888 research outputs found
Future orientation and planning in forestry: a comparison of forest managers' planning horizons in Germany and the Netherlands
- Author
- A Bandura
- A Nilsen
- AJ Maule
- B Taylor
- BK Boyd
- C Price
- CC Miller
- DL Martell
- E Hall
- FAO
- FJ Convery
- FJ Convery
- G Boniecki
- G Kasakos
- G Reith
- G Trommsdorff
- H Lamm
- H Nowotny
- H Schanz
- H Scheurer
- Heiner Schanz
- J Kangas
- J Orasanu
- J Simons
- JA Zivnuska
- JG March
- JM Mezias
- K Heijden Van der
- KW Marko
- L Gray
- LW Shannon
- M Penttinen
- M Wallace
- Marjanke A. Hoogstra
- ME Poole
- MS Cohen
- P Glück
- PF Drucker
- PJ Cooper
- R Jessor
- R Lipshitz
- RA Goodman
- RB Brown
- SH Olson
- SL Yaffee
- T Gjesme
- T Gjesme
- T Gjesme
- TD Graves
- TD Graves
- TJ Murphy
- TK Das
- TK Das
- V Ramanujam
- WA Duerr
- Y Friedman
- Publication venue
- Publication date
- 01/01/2009
- Field of study
Get PDFLong range (or strategic) planning is an important tool for forest management to deal with the complex and unpredictable future. However, it is the ability to make meaningful predictions about the rapidly changing future that is questioned. What appears to be particularly neglected is the question of the length of time horizons and the limits (if any) to these horizons, despite being considered one of the most critical factors in strategic planning. As the future creation of values lies within individual responsibility, this research empirically explored the limits (if any) of individual foresters¿ time horizons. To draw comparisons between countries with different traditions in forest management planning, data were collected through telephone surveys of forest managers in the state/national forest services of the Netherlands and Germany. In order to minimize other cultural differences, the research in Germany concentrated on the federal state of Nordrhein-Westfalen, which has considerable similarities with the Netherlands, e.g. in topography, forest types and forest functions. The results show that, in practice, 15 years appears to be the most distant horizon that foresters can identify with. This is in sharp contrast to the time horizons spanning decades and even generations that are always said to exist in forestry. The ¿doctrine of the long run¿¿the faith in the capacity of foresters to overcome the barriers of the uncertain future and look ahead and plan for long-range goals¿which in many countries still underlies traditional forest management, can therefore be rejected
Antihyperalgesia by α2-GABAA Receptors Occurs Via a Genuine Spinal Action and Does Not Involve Supraspinal Sites
- Author
- A Di Lio
- Alessandra Di Lio
- C Vidal
- CS Sang
- Dietmar Benke
- E Persohn
- FM Rivas
- G Munro
- G Munro
- GJ Bennett
- Gonzalo E Yévenes
- H Möhler
- HA Wieland
- Hanns Ulrich Zeilhofer
- HU Zeilhofer
- HU Zeilhofer
- HV Morris
- J Andre
- J Knabl
- J Knabl
- J Paul
- J Schouenborg
- JA Benson
- JA Coull
- JA Harris
- James M Cook
- Jean-Marc Fritschy
- JM Fritschy
- Jolly Paul
- JR Atack
- K Hösl
- K Löw
- L Jasmin
- Louis Scheurer
- MA Tatsuo
- NR Mirza
- P Scott-Stevens
- R Melzack
- R Witschi
- R Witschi
- RJ Harvey
- RM McKernan
- Robert Witschi
- RW Olsen
- S Ahmadi
- S Nickolls
- S Reichl
- TJ Luger
- U Rudolph
- U Rudolph
- Uwe Rudolph
- W Wisden
- William T Ralvenius
- Y Carrasquillo
- Publication venue
- 'Springer Science and Business Media LLC'
- Publication date
- 18/09/2013
- Field of study
