38 research outputs found
Experimental models and tools to tackle glioblastoma
- Author
- Publication venue
- 'The Company of Biologists'
- Publication date
- 06/09/2019
- Field of study
Get PDFReprogramming of Fibroblasts to Oligodendrocyte Progenitor-like Cells Using CRISPR/Cas9-Based Synthetic Transcription Factors
- Author
- Publication venue
- 'Elsevier BV'
- Publication date
- 07/11/2019
- Field of study
Get PDFLRIG1 is a gatekeeper to exit from quiescence in adult neural stem cells
- Author
- A Aguirre
- A Sakaue-Sawano
- AY Maslov
- B Martynoga
- B Neumeister
- BS Melin
- C Giachino
- CE Scott
- DA Lim
- E Kokovay
- E Llorens-Bobadilla
- E Pastrana
- E Raponi
- Ewan Harry Bulstrode
- F Doetsch
- F Doetsch
- F Doetsch
- G Kalamakis
- H Caren
- H Mira
- H-S Nam
- JT Gonçalves
- K Obernier
- KB Jensen
- L Conti
- L Martin-Hijano
- L Otsuki
- LC Fuentealba
- M Daynac
- M Rumman
- M Sonego
- MB Laederich
- MÁ Marqués-Torrejón
- N Urbán
- O Basak
- OR Lindberg
- P Codega
- PS Dewari
- Q Shen
- R Beckervordersandforth
- R Petrova
- RB Bressan
- RE Gross
- RL Mort
- RR Weichselbaum
- S Lugert
- T Oki
- TH Cheung
- V Silva-Vargas
- VWY Wong
- Y Sun
- Yutaka Suzuki
- Z Mirzadeh
- Publication venue
- 'Springer Science and Business Media LLC'
- Publication date
- 10/05/2021
- Field of study
Get PDFAdult neural stem cells (NSCs) must tightly regulate quiescence and proliferation. Single-cell analysis has suggested a continuum of cell states as NSCs exit quiescence. Here we capture and characterize in vitro primed quiescent NSCs and identify LRIG1 as an important regulator. We show that BMP-4 signaling induces a dormant non-cycling quiescent state (d-qNSCs), whereas combined BMP-4/FGF-2 signaling induces a distinct primed quiescent state poised for cell cycle re-entry. Primed quiescent NSCs (p-qNSCs) are defined by high levels of LRIG1 and CD9, as well as an interferon response signature, and can efficiently engraft into the adult subventricular zone (SVZ) niche. Genetic disruption of Lrig1 in vivo within the SVZ NSCs leads an enhanced proliferation. Mechanistically, LRIG1 primes quiescent NSCs for cell cycle re-entry and EGFR responsiveness by enabling EGFR protein levels to increase but limiting signaling activation. LRIG1 is therefore an important functional regulator of NSC exit from quiescence
Outcomes from elective colorectal cancer surgery during the SARS-CoV-2 pandemic
- Author
- 14 | COVIDSurg COllabOratIVe Tzovaras G. (General University Hospital of Larissa)
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- COVIDSurg COllabOratIVe | 15 Violante T. (IRCCS Azienda Ospedaliero – Universitaria di Bologna
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- Tweedle E. (Addenbrooke’s Hospital)
- Ugarte-Sierra B. (Hospital Universitario de Galdakao)
- Uludağ S. S.
- Umair M.
- Universiti Sains Malaysia)
- University of Amsterdam)
- Università di Ferrara)
- Université Mohammed V Rabat). Netherlands: Hompes R.
- Uras C. (Acibadem Maslak Hospital)
- Urbani A. (Azienda Ospedaliero Universitaria San’anna)
- Urbieta A. (Hospital Universitario la Paz)
- Uslu G.
- Utkan N. Z.
- Uyanik M. S. (Samsun Training and Research Hospital)
- Uzunoglu F. G. (University Medical Center Hamburg–Eppendorf). Greece: Antonakis P.
- Vaccarella G. (Azienda Ospedaliera Ospedali Riuniti Villa Sofia-Cervello)
- Valbuena Jabares V. (Marqués de Valdecilla University Hospital)
- Valdes- Hernandez J. (Hospital Universitario Virgen Macarena)
- Valero Soriano M. (Hospital General Reina Sofía)
- Valle Rubio A. (Getafe University Hospital)
- Valverde S. (Hospital Clinic Barcelona)
- Van den Eynde J.
