TY - JOUR

T1 - Design, Synthesis, and Cytotoxic Evaluation of New Structurally Simplified and Highly Potent Third-Generation Tubulysin Derivatives

AU - Yadav, Kratika

AU - Kalita, Tapash

AU - Sharma, Lekhnath

AU - Pandit, Amit

AU - Pathak, Biswarup

AU - Dräger, Gerald

AU - Kirschning, Andreas

AU - Chelvam, Venkatesh

N1 - Publisher Copyright: © 2025 Wiley-VCH GmbH.

PY - 2025/8/19

Y1 - 2025/8/19

N2 - Tubulysins belong to a class of natural products originally isolated from myxobacteria culture and are known to induce cell apoptosis through inhibition of microtubule assembly. Herein, we report the computationally designed, structurally simplified, and first solid-phase peptide synthesis of novel third-generation tubulin inhibitors in high yields. These inhibitors are devoid of tubuvaline and tubuphenylalanine fragments previously considered essential for tubulin inhibition activity. The most potent inhibitor contains four fragments arranged from the N terminal to the C terminal as N-methyl pipecolic acid, isoleucine, valine-thiazole, and asparagine. The hydrophilic tubulin inhibitors demonstrated significant anticancer activity, with IC50 values in the low nanomolar range (IC50 = 13–53 nM) within a 48 hours incubation period across prostate, lung, breast, skin, and cervical cancer cell lines. The synthetic strategy incorporates a simplified valine-thiazole ring structure, retaining both biological activity and chiral integrity of the molecules. The method enables the synthesis of potent tubulin inhibitors by avoiding multistep synthetic and purification procedures, supporting the inhibitor's applicability for large-scale synthesis and potential therapeutic development. The structural modifications at the N-terminal result in the loss of activity from nM to µM range, whereas the C-terminal modification had minimal impact on the potency.

AB - Tubulysins belong to a class of natural products originally isolated from myxobacteria culture and are known to induce cell apoptosis through inhibition of microtubule assembly. Herein, we report the computationally designed, structurally simplified, and first solid-phase peptide synthesis of novel third-generation tubulin inhibitors in high yields. These inhibitors are devoid of tubuvaline and tubuphenylalanine fragments previously considered essential for tubulin inhibition activity. The most potent inhibitor contains four fragments arranged from the N terminal to the C terminal as N-methyl pipecolic acid, isoleucine, valine-thiazole, and asparagine. The hydrophilic tubulin inhibitors demonstrated significant anticancer activity, with IC50 values in the low nanomolar range (IC50 = 13–53 nM) within a 48 hours incubation period across prostate, lung, breast, skin, and cervical cancer cell lines. The synthetic strategy incorporates a simplified valine-thiazole ring structure, retaining both biological activity and chiral integrity of the molecules. The method enables the synthesis of potent tubulin inhibitors by avoiding multistep synthetic and purification procedures, supporting the inhibitor's applicability for large-scale synthesis and potential therapeutic development. The structural modifications at the N-terminal result in the loss of activity from nM to µM range, whereas the C-terminal modification had minimal impact on the potency.

KW - anticancer

KW - computational design

KW - microtubule

KW - solid-phase peptide synthesis

KW - tubulin inhibitor

KW - tubulysin

UR - http://www.scopus.com/inward/record.url?scp=105012147847&partnerID=8YFLogxK

U2 - 10.1002/chem.202501965

DO - 10.1002/chem.202501965

M3 - Article

AN - SCOPUS:105012147847

VL - 31

JO - Chemistry - a European journal

JF - Chemistry - a European journal

SN - 0947-6539

IS - 46

M1 - e01965

ER -