Non-Clinical Toxicology Evaluation of the Novel Non-ATP Competitive Oral PI3 Kinase Delta Inhibitor Roginolisib.

IF 1.2 4区 医学 Q4 PHARMACOLOGY & PHARMACY
International Journal of Toxicology Pub Date : 2023-12-01 Epub Date: 2023-09-04 DOI:10.1177/10915818231200419
Lars van der Veen, Michael Schmitt, Marcel A Deken, Michael Lahn
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Abstract

Roginolisib (IOA-244) is a novel, non-ATP competitive phosphoinositide-3-kinase (PI3K) delta inhibitor that regulates Akt/mTOR signaling. Roginolisib was administered once daily to rats and dogs in dose-range finding (DRF) and 4-week GLP toxicology studies. Free plasma levels of roginolisib exceeded the cellular target engagement IC90 for PI3Kδ for ≥12 hours at doses of 5 mg/kg, the IC90 for PI3Kβ for ≥2 hours at doses ≥15 mg/kg, and the IC50 for PI3Kα for ≥2 hours at dose levels ≥45 mg/kg. Toxicity in rats occurred at doses ≥100 mg/kg. In dogs, we observed dose-dependent skin and gastrointestinal toxicity and doses ≥30 mg/kg had a greater incidence of mortality. Lymphoid tissue toxicity occurred in both species. Toxicities in dogs observed at the ≥15 mg/kg dose, affecting the digestive mucosa, liver, and skin, cleared after treatment cessation. Doses ≤75 mg/kg were tolerated in rats and the no-observed-adverse-effect-level (NOAEL) in rats was 15 mg/kg. Due to mainly epithelial lesions of the skin at 5 mg/kg and necrotizing damage of the intestinal epithelia at ≥15 mg/kg, no NOAEL was determined in dogs. However, the adverse effects observed in dogs at 5 mg/kg were considered monitorable and reversible in patients with advanced malignancies. Furthermore, the PK profile subsequently proved to be a decisive factor for achieving selective PI3Kδ inhibition without the toxicities observed in dogs. As the result of the unique PK profile of roginolisib, patients were able to take daily roginolisib without dose modification and showed pharmacodynamic PI3Kδ inhibition over several months without gastrointestinal or dermatologic toxicities.

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新型非ATP竞争性口服PI3激酶德尔塔抑制剂Roginalisib的非临床毒理学评价。
Roginalisib(IOA-244)是一种新型的非ATP竞争性磷酸肌醇-3-激酶(PI3K)δ抑制剂,可调节Akt/mTOR信号传导。在剂量范围发现(DRF)和4周GLP毒理学研究中,大鼠和狗每天服用一次Roginomib。roginolisib的游离血浆水平在5 mg/kg剂量下超过PI3Kδ细胞靶点结合IC90≥12小时,在≥15 mg/kg剂量下超出PI3Kβ细胞靶点接合IC90≥2小时,在剂量水平≥45 mg/kg剂量下超过PI3Kα细胞靶点接触IC50≥2小时。大鼠在剂量≥100 mg/kg时发生毒性。在狗身上,我们观察到了剂量依赖性的皮肤和胃肠道毒性,剂量≥30 mg/kg的狗死亡率更高。两个物种都发生了淋巴组织毒性。在狗身上观察到≥15 mg/kg剂量的毒性,影响消化粘膜、肝脏和皮肤,在停止治疗后清除。大鼠耐受剂量≤75 mg/kg,大鼠无不良反应水平(NOAEL)为15 mg/kg。由于5mg/kg时主要是皮肤上皮损伤,≥15mg/kg时主要是肠上皮坏死损伤,因此在狗中未检测到NOAEL。然而,在狗身上观察到的5 mg/kg的不良反应被认为是可监测的,并且在晚期恶性肿瘤患者中是可逆的。此外,PK谱随后被证明是实现选择性PI3Kδ抑制的决定性因素,而没有在狗中观察到的毒性。由于roginolisib独特的PK图谱,患者能够在不改变剂量的情况下每天服用roginolisb,并在几个月内表现出药效学PI3Kδ抑制作用,没有胃肠道或皮肤毒性。
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来源期刊
CiteScore
3.40
自引率
4.50%
发文量
53
审稿时长
4.5 months
期刊介绍: The International Journal of Toxicology publishes timely, peer-reviewed papers on current topics important to toxicologists. Six bi-monthly issues cover a wide range of topics, including contemporary issues in toxicology, safety assessments, novel approaches to toxicological testing, mechanisms of toxicity, biomarkers, and risk assessment. The Journal also publishes invited reviews on contemporary topics, and features articles based on symposia. In addition, supplemental issues are routinely published on various special topics, including three supplements devoted to contributions from the Cosmetic Review Expert Panel.
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