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更新于：2025-11-03

Cabozantinib (s)-Malate

苹果酸卡博替尼

更新于：2025-11-03

概要

基本信息

药物类型

小分子化药

别名

cabozantinib、Cabozantinib Malate、Cabozantinib s-malate (USAN)

+ [10]

靶点

AXL x RET x ROS1 x TYRO3 x Tie-2 x TrkB x VEGFR1 x VEGFR2 x VEGFR3 x c-Kit x c-Met

作用方式

抑制剂、拮抗剂

作用机制

AXL抑制剂(AXL受体酪氨酸激酶抑制剂)、RET抑制剂(酪氨酸蛋白激酶受体RET抑制剂)、ROS1抑制剂(原癌基因酪氨酸蛋白激酶ROS抑制剂)

治疗领域

肿瘤消化系统疾病内分泌与代谢疾病+ [11]

在研适应症

神经内分泌肿瘤高分化胰腺内分泌肿瘤胰腺外神经内分泌肿瘤+ [197]

非在研适应症

晚期胆管癌晚期乳腺癌肝外胆管癌+ [39]

原研机构

Exelixis, Inc.

在研机构

Exelixis, Inc.

Bristol Myers Squibb Co.

AstraZeneca PLC

+ [19]

非在研机构

University of Washington

EMD Serono, Inc.

江苏豪森药业集团有限公司

权益机构

Ipsen SA

Takeda Pharmaceutical Co., Ltd.

Chugai Pharmaceutical Co., Ltd.

+ [7]

最高研发阶段批准上市

首次获批日期

美国 (2012-11-29),

甲状腺髓样癌

最高研发阶段(中国)临床3期

特殊审评优先审评 (美国)、突破性疗法 (美国)、快速通道 (美国)、孤儿药 (美国)

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结构/序列

分子式C32H30FN3O10

InChIKeyHFCFMRYTXDINDK-WNQIDUERSA-N

CAS号1140909-48-3

关联

273

项与苹果酸卡博替尼相关的临床试验

NCT07187869

/ Not yet recruiting临床1期IIT

Modulation of the Bone Immune Microenvironment Following Cabozantinib Treatment of Bone Metastatic Clear Cell Renal Cell Carcinoma: Proof of Concept Study

The goal of our study is to explore how treatments affect the bone immune microenvironment and determine the best treatment options for patients with metastatic kidney cancer to the bone. This could prevent skeletal complications and improve patient outcomes.

开始日期2026-03-31

申办/合作机构

The University of Texas MD Anderson Cancer Center

[+1]

NCT06811116

/ Recruiting临床1/2期IIT

A Phase I/II Trial of Sapanisertib in Combination With Cabozantinib in β-catenin-mutated Hepatocellular Carcinoma (SAPHIRE)

This phase I/II trial studies the side effects and best dose of sapanisertib when given together with cabozantinib, and to see how well they work in treating patients with liver cancer that has spread from where it first started to other places in the body (metastatic) and contains a mutation (change) in the β-catenin gene. Sapanisertib and cabozantinib may stop the growth of tumor cells by blocking some of the enzymes needed for cell growth. Giving sapanisertib and cabozantinib together may work better than giving cabozantinib alone in treating β-catenin-mutated metastatic hepatocellular carcinoma.

开始日期2026-02-10

申办/合作机构

National Cancer Institute

NCT06502171

/ Not yet recruiting临床1期IIT

A Phase 1/1b/2 Study of Cabozantinib in Combination With Selumetinib for Plexiform Neurofibroma in Adults and Adolescents With Neurofibromatosis Type 1

Based on the clinical activity of both selumetinib and cabozantinib as monotherapies in clinical trials, the demonstrated activity of these agents in reduced doses in preclinical studies, and the non-overlapping toxicity profiles, the study will assess the tolerability and efficacy of selumetinib and cabozantinib in combination in participants with NF1 ≥16 years old with progressive and/or symptomatic PN in a phase 1/1b/2 clinical trial.
Trial Design Phase 1 This will be an open label, dose escalation phase. Dose level escalation will be determined by a rolling six design. In this design, up to 6 participants can be enrolled at a given dose level and then evaluated for dose limiting toxicity (DLT) within the DLT window. The DLT window is defined as 16 weeks in this study based on the long half-life of cabozantinib and the desire to have maximum confidence about long-term tolerability of the combination prior to proceeding to the next dose level.
Phase 1b Once the recommended phase 2 dose has been determined in phase 1, an expanded cohort of 12 participants will be enrolled in phase 1b portion of the study.
Phase 2 This will be an open label, single-arm phase using the recommended phase 2 dose.