Get PDFDrugs that enhance GABAergic inhibition alleviate inflammatory and neuropathic pain after spinal application. This antihyperalgesia occurs mainly through GABAA receptors (GABAARs) containing α2 subunits (α2-GABAARs). Previous work indicates that potentiation of these receptors in the spinal cord evokes profound antihyperalgesia also after systemic administration, but possible synergistic or antagonistic actions of supraspinal α2-GABAARs on spinal antihyperalgesia have not yet been addressed. Here we generated two lines of GABAAR-mutated mice, which either lack α2-GABAARs specifically from the spinal cord, or, which express only benzodiazepine-insensitive α2-GABAARs at this site. We analyzed the consequences of these mutations for antihyperalgesia evoked by systemic treatment with the novel non-sedative benzodiazepine site agonist HZ166 in neuropathic and inflammatory pain. Wild-type mice and both types of mutated mice had similar baseline nociceptive sensitivities and developed similar hyperalgesia. However, antihyperalgesia by systemic HZ166 was reduced in both mutated mouse lines by about 60% and was virtually indistinguishable from that of global point-mutated mice, in which all α2-GABAARs were benzodiazepine insensitive. The major (α2-dependent) component of GABAAR-mediated antihyperalgesia was therefore exclusively of spinal origin, whereas supraspinal α2-GABAARs had neither synergistic nor antagonistic effects on antihyperalgesia. Our results thus indicate that drugs that specifically target α2-GABAARs exert their antihyperalgesic effect through enhanced spinal nociceptive control. Such drugs may therefore be well-suited for the systemic treatment of different chronic pain conditions
Performance of the CMS Cathode Strip Chambers with Cosmic Rays
- Author
- Abadjiev K
- Abbaneo D
- Abbiendi G
- Abbrescia M
- Abdullin S
- Abelev B
- Acosta D
- Acosta JG
- Acosta MV
- Actis O
- Adam N
- Adam W
- Adams MR
- Adams T
- Adiguzel A
- Adler V
- Adolphi R
- Adzic P
- Afaq MA
- Agostino L
- Agram JL
- Aguilar-Benitez M
- Ahmad M
- Ahmad WH
- Ahmed I
- Ahmed W
- Ahuja S
- Aisa D
- Aisa S
- Akchurin N
- Akgun B
- Akgun U
- Akimenko S
- Akin IV
- Alagoz E
- Alampi G
- Albajar C
- Albayrak EA
- Alberdi J
- Albergo S
- Albert E
- Albrow M
- Alexander J
- Alidra M
- Aliev T
- Allfrey P
- Almeida N
- Altenhofer G
- Altsybeev I
- Alver B
- Alverson G
- Alves GA
- Amaglobeli N
- Amapane N
- Ambroglini F
- Amsler C
- Anagnostou G
- Ananthan B
- Anastassov A
- Andelin D
- Anderson M
- Andrea J
- Andreev V
- Andreev Y
- Anghel IM
- Anguelov T
- Anh T. Vu
- Anisimov A
- Antillon E
- Antipov P
- Antonelli L
- Anttila E
- Antunes JR
- Antunovic Z
- Apanasevich L
- Apollinari G
- Apresyan A
- Arce P
- Arcidiacono R
- Arenton MW
- Arfaei H
- Argiro S
- Arisaka K
- Arneodo M
- Arnold B
- Arora S
- Artamonov A
- Asaadi J
- Asghar MI
- Ashby S
- Askew A
- Atac M
- Atramentov O
- Auffray E
- Aurisano A
- Autermann C
- Avery P
- Avetisyan A
- Avila C
- Awan MIM
- Ayan AS
- Ayhan A
- Azhgirey I
- Aziz T
- Azzi P
- Azzurri P
- Baarmand MM
- Babb J
- Babucci E
- Baccaro S
- Bacchetta N
- Bacchi W
- Bachtis M
- Baden D
- Badgett W
- Baechler J
- Baer H
- Baesso P
- Baffioni S
- Bagby L
- Bagliesi G
- Bahk SY
- Bailleux D
- Baillon P
- Bainbridge R
- Bakhshiansohi H
- Bakirci MN
- Bakken JA
- Balazs M
- Baldin B
- Ball G
- Ball H
- Ballin J
- Bally SL
- Ban Y
- Bandurin D
- Banerjee S
- Banerjee S
- Banicz K
- Bansal S
- Banzuzi K
- Barashko V
- Barbagli G
- Barberis E
- Barbone L
- Barcala JM
- Barcellan L
- Bard R
- Bargassa P
- Baringer P
- Barnes VE
- Barnett BA
- Barney D
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- Bartalini P
- Bartoloni A
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- Bean A
- Beauceron S
- Beaudette F
- Beaumont W
- Bechtel F
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- Bedoya CF