- Van den Eynde R. (Uz Leuven). Bulgaria: Sokolov M. (University Hospital Alexandrovska). Canada: Boutros M.
- Varma M. (University of California
- Vasljević J.
- Vassiliu P. (Attikon University General Hospital)
- Vaz Pereira R.
- Vaz S. (Centro Hospitalar e Universitário de São João)
- Velchuru V.
- Velickovic D. (Clinic for Digestive Surgery
- Velidedeoglu M.
- Venn M. (Royal London Hospital)
- Venskutonis D. (Lithuanian University of Health Sciences Kaunas Clinical Hospital). Madagascar: Rasoaherinomenjanahary F.
- Vera Mansilla C. (Hospital Universitario Principe de Asturias)
- Verberne C. (John Radcliffe Hospital)
- Vergari R. (Ospedali Riuniti di Ancona)
- Vernon L. (Cork University Hospital)
- Vervoort D.
- Vescio G. (University ‘Magna Graecia’ of Catanzaro)
- Vezakis A. (Aretaieion Hospital)
- Videira J. F. (IPO Porto). Réunion: Kassir R.
- Vieira B. (Centro Hospitalar de Trás-Os-Montes e Alto Douro
- Vieira Caroço T. (IPO Coimbra)
- Vieira Paiva Lopes A. C. (Hospital de Torres Vedras – Centro Hospitalar do Oeste)
- Vignali A. (San Raffaele Scientific Institute
- Vigorita V. (Álvaro Cunqueiro Hospital)
- Vijayan D. (Queen Elizabeth Hospital Birmingham)
- Villalabeitia Ateca I. (Hospital Universitario Cruces)
- Vimalachandran D. (Countess of Chester Hospital)
- Viswanath Y. K. S. (James Cook University Hospital)
- Vitali A. (Ospedale San Giovanni di Dio)
- Vitone L. (Royal Blackburn Hospital)
- Vives R. V. (Bellvitge University Hospital)
- Vo U. G. (Fiona Stanley Hospital)
- Von Papen M.
- Vovola F. (Ospedali Riuniti Azienda Ospedaliera Universitaria Foggia)
- Vucic N.
- Vázquez Fernández A. (Hospital Clínico Universitario de Valladolid)
- Wadham B. (The University Hospital of South Manchester)
- Walkes K. (Queen Elizabeth Hospital). Belgium: Flamey N.
- Wani R. (Sher-I-Kashmir Institute of Medical Sciences)
- Waqar S. H. (Pakistan Institute of Medical Sciences). Poland: Major P. (Jagiellonian University Medical College). Portugal: Azevedo C.
- Warren O. (Chelsea and Westminster Hospital)
- Watson L. J. (Sunderland Royal Hospital)
- Watson N. (King’s Mill Hospital)
- Weitz J.
- Welsch T. (Carl-Gustav-Carus University Hospital
- Werner J. (LMU Klinikum Campus Innenstadt)
- Westwood E. (James Paget University NHS Foundation Trust Hospital)
- Whelan M. (Tallaght University Hospital)
- Whitmore H. (Torbay and South Devon NHS Trust)
- Wilkin R. J. W. (South Warwickshire NHS Foundation Trust)
- Wilkins A. (Hull University Teaching Hospitals NHS Trust)
- Williams G. (Royal Gwent Hospital)
- Williams K. (St George’s Hospital)
- Wilson M. (Forth Valley Royal Hospital)
- Wimmer A. (Paracelsus Medical University Salzburg). Barbados: Barker D.
- Wong M.
- Worku D. (Queens Medical Centre)
- Wullschleger M. (Gold Coast University Hospital)
- Xavier R. G.
- Xenaki S.
- Xynos E. (University Hospital of Heraklion Crete and Interclinic Hospital of Crete). Hong Kong: Futaba K.
- Yang W.
- Yassin N. (Royal Wolverhampton NHS Trust)
- Ye G.
- Yesantharao P.
- Yetkin S. G. (Sisli Hamidiye Etfal Training and Research Hospital)
- Yeşilyurt D. (University of Health Sciences Tepecik Training and Research Hospital)
- Yiallourou A. (Nicosia General Hospital). Czechia: Martinek L.
- Yıldırım A.
