Naphthoindole-2-carboxamides as a lipophilic chemotype of hetarene-anthraquinones potent against P-gp resistant tumor cells

Valeria A Litvinova; Vladimir B Tsvetkov; Yulia L Volodina; Lyubov G Dezhenkova; Alina A Markova; Minh Tuan Nguyen; Alexander S Tikhomirov; Andrey E Shchekotikhin

doi:10.1016/j.ejmech.2024.117013

Naphthoindole-2-carboxamides as a lipophilic chemotype of hetarene-anthraquinones potent against P-gp resistant tumor cells

Eur J Med Chem. 2024 Oct 30:281:117013. doi: 10.1016/j.ejmech.2024.117013. Online ahead of print.

Authors

Valeria A Litvinova¹, Vladimir B Tsvetkov², Yulia L Volodina³, Lyubov G Dezhenkova¹, Alina A Markova⁴, Minh Tuan Nguyen⁴, Alexander S Tikhomirov¹, Andrey E Shchekotikhin⁵

Affiliations

¹ Gause Institute of New Antibiotics, 11 B. Pirogovskaya Street, Moscow, 119021, Russia.
² Center for Mathematical Modeling in Drug Development, Sechenov First Moscow State Medical University, 8-2 Trubetskaya, 119991, Moscow, Russia; Lopukhin Federal Research and Clinical Center of Physical-Chemical Medicine, 1A M. Pirogovskaya Street, Moscow, 119435, Russia.
³ Gause Institute of New Antibiotics, 11 B. Pirogovskaya Street, Moscow, 119021, Russia; Blokhin National Medical Center of Oncology, 24 Kashirskoye Shosse, Moscow, 115478, Russia.
⁴ Emanuel Institute of Biochemical Physics, Russian Academy of Sciences, 4 Kosygin Street, Moscow, 119334, Russia.
⁵ Gause Institute of New Antibiotics, 11 B. Pirogovskaya Street, Moscow, 119021, Russia. Electronic address: [email protected].

PMID: 39500064
DOI: 10.1016/j.ejmech.2024.117013

Abstract

The acquisition of multidrug resistance (MDR) to chemotherapy is a major obstacle to successful cancer treatment. Aiming to improve the potency of anthraquinone-derived antitumor compounds against MDR cancer cells, we employed a rational design approach to develop new heteroarene-fused anthraquinones. Shifting the carboxamide group in the naphtho[2,3-f]indole scaffold from the 3-position to 2 increased the lipophilicity and P-glycoprotein (P-gp) binding of the derivatives, potentially enhancing their ability to circumvent P-gp-mediated MDR. To validate the computations, we developed a scheme for heterocyclization into esters of naphtho[2,3-f]indole-2-carboxylic acid, based on the 5-endo-dig cyclization of 2-alkynyl-3-amino-1,4-dimethoxyanthraquinone under mild basic conditions using tetra-n-butylammonium fluoride (TBAF). The synthesized naphthoindole-2-carboxamides, particularly compound 1a bearing (S)-3-aminopyrrolidine in the carboxamide fragment, demonstrated the highest antiproliferative activity. Most importantly, 1a suppressed the growth of the P-gp-positive K562/4 leukemia tumor cell line (resistance index = 2.4), while its 3-isomer LCTA-2640 and Dox did not (RI = 125 and 140, respectively). Studies of intracellular uptake and distribution showed that 1a, unlike its 3-substituted isomer, effectively accumulated in resistant tumor cells, confirming the correlation between in silico and experimental data. The lead compound 1a interacts with DNA duplex and inhibits topoisomerase 1 but does not induce oxidative stress. Treatment with 1a increases the population of apoptotic cells in both K562 and K562/4 sublines, regardless of the cell cycle phase. Taken together, this work provides an interesting example of how a little modification in chemical structure can lead to striking differences in antitumor properties. In conclusion, we have identified a potent class of compounds that offer distinct advantages in combating resistant tumor cells.

Keywords: Anthraquinone; Antiproliferative activity; Heterocyclization; Indole; Multidrug resistance; P-glycoprotein; Rational design; Topoisomerase 1.