
Ghavami S
Ghigo A
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Giamas G
Giampietri C
Giatromanolaki A
Gibson GE
Gibson SB
Ginet V
Giniger E
Giorgi C
Girao H
Girardin SE
Giridharan M
Giuliano S
Giulivi C
Giuriato S
Giustiniani J
Gluschko A
Goder V
Goginashvili A
Golab J
Goldstone DC
Golebiewska A
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Gomez-Puerto MC
Gomez-Sintes R
Gong Q
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Gonzalez-Hernandez T
Gonzalez-Polo RA
Gonzalez-Reyes JA
González-Gallego J
González-Rodríguez P
Goping IS
Gorbatyuk MS
Gorbunov NV
Gorojod RM
Gorski SM
Goruppi S
Gotor C
Gottlieb RA
Gozes I
Gozuacik D
Graef M
Granatiero V
Grasso D
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Green DR
Greenhough A
Gregory SL
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Grinstaff MW
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Gräler MH
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Guan J-L
Guardia CM
Guda K
Guerra F
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Guntur AR
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Gupta V
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Gustafsson AB
Gutterman DD
Gómez-Sánchez R
Görgülü K
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Hamacher-Brady A
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Helgason GV
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Ho WY
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Hoet PHM
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Holmberg CI
Hombrebueno JR
Hooper LV
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Horos R
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Hsin I-L
Hsu H-Y
Hu B
Hu D
Hu L-F
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Hu W
Hu Y-C
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Hua Y
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Huang R
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Huang YJ
Huber TB
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Hubner CA
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Iyer AKV
Izquierdo JM
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Jacomin A-C
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Jimenez-Sanchez M
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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
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Katare RG
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Kaufmann SHE
Kauppinen A
Kaushal GP
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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
Kim S-J
Kimball SR
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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
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Kittler JT
Kjaerulff O
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Kocaturk NM
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Koenig U
Koh YH
Kohlwein SD
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Komatsu M
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Kopp BT
Korcsmaros T
Korkmaz G
Korolchuk VI
Korsnes MS
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Kota J
Kotake Y
Kotler ML
Kou Y
Koukourakis MI
Koustas E
Kovacs AL
Kovács T
Koya D
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Kraft C
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Krasnodembskaya AD
Kretz-Remy C
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Kuchitsu K
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Kukar T
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Kunnumakkara AB
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Kutlu O
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Kwon YT
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Labonté P
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Laface I
Lafont F
Lagace DC
Lahiri V
Lai Z
Laird AS
Lakkaraju A
Lamark T
Lan S-H
Landajuela A
Lane DJR
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Lang CH
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Langer R
Lapaquette P
Laporte J
LaRusso NF
Lastres-Becker I
Lau WCY
Laurie GW
Lavandero S
Law BYK
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Lebrun J-J
Leck LYW
Leduc-Gaudet J-P
Lee C
Lee C-P
Lee D-H
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Lee H-J
Lee HK
Lee J-A
Lee J-Y
Lee JH
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Lee JS
Lee M
Lee M-S
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Lee MJ
Lee S-J
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Librizzi M
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Lilly MA
Lim HJ
Lima TRR
Limana F
Lin C
Lin C-W
Lin D-S
Lin F-C
Lin JD
Lin K-H
Lin KM
Lin L-T
Lin P-H
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Lin W
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Ling S-C
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Linnemann AK
Liou Y-C
Lipinski MM
Lipovšek S
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Liu C
Liu C-F
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Liu H-F
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Lizcano JM
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Lucocq JM
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Luis-Ravelo D
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Luo H
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Lyamzaev KG
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Ma N-F
Ma Q-H
Ma X
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MacIntosh GC
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Macleod KF
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Madrigal-Matute J
Maeda A
Maejima Y
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Martinez-Vicente M
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Martín-Segura A
Marzetti E
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Masclaux-Daubresse C
Mashek DG
Massa V
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Masson GR
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Mora AL
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Moratalla R
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Mulcahy Levy JM
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Mysorekar IU
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Naude RJ
Naumann C
Naveiras O
Navid F
Nawrocki ST
Nazarko TY
Nazio F
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Neisch AL
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Netea MG
Neubert P
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Neumann D
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Ortega-Villaizan MDM
Ortiz-Gonzalez XR
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Pan X
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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
Park SC
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Pimentel-Muiños FX
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Promponas VJ
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Pulinilkunnil T
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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 H
Zhou H
Zhou H
Zhou J
Zhou J
Zhou J
Zhou J
Zhou K
Zhou R
Zhou X-J
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