- Yildiz A. (Yildirim Beyazit University Yenimahalle Training and Research Hospital). Uganda: Lule H.
- Young R. (York Teaching Hospitals NHS Trust)
- Yousof E. A. (Assiut University Hospital)
- Youssef M. (Norfolk and Norwich University Hospital)
- Yurttas C. (University Hospital Tuebingen)
- Yánez C. (Royo Villanova)
- Yüksel E. (Kocaeli University Teaching Hospital)
- Zafar S. N. (University of Wisconsin)
- Zakaria A. D.
- Zakaria Z. (School of Medical Sciences and Hospital
- Zambon M. (Policlinico Umberto I Sapienza University of Rome)
- Zanus G. (Ca’ Foncello Treviso – DISCOG – Università di Padova)
- Zegarac M. (Institute for Oncology and Radiology of Serbia)
- Zelić M. (University Hospital Center Rijeka)
- Zengin A. K. (Istanbul Universty – Cerrahpaşa Medical Faculty)
- Zerbib P. (CHU Lille)
- Zervas K.
- Zese M. (Santa Maria degli Angeli Hospital ULSS 5 – Adria)
- Zhang H. (Concord Repatriation General Hospital)
- Zizzo M. (Azienda Unità Sanitaria Locale – IRCCS di Reggio Emilia)
- Zografos C. (Laiko University Hospital)
- Zorrilla Ortúzar J. (Hospital General Universitario Gregorio Marañón)
- Zourntou S. (General Hospital of Larissa ‘Koutlimpaneio and Triantafylleio’)
- Zubaidi A. M. (King Saud University). Serbia: Aleksić L.
- Ângelo M.
- Çelebi F.
- Çolak E.
- Öfner D. (Medical University of Innsbruck)
- Öhlberger L.
- Özçelık M. F.
- Öğücü H.
- Überrück L.
- Ćoza I.
- Publication venue
- 'Wiley'
- Publication date
- 01/01/2020
- Field of study
Get PDFThis study aimed to describe the change in surgical practice and the impact of SARS-CoV-2 on mortality after surgical resection of colorectal cancer during the initial phases of the SARS-CoV-2 pandemic
A new role of hindbrain boundaries as pools of neural stem/progenitor cells regulated by Sox2
- Author
- A Gagliardi
- A Geling
- A Geling
- A Kriegstein
- A Liu
- A Lumsden
- A Lumsden
- A Pataskar
- A Sarkar
- A Tallafuß
- A Watanabe
- AC Lekven
- AH Sinclair
- Ayelet Kohl
- BB Riley
- C Kiecker
- C Kiecker
- C Lesuisse
- C Stigloher
- CB Moens
- CD Katsetos
- CR Altmann
- CS Bjornsson
- D Hoof Van
- D Schulte
- D Sela-Donenfeld
- Dalit Sela-Donenfeld
- DJ Connolly
- E Fuchs
- E Jimenez-Guri
- F Cimadamore
- F Guillemot
- G Juan
- G Kayam
- Gideon Hen
- H Fong
- H Hirata
- H Kurose
- H Nakamura
- H Suh
- I Heyman
- I Heyman
- I Imayoshi
- I Mason
- J Chen
- J Gubbay
- J Jiang
- J Middeldorp
- J Neves
- J Ninkovic
- J Ninkovic
- J Tailor
- J Terriente
- J Terriente
- JDW Clarke
- JH Baek
- K Irmady
- K Shimozaki
- K Weisinger
- K Weisinger
- Karen Weisinger
- Karina Yaniv
- KG Storey
- KW McDermott
- L Caneparo
- L Dimou
- L Dirian
- L Evsen
- LA Boyer
- LH Pevny
- LH Pevny
- LM Julian
- M Amoyel
- M Cook
- M Gotz
- M Groysman
- M McCarthy
- M Rex
- M Rhinn
- M Tham
- M Uchikawa
- M Uchikawa
- M Wegner
- M Yanagisawa
- M Zervas
- MA Gates
- MA Selleck
- MK Lee
- MÁ Marqués-Torrejón
- N Perrone-Bizzozero
- N Xu
- Noa Eren
- P Chapouton
- P Ellis
- PM Kulesa
- Q Qu
- Q Xu
- R Favaro
- R Feng
- R Keynes
- R Mahmood
- R Mahmood
- RA Young
- RJT Wingate
- RM Albano
- S Ahmed
- S Dworkin
- S Fraser
- S Guthrie
- S Guthrie
- S Guthrie
- S Martinez
- S Masui
- S Miltenyi
- S Miyagi
- S Ohnuma
- S Ramasamy
- S Sirko
- S Tsuruzoe
- S Tümpel
- S Zhang
- SPHA Memberg
- SR Hutton
- V Graham
- W Ma
- W Wurst
- Y Kamachi
- Y Kee
- Y Li
- Y Yuan
- Y-C Cheng
- Y-S Lai
- YM Elkouby
- Yuval Cinnamon
- Yuval Peretz
- Z Jin
- Publication venue
- 'Springer Science and Business Media LLC'
- Publication date
- Field of study
Full text linkUV-Induced Somatic Mutations Driving Clonal Evolution in Healthy Skin, Nevus, and Cutaneous Melanoma
- Author
- Publication venue
- MDPI AG
- Publication date