开始日期2025-12-01

申办/合作机构

The University of Alabama at Birmingham

[+2]

100 项与苹果酸卡博替尼相关的临床结果

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100 项与苹果酸卡博替尼相关的转化医学

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100 项与苹果酸卡博替尼相关的专利（医药）

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2,486

项与苹果酸卡博替尼相关的文献（医药）

2025-12-01·Medicinal Chemistry

Reducing Cabozantinib Toxicity in Renal Cell Carcinoma Treatment through Structural Modifications

Article

作者: Lu, Yongliang ; Guo, Jiaxiang ; Yang, Yu ; Yin, Xiaotao

Background and Objectives::

Cabozantinib, a Tyrosine Kinase Inhibitor (TKI), is widely used in Renal Cell Carcinoma (RCC) therapy but often causes serious side effects such as myelosuppression, immunosuppression, and angiopathy. This study aims to identify key protein targets responsible for the therapeutic efficacy and adverse reactions of cabozantinib and to explore structural modifications to reduce toxicity while preserving efficacy.

Methods::

A non-randomized computational approach was employed, screening 400 potential protein targets using SwissTargetPrediction and ChemBL databases. Molecular docking and Structure-Activity Relationship (SAR) analysis were performed to assess interactions between cabozantinib and identified targets, focusing on structural elements contributing to toxicity.

Results::

Three primary proteins were identified as responsible for the anti-tumor effects of cabozantinib, while three others were linked to its side effects. Docking analysis revealed that the methoxyphenyl group in cabozantinib formed undesirable hydrogen bonds with toxicity-related proteins. Modulating these off-target interactions by minimizing hydrogen bonding in this region could significantly reduce adverse effects.

Conclusion::

These findings provide structural insights into cabozantinib’s dual effects and suggest optimization strategies for TKI design, offering a pathway toward safer and more effective RCC treatments.

2025-12-01·Clinical Genitourinary Cancer

Titrating Cabozantinib in Metastatic Renal Cell Carcinoma Patients Using Goldilocks Principle: A Real-World Evidence Study

Article

作者: Ahrenfeldt, Johanne ; Lyskjær, Iben ; Fristrup, Niels ; Thybo, Malou Aarønæs

INTRODUCTION:

The incidence of renal cell carcinoma (RCC) continues to rise worldwide, and this malignancy has demonstrated substantial sensitivity to both immunotherapies and targeted agents, particularly tyrosine kinase inhibitors (TKIs). Cabozantinib, a commonly utilized TKI, has shown promising efficacy across multiple clinical trials. This study aims to evaluate the real-world effectiveness of individualized cabozantinib dosing as a later-line treatment in patients with metastatic RCC (mRCC).

PATIENTS AND METHODS:

Patients with mRCC treated at the Department of Oncology, Aarhus University Hospital, Denmark, were identified to estimate the median progression free survival (mPFS) and median overall survival (mOS) from treatment initiation. Best radiological response was evaluated using RECIST 1.1. Multivariable cox regression analyses were performed, including covariates such as brain metastasis, first-line treatment, line of treatment, ECOG Performance Status, IMDC risk group, nephrectomy status, and toxicity.

RESULTS:

A total of 179 patients were included, of which 139 patients received second-line (2L) treatment, and 40 patients received third+-line (3+L) treatment. We found a mPFS of 11.2 months for 2L treatment and 11.6 months for 3+L treatment. The mOS was 15.6 months for the 2L group and 17.1 months for the 3+L group. The mPFS and mOS in the IMDC favourable risk group were 28.5 and 52.1 months, respectively. No significant differences in mPFS or mOS were observed based on prior 1L treatment or the presence of brain metastases. The mOS and mPFS found in this study are comparable to, and in some cases exceed, those reported in other real-world cohorts. Interestingly, we found treatment-related toxicity to correlate significantly with an increased survival (mOS 66.8 vs. 32.8 months, P = .016) (mPFS 14,7 vs. 8,5 months, P = .013).