- Beetz CP
- Behrens U
- Bejar JC
- Belforte S
- Beliy N
- Bell KW
- Bellan P
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- Bellato M
- Bellinger JN
- Belotelov I
- Benaglia A
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- Bendavid J
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- Benedetti D
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- Cheung HWK
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- Cirino G
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- Ciulli V
- Civinini C
- Claes DR
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- Hadley NJ
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- Hahn A
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- Publication venue
- 'IOP Publishing'
- Publication date
- 01/01/2009
- Field of study
Get PDFThe Cathode Strip Chambers (CSCs) constitute the primary muon tracking device
in the CMS endcaps. Their performance has been evaluated using data taken
during a cosmic ray run in fall 2008. Measured noise levels are low, with the
number of noisy channels well below 1%. Coordinate resolution was measured for
all types of chambers, and fall in the range 47 microns to 243 microns. The
efficiencies for local charged track triggers, for hit and for segments
reconstruction were measured, and are above 99%. The timing resolution per
layer is approximately 5 ns
Performance of CMS muon reconstruction in pp collision events at sqrt(s) = 7 TeV
- Author
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- Zoeller MH
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- Zumerle G
- Zuranski A
- Publication venue
- 'IOP Publishing'
- Publication date
- 01/01/2012
- Field of study
Get PDFThe performance of muon reconstruction, identification, and triggering in CMS
has been studied using 40 inverse picobarns of data collected in pp collisions
at sqrt(s) = 7 TeV at the LHC in 2010. A few benchmark sets of selection
criteria covering a wide range of physics analysis needs have been examined.
For all considered selections, the efficiency to reconstruct and identify a
muon with a transverse momentum pT larger than a few GeV is above 95% over the
whole region of pseudorapidity covered by the CMS muon system, abs(eta) < 2.4,
while the probability to misidentify a hadron as a muon is well below 1%. The
efficiency to trigger on single muons with pT above a few GeV is higher than
90% over the full eta range, and typically substantially better. The overall
momentum scale is measured to a precision of 0.2% with muons from Z decays. The
transverse momentum resolution varies from 1% to 6% depending on pseudorapidity
for muons with pT below 100 GeV and, using cosmic rays, it is shown to be
better than 10% in the central region up to pT = 1 TeV. Observed distributions
of all quantities are well reproduced by the Monte Carlo simulation.Comment: Replaced with published version. Added journal reference and DO
Performance of CMS muon reconstruction in pp collision events at sqrt(s) = 7 TeV
- Author
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- Abbiendi G
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- Zoeller MH
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- Zumerle G
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- Publication venue
- 'IOP Publishing'
- Publication date
- 01/01/2012
- Field of study
Get PDFThe performance of muon reconstruction, identification, and triggering in CMS
has been studied using 40 inverse picobarns of data collected in pp collisions
at sqrt(s) = 7 TeV at the LHC in 2010. A few benchmark sets of selection
criteria covering a wide range of physics analysis needs have been examined.