- 01/08/2022
- Field of study
No full textIntroduction: Due to its aggressiveness, cutaneous melanoma (CM) is responsible for most skin cancer-related deaths worldwide. The origin of CM is closely linked to the appearance of UV-induced somatic mutations in melanocytes present in normal skin or in CM precursor lesions (nevi or dysplastic nevi). In recent years, new NGS studies performed on CM tissue have increased the understanding of the genetic somatic changes underlying melanomagenesis and CM tumor progression. Methods: We reviewed the literature using all important scientific databases. All articles related to genomic mutations in CM as well as normal skin and nevi were included, in particular those related to somatic mutations produced by UV radiation. Conclusions: CM development and progression are strongly associated with exposure to UV radiation, although each melanoma subtype has different characteristic genetic alterations and evolutionary trajectories. While BRAF and NRAS mutations are common in the early stages of tumor development for most CM subtypes, changes in CDKN2A, TP53 and PTEN, together with TERT promoter mutations, are especially common in advanced stages. Additionally, large genome duplications, loss of heterozygosity, and copy number variations are hallmarks of metastatic disease. Finally, the mutations driving melanoma targeted-therapy drug resistance are also summarized. The complete sequential stages of clonal evolution leading to CM onset from normal skin or nevi are still unknown, so further studies are needed in this field to shed light on the molecular pathways involved in CM malignant transformation and in melanoma acquired drug resistance
Telomere Shortening in Neural Stem Cells Disrupts Neuronal Differentiation and Neuritogenesis
- Author
- Publication venue
- 'Society for Neuroscience'
- Publication date
- 18/11/2009
- Field of study
No full textSignaling through BMPR-IA regulates quiescence and long-term activity of neural stem cells in the adult hippocampus.
- Author
- Publication venue
- Publication date
- 01/01/2010
- Field of study
No full textNeural stem cells (NSCs) in the adult hippocampus divide infrequently, and the molecules that modulate their quiescence are largely unknown. Here, we show that bone morphogenetic protein (BMP) signaling is active in hippocampal NSCs, downstream of BMPR-IA. BMPs reversibly diminish proliferation of cultured NSCs while maintaining their undifferentiated state. In vivo, acute blockade of BMP signaling in the hippocampus by intracerebral infusion of Noggin first recruits quiescent NSCs into the cycle and increases neurogenesis; subsequently, it leads to decreased stem cell division and depletion of precursors and newborn neurons. Consistently, selective ablation of Bmpr1a in hippocampal NSCs, or inactivation of BMP canonical signaling in conditional Smad4 knockout mice, transiently enhances proliferation but later leads to a reduced number of precursors, thereby limiting neuronal birth. BMPs are therefore required to balance NSC quiescence/proliferation and to prevent loss of the stem cell activity that supports continuous neurogenesis in the mature hippocampus
Simultaneous disruption of PRC2 and enhancer function underlies histone H3.3-K27M oncogenic activity in human hindbrain neural stem cells
- Author
- Publication venue
- 'Springer Science and Business Media LLC'
- Publication date
- 22/07/2021
- Field of study
No full textIntracerebral hemorrhage influences hippocampal neurogenesis and neurological function recovery via Notch1 signaling
- Author
- Publication venue
- 'Ovid Technologies (Wolters Kluwer Health)'
- Publication date
- Field of study
No full text
