TY - JOUR
T1 - Semisynthesis of segmentally isotope-labeled and site-specifically palmitoylated CD44 cytoplasmic tail
AU - Vogl, Dominik P.
AU - Mateos, Borja
AU - Migotti, Mario
AU - Felkl, Manuel
AU - Conibear, Anne C.
AU - Konrat, Robert
AU - Becker, Christian F.W.
N1 - Accession Number: WOS:001174332800001
PubMed ID: 38306881
PY - 2024/2/15
Y1 - 2024/2/15
N2 - CD44, a ubiquitously expressed transmembrane receptor, plays a crucial role in cell growth, migration, and tumor progression. Dimerization of CD44 is a key event in signal transduction and has emerged as a potential target for anti-tumor therapies. Palmitoylation, a posttranslational modification, disrupts CD44 dimerization and promotes CD44 accumulation in ordered membrane domains. However, the effects of palmitoylation on the structure and dynamics of CD44 at atomic resolution remain poorly understood. Here, we present a semisynthetic approach combining solid-phase peptide synthesis, recombinant expression, and native chemical ligation to investigate the impact of palmitoylation on the cytoplasmic domain (residues 669-742) of CD44 (CD44ct) by NMR spectroscopy. A segmentally isotope-labeled and site-specifically palmitoylated CD44 variant enabled NMR studies, which revealed chemical shift perturbations and indicated local and long-range conformational changes induced by palmitoylation. The long-range effects suggest altered intramolecular interactions and potential modulation of membrane association patterns. Semisynthetic, palmitoylated CD44ct serves as the basis for studying CD44 clustering, conformational changes, and localization within lipid rafts, and could be used to investigate its role as a tumor suppressor and to explore its therapeutic potential.
AB - CD44, a ubiquitously expressed transmembrane receptor, plays a crucial role in cell growth, migration, and tumor progression. Dimerization of CD44 is a key event in signal transduction and has emerged as a potential target for anti-tumor therapies. Palmitoylation, a posttranslational modification, disrupts CD44 dimerization and promotes CD44 accumulation in ordered membrane domains. However, the effects of palmitoylation on the structure and dynamics of CD44 at atomic resolution remain poorly understood. Here, we present a semisynthetic approach combining solid-phase peptide synthesis, recombinant expression, and native chemical ligation to investigate the impact of palmitoylation on the cytoplasmic domain (residues 669-742) of CD44 (CD44ct) by NMR spectroscopy. A segmentally isotope-labeled and site-specifically palmitoylated CD44 variant enabled NMR studies, which revealed chemical shift perturbations and indicated local and long-range conformational changes induced by palmitoylation. The long-range effects suggest altered intramolecular interactions and potential modulation of membrane association patterns. Semisynthetic, palmitoylated CD44ct serves as the basis for studying CD44 clustering, conformational changes, and localization within lipid rafts, and could be used to investigate its role as a tumor suppressor and to explore its therapeutic potential.
KW - CD44
KW - Native chemical ligation
KW - Paramagnetic Relaxation Enhancement (PRE)
KW - Protein lipidation
KW - Protein NMR
KW - Protein semisynthesis
KW - Segmental isotope labeling
KW - Solid phase peptide synthesis
UR - http://www.scopus.com/inward/record.url?scp=85183941155&partnerID=8YFLogxK
U2 - 10.1016/j.bmc.2024.117617
DO - 10.1016/j.bmc.2024.117617
M3 - Article
C2 - 38306881
AN - SCOPUS:85183941155
SN - 0968-0896
VL - 100
JO - Bioorganic and Medicinal Chemistry
JF - Bioorganic and Medicinal Chemistry
M1 - 117617
ER -