CONCLUSION:

This study reinforces the existing data on effectiveness of cabozantinib as a later-line treatment for mRCC in real-world settings. We report 40 mg as the preferred landing zone. Furthermore we identify patients needing dose reductions due to toxicity as a subgroup carrying a significantly better prognosis. The results emphasize the importance of individual dosage for optimizing treatment outcomes and points out treatment-related toxicity as a surrogate marker for sufficient serum concentration of the active substance.

2025-12-01·Clinical Genitourinary Cancer

CABOSEQ 3—Comparison of Cabozantinib versus Sunitinib Following First-Line Nivolumab- Ipilimumab for Metastatic Renal Cell Carcinoma: A Target Trial Emulation Using Real-World Data from the International Metastatic Renal Cell Carcinoma Database Consortium (IMDC)

Article

作者: Labaki, Chris ; Wells, Connor ; Heng, Daniel Y C ; Szabados, Bernadett ; Yuasa, Takeshi ; Powles, Thomas ; Lemelin, Audreylie ; McKay, Rana R ; Choueiri, Toni K ; Takemura, Kosuke ; Maj, David ; Beuselinck, Benoit ; Brenner, Darren R ; McGregor, Bradley A ; Pal, Sumanta K ; Cheung, Winson Y ; Warkentin, Matthew T ; Boyne, Devon J ; Contreras, Luis Meza ; Ludwig, Lisa

BACKGROUND AND OBJECTIVE:

While the benefit of cabozantinib in metastatic renal cell carcinoma (mRCC) is well established post-tyrosine kinase inhibitor therapy, its comparative effectiveness versus sunitinib after first-line (1L) nivolumab-ipilimumab is uncertain.

METHODS:

A target trial emulation was designed using data from the IMDC to estimate the effect of second-line (2L) cabozantinib versus sunitinib within 18 months of discontinuing 1L nivolumab-ipilimumab on overall survival (OS). Patients diagnosed after January 1, 2017 were followed from initiation of 2L until death or last known contact. Inverse-probability of treatment weighting was used to adjust for hemoglobin, calcium, platelets, and neutrophils at 2L, Karnofsky performance score (KPS) at 2L, time from diagnosis to initiation of 2L, and response to 1L nivolumab-ipilimumab. Treatments were compared using adjusted Kaplan-Meier curves and adjusted hazard ratios (HR) from a Cox regression model. Missing data were addressed with multiple imputation by chained equations. E-values were used to assess the likelihood findings could be explained by residual confounding.

KEY FINDINGS AND LIMITATIONS:

A total of 120 and 121 patients who received cabozantinib or sunitinib after 1L nivolumab-ipilimumab were included. The proportion with a KPS < 80% at 2L (21% vs. 46% P = .001) and the overall response rate to first line therapy (12.7% vs. 17.9% P = .002) differed significantly between cabozantinib and sunitinib. The objective response was 27% for cabozantinib versus 20% for sunitinib with a median time to treatment failure of 8.5 (95% CI: 6.9-12.9) and 4.5 (95% CI: 3.7-5.8) months. Median OS was 21.4 (95% CI: 17.9-NA) months from initiation of cabozantinib and 10.1 (95% CI: 7.6-17.7) months for sunitinib (Adjusted HR 0.44 (95% CI: 0.22-0.86)). The E-value was 2.92, suggesting a low likelihood of findings being due to residual confounding alone.

CONCLUSIONS:

These data provide real-world evidence supporting cabozantinib as a second-line treatment option in mRCC following 1L nivolumab-ipilimumab.