For all considered selections, the efficiency to reconstruct and identify a
muon with a transverse momentum pT larger than a few GeV is above 95% over the
whole region of pseudorapidity covered by the CMS muon system, abs(eta) < 2.4,
while the probability to misidentify a hadron as a muon is well below 1%. The
efficiency to trigger on single muons with pT above a few GeV is higher than
90% over the full eta range, and typically substantially better. The overall
momentum scale is measured to a precision of 0.2% with muons from Z decays. The
transverse momentum resolution varies from 1% to 6% depending on pseudorapidity
for muons with pT below 100 GeV and, using cosmic rays, it is shown to be
better than 10% in the central region up to pT = 1 TeV. Observed distributions
of all quantities are well reproduced by the Monte Carlo simulation.Comment: Replaced with published version. Added journal reference and DO
Identification and Filtering of Uncharacteristic Noise in the CMS Hadron Calorimeter
- Author
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- 01/01/1
- Field of study
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Performance of CMS hadron calorimeter timing and synchronization using test beam, cosmic ray, and LHC beam data
- Author
- Abadjiev K
- Abbaneo D
- Abbiendi G
- Abbrescia M
- Abdullin S
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- Taylor R
- Teischinger F
- Temple J
- Tenchini R
- Teng H
- Teo WD
- Teodorescu L
- Terentyev N
- Teyssier D
- Thea A
- Themel T
- Theofilatos K
- Thiebaux C
- Thom J
- Thomas M
- Thomas S
- Thomsen J
- Thyssen F
- Tikhonenko E
- Tikhonov A
- Timciuc V
- Timlin C
- Titov M
- Tkaczyk S
- To W
- Toback D
- Tokesi K
- Tolaini S
- Tomalin IR
- Tonelli G
- Toniolo N
- Tonjes MB
- Tonoiu D
- Tonwar SC
- Toole T
- Topakli H
- Topaksu AK
- Topkar A
- Torassa E
- Tornier D
- Toropin A
- Torre P
- Torromeo G
- Tosi M
- Toteva Z
- Toth N
- Tourneur S
- Tourtchanovitch L
- Traczyk P
- Tran NV
- Trapani PP
- Travaglini R
- Trayanov R
- Treille D
- Trentadue R
- Triantis FA
- Tricomi A
- Triossi A
- Tripathi M
- Trocino D
- Trocsanyi ZL
- Troendle D
- Troitsky S
- Tropea P
- Tropiano A
- Troshin S
- Troska J
- Trueb P
- Trunov A
- Tsang KV
- Tsiakkouri D
- Tsirigkas D
- Tsirou A
- Tucker J
- Tully C
- Tumanov A
- Tuominen E
- Tuominiemi J
- Tupputi S
- Tuura L
- Tuuva T
- Tuve C
- Twedt E
- Tytgat M
- Tyurin N
- Tzeng YM
- Ueno K
- Uhl D
- Ujvari B
- Ulmer K
- Ungaro D
- Uplegger L
- Uvarov L
- Uzun D
- Uzunian A
- Vaandering EW
- Valuev V
- Van Doninck W
- Van Haevermaet H
- Van Hove P
- Van Mechelen P
- Van Mulders P
- Van Remortel N
- Vander Donckt M
- Vander Velde C
- Vanelderen L
- Vanini S
- Vankov I
- Vanlaer P
- Vardanyan I
- Varela J
- Varelas N
- Vargas JER
- Vasil'ev S
- Vaughan J
- Vaurynovich S
- Vavilov S
- Vedaee A
- Veelken C
- Veillet L
- Velasco M
- Velichko G
- Velikzhanin Y
- Velthuis J
- Ventura S
- Venturi A
- Verdier P
- Verdini PG
- Veres GI
- Vergili LN
- Vergili M
- Verrecchia P
- Verwilligen P
- Veszpremi V
- Vesztergombi G
- Veverka J
- Vicini A
- Vidal R
- Vila I
- Vilar Cortabitarte R
- Villella I
- Vinogradov A
- Virdee T
- Visca L
- Vishnevskiy A
- Vishnevskiy D
- Vitulo P
- Viviani C
- Vizan Garcia JM
- Vlasov E
- Vlimant JR
- Vodopiyanov I
- Vogel H
