Ligand bias underlies differential signaling of multiple FGFs
via FGFR1

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Ligand bias underlies differential signaling of multiple FGFs via FGFR1

Přehled o publikaci

J 2024

Ligand bias underlies differential signaling of multiple FGFs via FGFR1

KARL, Kelly, Del Piccolo NUALA, Taylor LIGHT, Tanaya ROY, Pooja DUDEJA et. al.

Základní údaje

Originální název

Ligand bias underlies differential signaling of multiple FGFs via FGFR1

Autoři

KARL, Kelly, Del Piccolo NUALA, Taylor LIGHT, Tanaya ROY, Pooja DUDEJA, Vlad-Constantin URSACHI, Bohumil FAFÍLEK, Pavel KREJČÍ a Kalina HRISTOVA

Vydání

eLife, CAMBRIDGE, ELIFE SCIENCES PUBL LTD, 2024, 2050-084X

Další údaje

Jazyk

angličtina

Typ výsledku

Článek v odborném periodiku

Stát vydavatele

Velká Británie a Severní Irsko

Utajení

není předmětem státního či obchodního tajemství

Odkazy

URL

Organizace

Lékařská fakulta – Masarykova univerzita – Repozitář

DOI

http://dx.doi.org/10.7554/eLife.88144

UT WoS

001196755600001

EID Scopus

2-s2.0-85190082610

Klíčová slova anglicky

signal transduction; FGFR; biased signaling; None

Návaznosti

GA19-20123S, projekt VaV. GF21-26400K, projekt VaV. LX22NPO5102, projekt VaV. MUNI/G/1771/2020, interní kód Repo. NU21-06-00512, projekt VaV.

Změněno: 16. 10. 2024 00:50, RNDr. Daniel Jakubík

Anotace

V originále

The differential signaling of multiple FGF ligands through a single fibroblast growth factor (FGF) receptor (FGFR) plays an important role in embryonic development. Here, we use quantitative biophysical tools to uncover the mechanism behind differences in FGFR1c signaling in response to FGF4, FGF8, and FGF9, a process which is relevant for limb bud outgrowth. We find that FGF8 preferentially induces FRS2 phosphorylation and extracellular matrix loss, while FGF4 and FGF9 preferentially induce FGFR1c phosphorylation and cell growth arrest. Thus, we demonstrate that FGF8 is a biased FGFR1c ligand, as compared to FGF4 and FGF9. Forster resonance energy transfer experiments reveal a correlation between biased signaling and the conformation of the FGFR1c transmembrane domain dimer. Our findings expand the mechanistic understanding of FGF signaling during development and bring the poorly understood concept of receptor tyrosine kinase ligand bias into the spotlight.

Přiložené soubory

https://is.muni.cz/publication/2407657/Ligand_bias_underlies_differential_signaling_of_multiple_FGFs_via_FGFR1.pdf

Citovat

KARL, Kelly, Del Piccolo NUALA, Taylor LIGHT, Tanaya ROY, Pooja DUDEJA, Vlad-Constantin URSACHI, Bohumil FAFÍLEK, Pavel KREJČÍ a Kalina HRISTOVA. Ligand bias underlies differential signaling of multiple FGFs via FGFR1. eLife. CAMBRIDGE: ELIFE SCIENCES PUBL LTD, 2024, roč. 12, April 2024, s. 1-28. ISSN 2050-084X. Dostupné z: https://dx.doi.org/10.7554/eLife.88144.

@article{61469,
   author = {Karl, Kelly and Nuala, Del Piccolo and Light, Taylor and Roy, Tanaya and Dudeja, Pooja and Ursachi, VladandConstantin and Fafílek, Bohumil and Krejčí, Pavel and Hristova, Kalina},
   article_location = {CAMBRIDGE},
   article_number = {April 2024},
   doi = {http://dx.doi.org/10.7554/eLife.88144},
   keywords = {signal transduction; FGFR; biased signaling; None},
   language = {eng},
   issn = {2050-084X},
   journal = {eLife},
   title = {Ligand bias underlies differential signaling of multiple FGFs via FGFR1},
   url = {https://elifesciences.org/articles/88144},
   volume = {12},
   year = {2024}
}

TY  - JOUR
ID  - 61469
AU  - Karl, Kelly - Nuala, Del Piccolo - Light, Taylor - Roy, Tanaya - Dudeja, Pooja - Ursachi, Vlad-Constantin - Fafílek, Bohumil - Krejčí, Pavel - Hristova, Kalina
PY  - 2024
TI  - Ligand bias underlies differential signaling of multiple FGFs via FGFR1
JF  - eLife
VL  - 12
IS  - April 2024
SP  - 1-28
EP  - 1-28
PB  - ELIFE SCIENCES PUBL LTD
SN  - 2050-084X
KW  - signal transduction
KW  - FGFR
KW  - biased signaling
KW  - None
UR  - https://elifesciences.org/articles/88144
N2  - The differential signaling of multiple FGF ligands through a single fibroblast growth factor (FGF) receptor (FGFR) plays an important role in embryonic development. Here, we use quantitative biophysical tools to uncover the mechanism behind differences in FGFR1c signaling in response to FGF4, FGF8, and FGF9, a process which is relevant for limb bud outgrowth. We find that FGF8 preferentially induces FRS2 phosphorylation and extracellular matrix loss, while FGF4 and FGF9 preferentially induce FGFR1c phosphorylation and cell growth arrest. Thus, we demonstrate that FGF8 is a biased FGFR1c ligand, as compared to FGF4 and FGF9. Forster resonance energy transfer experiments reveal a correlation between biased signaling and the conformation of the FGFR1c transmembrane domain dimer. Our findings expand the mechanistic understanding of FGF signaling during development and bring the poorly understood concept of receptor tyrosine kinase ligand bias into the spotlight.
ER  -

KARL, Kelly, Del Piccolo NUALA, Taylor LIGHT, Tanaya ROY, Pooja DUDEJA, Vlad-Constantin URSACHI, Bohumil FAFÍLEK, Pavel KREJČÍ a Kalina HRISTOVA. Ligand bias underlies differential signaling of multiple FGFs via FGFR1. \textit{eLife}. CAMBRIDGE: ELIFE SCIENCES PUBL LTD, 2024, roč.~12, April 2024, s.~1-28. ISSN~2050-084X. Dostupné z: https://dx.doi.org/10.7554/eLife.88144.