LE TRAVERSATE DELLE MIGRAZIONI STORICHE ITALIANE TRA EVENTO E RACCONTO

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AS TRAVESSIAS DAS HISTÓRICAS MIGRAÇÕES ITALIANAS: entre fatos e narrações

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A case–control analysis of oral contraceptive use and breast cancer subtypes in the African American Breast Cancer Epidemiology and Risk Consortium

Author: A Iversen
AB Edelman
AB Edelman
AB Edelman
AI Phipps
Andrew F Olshan
BB Gerstman
C Hoften Van
C Kahlenborn
C Sweeney
CA Parise
CB Ambrosone
CB Ambrosone
Chi-Chen Hong
Christine B Ambrosone
CM Perou
Collaborative Group on Hormonal Factors in Breast Cancer
CU Ihemelandu
DJ Hunter
E Isaksson
EF Beaber
EF Beaber
Elisa V Bandera
EV Bandera
EV Bandera
FP Turkoz
G Ursin
GS Merki-Feld
H Ma
H Ma
HG Kaplan
I Campesi
IJ Hall
JM Dolle
JP Higgins
JR Palmer
JR Palmer
JR Palmer
JS Reis-Filho
Julie R Palmer
KA Rosenblatt
Kathryn L Lunetta
KM Flegal
KR Bauer
L Rosenberg
L Rosenberg
L Rosenberg
LA Carey
Laurence N Kolonel
Lynn Rosenberg
M Cotterchio
M Kumle
M Szyf
M Urban
MD Althuis
MD Althuis
MD Althuis
Melissa A Troester
MJ Rosenberg
MM Gaudet
P Nischan
PA Marchbanks
PA Marchbanks
PB Gupta
PC Hannaford
Pepper Schedin
PG Moorman
PM Ravdin
PP Bao
R Ritte
R Sitruk-Ware
RC Millikan
S Shapiro
SE Hankinson
SL Ooi
SM Gapstur
T Dorjgochoo
TJ Key
TJ Powles
Traci N Bethea
U Chandran
V Cogliano
WY Huang
XR Yang
Publication venue: BioMed Central
Publication date: 01/01/2015
Field of study

Abstract Introduction Recent oral contraceptive (OC) use has been consistently associated with increased risk of breast cancer, but evidence on specific breast cancer subtypes is sparse. Methods We investigated recency and duration of OC use in relation to molecular subtypes of breast cancer in a pooled analysis of data from the African American Breast Cancer Epidemiology and Risk Consortium. The study included 1,848 women with estrogen receptor-positive (ER+) breast cancer, 1,043 with ER-negative (ER-) breast cancer (including 494 triple negative (TN) tumors, which do not have receptors for estrogen, progesterone, and human epidermal growth factor 2), and 10,044 controls. Multivariable polytomous logistic regression models were used to estimate odds ratios (ORs) and 95% confidence intervals (CIs) for exposure categories relative to never use, controlling for potential confounding variables. Results OC use within the previous 5 years was associated with increased risk of ER+ (OR 1.46, 95% CI 1.18 to 1.81), ER- (OR 1.57, 95% CI 1.22 to 1.43), and TN (OR 1.78, 95% CI 1.25 to 2.53) breast cancer. The risk declined after cessation of use but was apparent for ER+ cancer for 15 to 19 years after cessation and for ER- breast cancer for an even longer interval after cessation. Long duration of use was also associated with increased risk of each subtype, particularly ER-. Conclusions Our results suggest that OC use, particularly recent use of long duration, is associated with an increased risk of ER+, ER-, and TN breast cancer in African American women. Research into mechanisms that explain these findings, especially the association with ER- breast cancer, is needed

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Springer - Publisher Connector

PubMed Central

Carolina Digital Repository

The Effect of Patient Sex on the Incidence of Early Adverse Events in a Population of Elderly Patients

Author: Campesi I.
Kiekkas P.
Publication venue: 'SAGE Publications'
Publication date
Field of study

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