- Volkov A
- Volkov S
- Volobouev I
- Volodko A
- Volpe R
- Volyanskyy D
- von Dratzig AS
- Vorobiev I
- Vorobyev A
- Voutilainen M
- Wagner P
- Wagner SR
- Wagner W
- Wagner-Kuhr J
- Wakefield S
- Wallny R
- Waltenberger W
- Walton R
- Walzel G
- Wan Z
- Wang CC
- Wang D
- Wang J
- Wang M
- Wang Z
- Warchol J
- Wardrope D
- Washington E
- Watts TL
- Wayne M
- Weber M
- Weber M
- Wehrli L
- Weinberg M
- Weinberger M
- Wendland L
- Weng J
- Weng Y
- Wenger EA
- Wenman D
- Wensveen M
- Werner JS
- Wertelaers P
- Wetzel J
- White A
- Whitmore J
- Whyntie T
- Wickens J
- Wicklund E
- Widl E
- Wigmans R
- Wildish T
- Wilke L
- Wilken R
- Wilkinson R
- Williams G
- Williams JC
- Williams JH
- Willmott C
- Wimpenny S
- Wingham M
- Winn D
- Wissing C
- Witherell M
- Wittich P
- Wittmer B
- Wlochal M
- Woehri HK
- Wolf R
- Womersley WJ
- Won S
- Wood JS
- Worm SD
- Wright D
- Wrochna G
- Wu S
- Wu W
- Wuerthwein F
- Wulz C-E
- Wyslouch B
- Xie S
- Xie Z
- Xue Z
- Yagil A
- Yan M
- Yang X
- Yang Y
- Yang ZC
- Yarba J
- Yaselli I
- Yazgan E
- Yelton J
- Yetkin T
- Yi K
- Yilmaz Y
- Yohay R
- Yoo HD
- Yoon AS
- York A
- Yumiceva F
- Yun JC
- Yuste C
- Zabi A
- Zabolotny W
- Zachariadou A
- Zalewski P
- Zampieri A
- Zanetti M
- Zang SL
- Zarubin A
- Zatzerklyany A
- Zeidler C
- Zeinali M
- Zeise M
- Zelepoukine S
- Zeuner WD
- Zeyrek M
- Zhang J
- Zhang L
- Zhang Y
- Zhang Z
- Zheng Y
- Zhiltsov V
- Zhokin A
- Zhu B
- Zhu K
- Zhu RY
- Zhukov V
- Zhukova V
- Ziebarth EB
- Zielinski M
- Zilizi G
- Zinonos Z
- Zito G
- Zoeller MH
- Zotto P
- Zub S
- Zumerle G
- Zuranski A
- Zuyeuski R
- Zych P
- Publication venue
- Institute of Physics Publishing
- Publication date
- 01/01/1
- Field of study
Get PDFThis paper discusses the design and performance of the time measurement technique and of the synchronization systems of the CMS hadron calorimeter. Time measurement performance results are presented from test beam data taken in the years 2004 and 2006. For hadronic showers of energy greater than 100 GeV, the timing resolution is measured to be about 1.2 ns. Time synchronization and out-of-time background rejection results are presented from the Cosmic Run At Four Tesla and LHC beam runs taken in the Autumn of 2008. The inter-channel synchronization is measured to be within ±2 ns
Ambient Stable Quantitative PCR Reagents for the Detection of Yersinia pestis
- Author
- AM Woron
- C Loiez
- C Wolff
- CA Whitehouse
- CF Felix
- CJ Chase
- CP Ooi
- D Wong
- DM Engelthaler
- Dongsheng Zhou
- F Kramer
- GP Anderson
- H Tomaso
- H Tomaso
- H Tsukano
- H Wei
- J Hinnebusch
- JA Higgins
- JP Amorij
- Junhui Zhai
- Kirsten E. Lyke
- L Radnedge
- LE Lindler
- Lei Zhou
- M Varma-Basil
- MD Braid
- ME Argall
- ME Scheurer
- MP Nunes
- OV Norkina
- P Thullier
- PE Saikaly
- Qinghai Shi
- R Ramanujam
- RA Greenfield
- RD Perry
- RJ Watson
- Ruifu Yang
- S Ayyadurai
- S Chanteau
- S Chanteau
- Shi Qu
- SR Gaval
- SS Iqbal
- T Skottman
- TV Inglesby
- Z Yan
- Zhaobiao Guo
- Publication venue
- Public Library of Science
- Publication date
- 01/01/2010
- Field of study
