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14 research outputs found

Receptor Tyrosine Kinases in Osteosarcoma: 2019 Update

Author: A Arthur
A Drilon
A Gattelli
A Giaccia
A Girnita
A Gvozdenovic
A Longhi
A Raciborska
A Rettew
A Safwat
A Varelias
A Waraky
AE Armstrong
AN Rettew
AS Pappo
B Davaadelger
B Gobin
B Zhu
BC Widemann
C Collier
C DeRenzo
C Jian
C Mancarella
D Kitagawa
D Mahadevan
D Warsito
D Weekes
D Yu
E Fox
EA Kolb
EA Kolb
EB Pasquale
EB Rankin
ER Sampson
F Duffaud
F Li
F Luk
F Navid
F Sevelda
G Chen
G Grignani
G Grignani
GK Schwartz
H Yang
H Zhao
HG Ljunggren
I Asmane
I Gudernova
J Campbell
J Dong
J Han
J Hong
J Posthumadeboer
J Xu
JB Allard
JD Vasta
JH Pahl
JI Geller
JL Glade Bender
K Baird
K Marley
K Mross
K Scotlandi
K Takeuchi
K Umeda
K Zhang
K Zheng
KA Lodhia
KV Myers
L Chen
L Cheng
L Maniscalco
L Xie
L Xie
LE Davis
LM Wagner
M Ahmadi
M Bond
M Fernanda Amary
M Gaebler
M Penel-Page
M Rovithi
M Rovithi
M Schoumacher
MI Davis
MK Chuk
ML Kuijjer
MS Kariolis
MS Kariolis
N Berlow
N Habel
N Jaffe
N Jiang
NJ Sumi
NK McDaniel
P Anderson
P Chaiyawat
P Hingorani
P Kanlikilicer
P Messerschmitt
PA Meyers
PI Croucher
PJ Beltran
PJ Pan
PM Anderson
R Aplenc
R Barco
R Cathomas
R Chugh
R Fritsche-Guenther
R Roskoski Jr
R Solomon-Zemler
R Tian
R Yang
RD Roberts
RM Kumar
RT Kurmasheva
S Avnet
S Behjati
S Kallus
S Klaeger
S Kumar
S Tian
S Tonna
SG Dubois
SG Kimani
SI Yamaguchi
SJ Holland
SM Schuetze
SM Wilhelm
T Aleksic
T Baroy
T Higuchi
T Higuchi
T Jentzsch
T Nakano
T Seto
T Shimizu
T Shimizu
T Tanaka
TA Aguilera
TM Brand
U Basu-Roy
V Guagnano
VB Sampson
W Zhang
X Tan
X Wu
X Ye
X Zhao
Y Bai
Y Cao
Y Cha
Y Chen
Y Dong
Y Liu
Y Pignochino
Y Pignochino
Y Su
Y Wang
Y Zhang
Y Zhou
YH Wang
YP Mosse
YT Akalu
Z Duan
Z Liao
Z Tian
Z Wang
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2020
Field of study

The primary conclusions of our 2014 contribution to this series were as follows: Multiple receptor tyrosine kinases (RTKs) likely contribute to aggressive phenotypes in osteosarcoma and, therefore, inhibition of multiple RTKs is likely necessary for successful clinical outcomes. Inhibition of multiple RTKs may also be useful to overcome resistance to inhibitors of individual RTKs as well as resistance to conventional chemotherapies. Different combinations of RTKs are likely important in individual patients. AXL, EPHB2, FGFR2, IGF1R, and RET were identified as promising therapeutic targets by our in vitro phosphoproteomic/siRNA screen of 42 RTKs in the highly metastatic LM7 and 143B human osteosarcoma cell lines. This chapter is intended to provide an update on these topics as well as the large number of osteosarcoma clinical studies of inhibitors of multiple tyrosine kinases (multi-TKIs) that were recently published

ScholarWorks IU Indianapolis

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AXL degradation in combination with EGFR-TKI can delay and overcome acquired resistance in human non-small cell lung cancer cells

Author: AS Meyer
B Halmos
BC Varnum
C Wilson
CK Liam
DH Bach
DH Bach
ES Linklater
F Passiglia
G Lemke
GM Burslem
H Axelrod
H Taniguchi
H Uramoto
H Zhang
HN Kang
HY Min
I Ben-Batalla
J Antony
J Antony
J Antony
J Boshuizen
J Muller
J Soh
JY Hong
K Jacobsen
K Raina
KM Giles
M Elkabets
M Gunther
MA Goyette
MK Asiedu
MS Kariolis
MS Kariolis
N Karachaliou
N Normanno
S Ammoun
SG Wu
SK Jo
SY Bae
SY Bae
TA Aguilera
TC Chou
TC Chou
TM Brand
TM Brand
TY Kim
WK Kim
Z Yang
ZF Zhang
Publication venue: 'Springer Science and Business Media LLC'
Publication date
Field of study

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Small molecule inhibitors block Gas6-inducible TAM activation and tumorigenicity

