Tankyrase, the fifth and sixth members of the poly(ADP-ribose) polymerase (PARP) family (PARP-5a/b), is responsible for poly(ADP-ribosyl)ation (PARylation), and was originally identified as a factor that promotes the function of telomerase, an enzyme that elongates telomeres. Subsequently, it was reported that tankyrase enhances Wnt/beta-catenin signaling by PARylation and subsequent degradation of AXIN, a negative regulator of Wnt/beta-catenin signaling, suggesting that tankyrase inhibitors may be a new treatment for colorectal cancer.
RK-582 was discovered through lead optimization from a tankyrase inhibitor that suppresses the growth of human colorectal cancer cells. It was confirmed that RK-582 selectively inhibited tankyrase among the PARP family enzymes, suppressed the growth of Wnt/beta-catenin signal-dependent human colorectal cancer cells at both the levels of cultured cells and xenograft tumors in immunodeficient mice, and accumulated AXIN to decrease beta-catenin and downregulate the target gene expression as pharmacodynamic biomarkers.
Based on these findings, RK-582 is thought to have potential as a new treatment for colorectal cancer patients. At present, however, the efficacy and safety of RK-582 in humans have not been confirmed. Thus, this clinical trial is conducted with the aim of investigating the tolerability and safety of RK-582 for patients with unresectable advanced or recurrent colorectal cancer as a first-in-human trial, in which RK-582 is administered to humans for the first time.

开始日期2025-03-01

申办/合作机构

Japanese Foundation for Cancer Research

[+1]

100 项与 RK-582 相关的临床结果

登录后查看更多信息

100 项与 RK-582 相关的转化医学

登录后查看更多信息

100 项与 RK-582 相关的专利（医药）

登录后查看更多信息

项与 RK-582 相关的文献（医药）

2024-01-31·BRITISH JOURNAL OF CANCER

APC/PIK3CA mutations and β-catenin status predict tankyrase inhibitor sensitivity of patient-derived colorectal cancer cells

Article

作者: Yamaguchi, Kensei ; Sato, Ayana ; Chen, Mingjue ; Inaba, Saori ; Oishi, Taichi ; Takamatsu, Manabu ; Nagayama, Satoshi ; Yoshida, Haruka ; Suzuki, Mai ; Seto, Yosuke ; Kawata, Naomi ; Takeuchi, Kengo ; Seimiya, Hiroyuki ; Maruyama, Kohei ; Mashima, Tetsuo ; Jang, Myung-Kyu ; Shirai, Fumiyuki ; Mizutani, Anna ; Katayama, Ryohei ; Nakamura, Ayane ; Muramatsu, Yukiko ; Morino, Shun ; Yuan, Xunmei

BACKGROUND:

Aberrant WNT/β-catenin signaling drives carcinogenesis. Tankyrases poly(ADP-ribosyl)ate and destabilize AXINs, β-catenin repressors. Tankyrase inhibitors block WNT/β-catenin signaling and colorectal cancer (CRC) growth. We previously reported that 'short' APC mutations, lacking all seven β-catenin-binding 20-amino acid repeats (20-AARs), are potential predictive biomarkers for CRC cell sensitivity to tankyrase inhibitors. Meanwhile, 'Long' APC mutations, which possess more than one 20-AAR, do not predict inhibitor-resistant cells. Thus, additional biomarkers are needed to precisely predict the inhibitor sensitivity.

METHODS:

Using 47 CRC patient-derived cells (PDCs), we examined correlations between the sensitivity to tankyrase inhibitors (G007-LK and RK-582), driver mutations, and the expressions of signaling factors. NOD.CB17-Prkdc^scid/J and BALB/c-nu/nu xenograft mice were treated with RK-582.

RESULTS:

Short APC mutant CRC cells exhibited high/intermediate sensitivities to tankyrase inhibitors in vitro and in vivo. Active β-catenin levels correlated with inhibitor sensitivity in both short and long APC mutant PDCs. PIK3CA mutations, but not KRAS/BRAF mutations, were more frequent in inhibitor-resistant PDCs. Some wild-type APC PDCs showed inhibitor sensitivity in a β-catenin-independent manner.

CONCLUSIONS:

APC/PIK3CA mutations and β-catenin predict the sensitivity of APC-mutated CRC PDCs to tankyrase inhibitors. These observations may help inform the strategy of patient selection in future clinical trials of tankyrase inhibitors.

2020-04-23·Journal of medicinal chemistry1区 · 医学

Design and Discovery of an Orally Efficacious Spiroindolinone-Based Tankyrase Inhibitor for the Treatment of Colon Cancer

1区 · 医学

Article

作者: Yashiroda, Yoko ; Niwa, Hideaki ; Mazaki, Yui ; Washizuka, Kenichi ; Okue, Masayuki ; Chikada, Tsubasa ; Yuki, Hitomi ; Muramatsu, Yukiko ; Shirai, Fumiyuki ; Kitamura, Kouichi ; Shirouzu, Mikako ; Kano, Yuko ; Nagamori, Akiko ; Umehara, Takashi ; Fukami, Takehiro ; Honma, Teruki ; Sato, Shin ; Koda, Yasuko ; Yoshida, Minoru ; Yoshida, Haruka ; Tsumura, Takeshi ; Seimiya, Hiroyuki ; Jang, Myung-Kyu ; Watanabe, Takashi ; Shitara, Eiki ; Koyama, Hiroo ; Mizutani, Anna

Tankyrases (TNKS/TNKS2) belong to the poly(ADP-ribose) polymerase family. Inhibition of their enzymatic activities attenuates the Wnt/β-catenin signaling, which plays an important role in cancer pathogenesis. We previously reported the discovery of RK-287107, a spiroindoline-based, highly selective, potent tankyrase inhibitor. Herein we describe the optimization process of RK-287107 leading to RK-582, which exhibits a markedly improved robust tumor growth inhibition in a COLO-320DM mouse xenograft model when orally administered. In addition to the dose-dependent elevation and attenuation of the levels of biomarkers AXIN2 and β-catenin, respectively, results of the TCF reporter and cell proliferation studies on COLO-320DM are discussed.

100 项与 RK-582 相关的药物交易

登录后查看更多信息

研发状态

10 条进展最快的记录,

后查看更多信息

适应症	最高研发状态	国家/地区	公司	日期
转移性结直肠癌	临床1期	日本	Japanese Foundation for Cancer Research	2025-03-01
不能切除的大肠癌	临床1期	日本	Japanese Foundation for Cancer Research	2025-03-01
结肠癌	药物发现	日本	Riken Corp.	2020-04-23