Get PDFPlague, caused by Yersinia pestis, is one of the oldest and most dangerous diseases in human history, and has claimed millions of lives in the three major historical pandemics. Although panic caused by the Black Death is fading, the threat of the reemergence of plague pandemics still exists, with the additional potential of misuse in biowarfare or bioterrorism. Rapid on-site detection and identification of the pathogen is of paramount significance for timely implementation of effective countermeasures. TaqMan probe-based real-time PCR assays can give quick and accurate identification; however, the need for cold delivery and storage prevents its potential on-site application. The objective of this study was to develop a stable PCR system for easy delivery and storage under room temperature, which is vital for conventional plague surveillance and for preparedness in public health emergencies. We present a solution to this particular issue, hoping that it is helpful to future applications
Reduced Expression of Brain-Enriched microRNAs in Glioblastomas Permits Targeted Regulation of a Cell Death Gene
- Author
- B Kefas
- BD Brown
- BD Brown
- BJ Huntly
- BP Lewis
- Bryan R. Cullen
- C Beltinger
- C Conaco
- C Evangelisti
- C Wu
- Consuelo Borras
- CS Cobbs
- DA Mitchell
- DS Schwarz
- E Gottwein
- E Marti
- EJ Kelly
- FL Moolten
- G Gabriely
- GA Calin
- H Ohgaki
- H Ohgaki
- H Ohgaki
- H Seitz
- HI Im
- J Godlewski
- J Godlewski
- J Lu
- J Silber
- JA Chan
- JC Pang
- JL Umbach
- JR Crawford
- JR Crawford
- JS Yang
- JT Huse
- K Nishikura
- KJ Pulkkanen
- L Shi
- LF Sempere
- MB Eisen
- ME Klein
- ME Scheurer
- MR Friedlander
- MS Maginnis
- MT Le
- MV Iorio
- NG Rainov
- PY Wen
- R Ronen
- RC Friedman
- Rebecca L. Skalsky
- RL Skalsky
- S Griffiths-Jones
- S Meseguer
- S Volinia
- SA Ciafre
- SK Singh
- SK Singh
- ST Magill
- X Li
- Y Kawahara
- Y Kawahara
- Y Kawahara
- Y Zhang
- Publication venue
- Public Library of Science
- Publication date
- 02/09/2011
- Field of study
Get PDFGlioblastoma is a highly aggressive malignant tumor involving glial cells in the human brain. We used high-throughput sequencing to comprehensively profile the small RNAs expressed in glioblastoma and non-tumor brain tissues. MicroRNAs (miRNAs) made up the large majority of small RNAs, and we identified over 400 different cellular pre-miRNAs. No known viral miRNAs were detected in any of the samples analyzed. Cluster analysis revealed several miRNAs that were significantly down-regulated in glioblastomas, including miR-128, miR-124, miR-7, miR-139, miR-95, and miR-873. Post-transcriptional editing was observed for several miRNAs, including the miR-376 family, miR-411, miR-381, and miR-379. Using the deep sequencing information, we designed a lentiviral vector expressing a cell suicide gene, the herpes simplex virus thymidine kinase (HSV-TK) gene, under the regulation of a miRNA, miR-128, that was found to be enriched in non-tumor brain tissue yet down-regulated in glioblastomas, Glioblastoma cells transduced with this vector were selectively killed when cultured in the presence of ganciclovir. Using an in vitro model to recapitulate expression of brain-enriched miRNAs, we demonstrated that neuronally differentiated SH-SY5Y cells transduced with the miRNA-regulated HSV-TK vector are protected from killing by expression of endogenous miR-128. Together, these results provide an in-depth analysis of miRNA dysregulation in glioblastoma and demonstrate the potential utility of these data in the design of miRNA-regulated therapies for the treatment of brain cancers