Author: A Kirane
A Verma
A Zagorska
AB Lee-Sherick
AK Keating
AS Meyer
AT Laurie
CT Cummings
CT Cummings
CV Rothlin
CV Rothlin
D Trommeshauser
DJ Diller
DK Graham
DN Debruyne
EB Rankin
F Saller
F Wu
G Lemke
HM Seitz
IK Park
J Liu
J Schlegel
JF Gainor
JJ Irwin
JJ Irwin
JM Cosemans
K Wnuk-Lipinska
KH Knubel
KM Giles
KQ Nguyen
L Meertens
M Elkabets
M Paolino
MD Blostein
MK Asiedu
MK Callahan
MS Kariolis
MS Kariolis
MW Schmitt
N Bansal
NY Kim
O Martinho
O Trott
Q Lu
R Hamel
RB Birge
RM Linger
RM Linger
RM Linger
RS Cook
S Kumar
S Kumar
S Xie
SG Kimani
SG Kimani
SH Myers
SJ Holland
T Sasaki
TA Halgren
TM Brand
TM Brand
TN Stitt
W Ji
WI Tsou
WR Gould
X Ye
Z Zhang
Publication venue: 'Springer Science and Business Media LLC'
Publication date
Field of study

Crossref

Directed evolution of a soluble human DR3 receptor for the inhibition of TL1A induced cytokine secretion

Author: A Aharoni
A Aharoni
A Herman
Amir Aharoni
BP Pappu
C Zhan
D Amar
F Meylan
F Meylan
G Bamias
G Bamias
G Chao
H Tao
HA Young
Itay Levin
J Bayry
J Yang
Jagadeesh Bayry
JD Bloom
JH Naismith
JM Gershoni
K Yamazaki
KA Papadakis
KY Yu
L Fang
LJ Chew
M Lehmann
M Umetsu
M Zaretsky
MA Cassatella
Marianna Zaretsky
MJ Bull
MS Kariolis
RM Pitti
S Bershtein
S Lutz
SA Gai
TL Tootle
TS Migone
WP Stemmer
Publication venue: 'Public Library of Science (PLoS)'
Publication date
Field of study

Crossref

Determination of equilibrium dissociation constants for recombinant antibodies by high-throughput affinity electrophoresis

Author: A Azimzadeh
A Bradbury
A Bromberg
AA Apori
AE Herr
AHC Ng
AJ Hughes
AJ Hughes
AJ Hughes
B Friguet
B Hadimioglu
C-C Kang
CM Hammers
DJ Winzor
ET Boder
F Hardy
G Gauglitz
G Rippel
G Roncador
H Waldmann-Meyer
J Bordeaux
JM Reichert
JR Birch
JW Goding
K Karns
K Karns
LA Sternberger
M Baker
M Hornsby
M Kiyoshi
MA Kapil
MK Araz
MS Kariolis
P Estep
P Mitchell
P Schuck
R Jefferis
R Karlsson
RW Wood
S Sirin
SN Krylov
SP Mulvaney
T Sulea
TA Duncombe
TM Squires
W Weiss
Y Gao
Y Pan
Y Pan
YN Abdiche
Publication venue: 'Springer Science and Business Media LLC'
Publication date
Field of study

Crossref

Immunogenomic engineering of a plug-and-(dis)play hybridoma platform

Author: A Bradbury
A Krebber
AJ Lam
B Ramesh
BR Harvey
CD Richardson
DG Gibson
FA Ran
FM Wurm
G Georgiou
G Köhler
H Liu
HP Fell
HR Hoogenboom
IB Hilton
J Chusainow
J Fang
J Hanes
J Li
JA Van Deventer
JD Sander
JE DiCarlo
JG Doench
JG Zalatan
JM Geisinger
JY Kim
KJ Morrow
L Cong
L M Barnes
LE Macdonald
M Jinek
M Shulman
MD Baker
MD Baker
MD Baker
MJ Feldhaus
MS Kariolis
O Brady
P Ng
RA Horlick
RJ Platt
S Geisse
S Kredel
S Schlatter
S Turan
SCL Ho
SR Bruce
ST Reddy
T Gaj
T Jostock
T Maruyama
T-C Cheong
TA Khan
TG Phan
VT Chu
W Shi
X Qiu
X Qiu
Y Fu
YQ Feng
Z Mao
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2016
Field of study

Hybridomas, fusions of primary mouse B cells and myelomas, are stable, rapidly-proliferating cell lines widely utilized for antibody screening and production. Antibody specificity of a hybridoma clone is determined by the immunoglobulin sequence of the primary B cell. Here we report a platform for rapid reprogramming of hybridoma antibody specificity by immunogenomic engineering. Here we use CRISPR-Cas9 to generate double-stranded breaks in immunoglobulin loci, enabling deletion of the native variable light chain and replacement of the endogenous variable heavy chain with a fluorescent reporter protein (mRuby). New antibody genes are introduced by Cas9-targeting of mRuby for replacement with a donor construct encoding a light chain and a variable heavy chain, resulting in full-length antibody expression. Since hybridomas surface express and secrete antibodies, reprogrammed cells are isolated using flow cytometry and cell culture supernatant is used for antibody production. Plug-and-(dis)play hybridomas can be reprogrammed with only a single transfection and screening step

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PubMed Central