746

项与苹果酸卡博替尼相关的新闻（医药）

2025-11-01

·三优生物医药

三优十周年｜肿瘤免疫2025及2018双诺奖解析

作者：汪梓昱美工：何国红罗真真排版：马超 01 引言：肿瘤免疫抗体疗法的崛起在人类对抗癌症的征途中，治疗手段正经历深刻变革——从传统的手术、放疗和化疗，逐步演进至精准的分子靶向治疗，再到以激活自身免疫力为核心的肿瘤免疫治疗。 2025年诺贝尔生理学或医学奖授予Mary Brunkow、Fred Ramsdell与Shimon Sakaguchi，以表彰他们揭示调节性T细胞（Tregs）在维持“外周免疫耐受”中的关键机制。这一发现奠定了理解免疫系统如何避免攻击自身组织的基础，推动了针对癌症的免疫疗法开发。这一奖项与2018年诺贝尔生理学或医学奖相呼应，后者授予James P. Allison和Tasuku Honjo，以表彰他们发现通过抑制免疫负调控（如PD-1和CTLA-4通路）来治疗癌症的核心原理。这两次诺奖共同突显了免疫调控在癌症治疗中的里程碑意义：2018年的工作聚焦于解除T细胞上的“抑制信号”，而2025年的发现则强调Tregs在整体免疫平衡中的作用，二者结合为现代免疫疗法提供了从基础机制到临床应用的坚实基础。 ▲ 图1. 两次诺贝尔生理学或医学奖 ▼ 表1. 两次诺贝尔生理或医学奖在关键维度的简要比较诺贝尔奖对T细胞调控的认可强调了基础免疫学在肿瘤免疫治疗（IO）中的重要性。通过理解Tregs在免疫平衡中的作用，研究者可精准设计Treg抑制剂或增强剂，推动IO从单一检查点阻断向多靶点协同演进，以解决耐药性和低应答率问题。此外，IO靶点通过调节免疫系统活性，在抗肿瘤和自体免疫疾病中发挥相反作用：激活免疫用于抗肿瘤，抑制免疫用于自体免疫病。肿瘤免疫治疗已成为全球药物研发与投资的焦点，预计市场规模将从2024年的137.42亿美元增长至2033年的2960.1亿美元。本文将探讨免疫检查点抑制剂（ICI）及新兴靶点（如LAG-3、VEGF）的机制和挑战，结合Tregs研究分析如何通过调节免疫耐受逃避免疫清除，并探讨协同治疗在提升疗效中的关键作用。 ▲ 图2. 全球肿瘤免疫治疗市场规模（十亿美元） 02 免疫检查点抑制剂：经典的“刹车松动”策略免疫系统的平衡至关重要。作为核心“战士”的T细胞，其活化需要双重信号：一是T细胞受体（TCR）识别抗原呈递细胞（APC）上的抗原-MHC复合物，二是共刺激信号（如CD28与B7结合）。与此同时，免疫系统还设有多重“刹车”机制——即免疫检查点——以防止过度活化及自身免疫损伤。免疫检查点抑制剂的作用正是解除这类刹车，从而增强T细胞对癌细胞的攻击能力。 01 CTLA-4：先驱者的挑战与新策略 CTLA-4是首个成功靶向的免疫检查点，位于T细胞表面，通过与B7分子结合抑制CD28的共刺激作用，防止T细胞过度活化。2011年，CTLA-4抑制剂伊匹木单抗（Yervoy®）获FDA批准，用于晚期黑色素瘤，开启了肿瘤免疫治疗的新纪元。然而，高毒性限制了其应用。当前的研究通过差异化策略，如局部给药和新作用机制，旨在提升疗效并降低毒性。新型HL12/HL32抗体通过避免降解、减少Treg耗竭和增强抗肿瘤作用，提出了更安全的治疗方案。此外，低剂量联用、抗体偶联药物（ADCs）和双特异性抗体等新技术，优化了CTLA-4抑制剂的治疗窗口，增强了与PD-1抑制剂联合使用时的协同抗癌效果。 ▲ 图3. CTLA4阻断抗体的效果 02 PD-1/PD-L1：时代里程碑的差异化新策略 PD-1/PD-L1抑制剂是肿瘤免疫治疗的核心，能够通过阻断肿瘤的免疫逃逸机制，恢复T细胞的抗癌功能。自2014年获批以来，这类药物取得了显著成果，但耐药性问题仍限制其广泛应用。