Human monoclonal antibodies targeting carbonic anhydrase IX for the molecular imaging of hypoxic regions in solid tumours
- Author
- A Ammar
- A Cecchi
- A Chrastina
- A Chrastina
- A Pini
- A Thiry
- A Villa
- AH Brouwers
- AM Wu
- AM Wu
- B Jankovic
- BM Tijink
- C Pendley
- C Schliemann
- C Schliemann
- CC Wykoff
- CC Wykoff
- CT Supuran
- D Berndorff
- D Neri
- D Neri
- D Schrama
- DJ Chaplin
- E El Emir
- E El-Emir
- E Svastová
- EF Fidarova
- F Viti
- FG van Schaijk
- G Hale
- G Payne
- G Walsh
- G Winter
- G Winter
- GK Miller
- GP Adams
- GP Adams
- HH Street
- IM Tomlinson
- J Chiche
- J Folkman
- J K J Ahlskog
- J Mårlind
- J Pouyssegur
- J van Dijk
- JA Bertout
- JA Loncaster
- JE Schnitzer
- JL Dearling
- JN Rybak
- JV Leyton
- K Bosslet
- K Grabmaier
- K Zuberbühler
- L Borsi
- L Borsi
- L Dubois
- L Tarli
- LG Presta
- LH Wei
- M Hockel
- M Silacci
- M Silacci
- M Weinmann
- MC Brahimi-Horn
- MI Koukourakis
- MS Dennis
- NJ Beasley
- NM Mazure
- P Staller
- P Vaupel
- PE Thorpe
- PJ Carter
- PJ Carter
- PJ Hoskin
- PL Olive
- PS Low
- R B Pedley
- R Kerbel
- RD Hofheinz
- RK Jain
- S Demartis
- S Pastorekova
- S Sauer
- S Sobhanifar
- SB Scheurer
- SC Williams
- SS Brack
- T Ebert
- T Olafsen
- T von Lukowicz
- T Yokota
- TB Lavoie
- U Qureshi
- V Castronovo
- V Kenanova
- WK Rathmell
- XF Li
- Y Pocker
- Publication venue
- Nature Publishing Group
- Publication date
- 01/01/2009
- Field of study
Get PDFBACKGROUND: Hypoxia, which is commonly observed in areas of primary tumours and of metastases, influences response to treatment. However, its characterisation has so far mainly been restricted to the ex vivo analysis of tumour sections using monoclonal antibodies specific to carbonic anhydrase IX (CA IX) or by pimonidazole staining, after the intravenous administration of this 2-nitroimidazole compound in experimental animal models.METHODS: In this study, we describe the generation of high-affinity human monoclonal antibodies (A3 and CC7) specific to human CA IX, using phage technology.RESULTS: These antibodies were able to stain CA IX ex vivo and to target the cognate antigen in vivo. In one of the two animal models of colorectal cancer studied (LS174T), CA IX imaging closely matched pimonidazole staining, with a preferential staining of tumour areas characterised by little vascularity and low perfusion. In contrast, in a second animal model (SW1222), distinct staining patterns were observed for pimonidazole and CA IX targeting. We observed a complementary pattern of tumour regions targeted in vivo by the clinical-stage vascular-targeting antibody L19 and the anti-CA IX antibody A3, indicating that a homogenous pattern of in vivo tumour targeting could be achieved by a combination of the two antibodies.CONCLUSION: The new human anti-CA IX antibodies are expected to be non-immunogenic in patients with cancer and may serve as broadly applicable reagents for the non-invasive imaging of hypoxia and for pharmacodelivery applications. British Journal of Cancer (2009) 101, 645-657. doi: 10.1038/sj.bjc.6605200 www.bjcancer.com Published online 21 July 2009 (C) 2009 Cancer Research U
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