Fokin Artem I, Chuprov-Netochin Roman N, Malyshev Alexander S, Romero Stéphane, Semenova Marina N, Konyushkin Leonid D, Leonov Sergey V, Semenov Victor V, Gautreau Alexis M
CNRS UMR7654, Ecole Polytechnique, Institut Polytechnique de Paris, Palaiseau, France.
Department of Molecular and Bio Physics, Moscow Institute of Physics and Technology, Dolgoprudny, Russia.
Front Pharmacol. 2022 May 30;13:896994. doi: 10.3389/fphar.2022.896994. eCollection 2022.
Branched actin networks polymerized by the Actin-related protein 2 and 3 (Arp2/3) complex play key roles in force generation and membrane remodeling. These networks are particularly important for cell migration, where they drive membrane protrusions of lamellipodia. Several Arp2/3 inhibitory compounds have been identified. Among them, the most widely used is CK-666 (2-Fluoro-N-[2-(2-methyl-1H-indol-3-yl)ethyl]-benzamide), whose mode of action is to prevent Arp2/3 from reaching its active conformation. Here 74 compounds structurally related to CK-666 were screened using a variety of assays. The primary screen involved EdU (5-ethynyl-2'-deoxyuridine) incorporation in untransformed MCF10A cells. The resulting nine positive hits were all blocking lamellipodial protrusions and cell migration in B16-F1 melanoma cells in secondary screens, showing that cell cycle progression can be a useful read-out of Arp2/3 activity. Selected compounds were also characterized on sea urchin embryos, where Arp2/3 inhibition yields specific phenotypes such as the lack of triradiate spicules and inhibition of archenteron elongation. Several compounds were filtered out due to their toxicity in cell cultures or on sea urchin development. Two CK-666 analogs, (N-{2-[5-(Benzyloxy)-2-methyl-1H-indol-3-yl] ethyl}-3-bromobenzamide) and (2,4-Dichloro-N-[2-(7-chloro-2-methyl-1H-indol-3-yl) ethyl]-5-[(dimethylamino) sulfonyl] benzamide), were active in all assays and significantly more efficient than CK-666. These best hits with increased potency were, however, slightly less efficient than CK-666 in the classical pyrene-actin assay. Induced-fit docking of selected compounds and their possible metabolites revealed interaction with Arp2/3 that suppresses Arp2/3 activation. The data obtained in our screening validated the applicability of original assays for Arp2/3 activity. Several previously unexplored CK-666 structural analogs were found to suppress Arp2/3 activation, and two of them were identified as Arp2/3 inhibitors with improved efficiency.
由肌动蛋白相关蛋白2和3(Arp2/3)复合物聚合形成的分支状肌动蛋白网络在力的产生和膜重塑中发挥着关键作用。这些网络对于细胞迁移尤为重要,它们驱动片状伪足的膜突出。已经鉴定出几种Arp2/3抑制性化合物。其中,使用最广泛的是CK-666(2-氟-N-[2-(2-甲基-1H-吲哚-3-基)乙基]-苯甲酰胺),其作用方式是阻止Arp2/3达到其活性构象。在此,使用多种测定方法筛选了74种与CK-666结构相关的化合物。初步筛选涉及在未转化的MCF10A细胞中掺入EdU(5-乙炔基-2'-脱氧尿苷)。在二次筛选中,得到的9个阳性命中物均能阻断B16-F1黑色素瘤细胞中的片状伪足突出和细胞迁移,表明细胞周期进程可以作为Arp2/3活性的有用读数。所选化合物还在海胆胚胎上进行了表征,在海胆胚胎中,Arp2/3抑制会产生特定的表型,如缺乏三叉棘和抑制原肠伸长。由于它们在细胞培养物中或对海胆发育有毒性,几种化合物被筛选掉。两种CK-666类似物,(N-{2-[5-(苄氧基)-2-甲基-1H-吲哚-3-基]乙基}-3-溴苯甲酰胺)和(2,4-二氯-N-[2-(7-氯-2-甲基-1H-吲哚-3-基)乙基]-5-[(二甲氨基)磺酰基]苯甲酰胺),在所有测定中均有活性,并且比CK-666效率显著更高。然而,这些效力增强的最佳命中物在经典的芘-肌动蛋白测定中比CK-666效率略低。所选化合物及其可能代谢物的诱导契合对接揭示了与Arp2/3的相互作用,该相互作用抑制Arp2/3活化。我们筛选中获得的数据验证了原始测定方法对Arp2/3活性的适用性。发现了几种以前未探索的CK-666结构类似物可抑制Arp2/3活化,其中两种被鉴定为效率提高的Arp2/3抑制剂。