为突破这一瓶颈，新一代PD-1/PD-L1药物正在朝着精细化方向发展，力求提高疗效并拓宽适应人群。研究者正在探索与PD-1/PD-L1不同表位结合的抗体，并通过工程化改造增强抗体依赖性细胞毒性（ADCC），实现双重抗癌效果。同时，针对PD-1的抗体设计了Fc silent结构（如IgG4/S228P），避免非期望性清除活化T细胞。此外，组合疗法与局部给药策略正在发展，结合其他免疫检查点抑制剂或靶向治疗，或通过局部高浓度给药，以进一步提升疗效并减少全身副作用。 ▲ 图4. PD-1/PD-L1阻断抗体的效果 03 打破肿瘤的免疫屏障：从诺奖发现到Tregs靶向疗法调节性T细胞（Tregs）作为“和平卫士”，在肿瘤免疫疗法中一直是关键靶点。2025年诺贝尔奖肯定了Tregs在免疫耐受中的核心作用，推动了相关研究的进展。许多肿瘤通过诱导和富集Tregs，构建免疫屏障，抑制效应T细胞的攻击。因此，如何精准调控或削弱这些肿瘤“招安”的Tregs，成为免疫治疗的重要突破口。直接靶向Tregs的抗体药物最具针对性，常通过识别Tregs特异性表面分子（如CCR8、CD25、OX40）选择性地耗竭肿瘤微环境中的免疫抑制细胞，恢复效应T细胞的活性。例如，anti-CCR8抗体DT-7012和CHS-114正在临床试验中评估其在实体瘤中的安全性与疗效。同时，CD25靶向的抗体药物偶联物（如PF-08046032）能够精确清除Tregs，减少对效应T细胞的干扰。然而，直接靶向Tregs的挑战在于平衡疗效与安全性，避免破坏外周免疫耐受，防止引发自身免疫反应。间接靶向Tregs的药物通过干扰其信号通路或功能来削弱抑制作用。经典免疫检查点抑制剂如抗CTLA-4和PD-1/PD-L1药物，能削弱Tregs功能，增强效应T细胞活性。新兴靶点如TIGIT抗体（tiragolumab）进一步增强免疫反应。虽然这些策略安全性较高，但通常需要与直接靶向疗法联合使用，以实现更显著的抗肿瘤效果。 ▲ 图5. 靶向调节性T细胞 (Treg) 的抗肿瘤疗法 04 TCE疗法：精准“搭桥”，激活肿瘤免疫 T细胞衔接器（T-cell Engager, TCE）是肿瘤免疫疗法中的一项革命性突破。其本质是一种双特异性抗体，如同一个“分子桥梁”，一端抓住免疫T细胞表面的CD3蛋白，另一端则精准识别并结合肿瘤细胞表面的特定抗原（Tumor-Associated Antigen, TAA）。通过这种物理上的强制连接，TCE能绕过传统的免疫识别步骤，直接将T细胞引导至癌细胞旁，并强效激活T细胞，使其释放细胞毒性颗粒，进而“精准引爆”，高效杀伤肿瘤。随着技术的成熟，TCE的研发正朝着高度差异化的方向发展，力求在提升疗效的同时，扩大应用范围并优化安全性。目前的差异化主要体现在以下几个方面： 1) 靶点拓展与创新：早期TCE主要靶向血液肿瘤，如CD19和BCMA，而如今研发已进入实体瘤领域，探索如GPRC5D、Claudin 18.2等新靶点，攻克实体瘤治疗难题。 2) 分子结构优化：新一代TCE采用接近天然IgG的结构，显著延长体内半衰期，支持间歇性给药，并通过“静音”改造Fc片段，减少免疫激活，降低细胞因子释放综合征（CRS）等副作用。 3) 多特异性与条件性激活：最前沿的三特异性抗体，除连接T细胞和肿瘤细胞外，还结合肿瘤微环境中的蛋白，实现更精准的靶向。同时，“前药”设计使TCE仅在肿瘤富集的特定环境下激活，扩展了治疗窗口。 4) 强弱CD3设计：选择CD3结合强度影响药物的活性与安全性。强效CD3策略快速激活T细胞，但增加CRS风险；弱效CD3策略温和激活T细胞，减少毒性，特别是在实体瘤治疗中展现出巨大潜力。总之，TCE疗法正在从单一的“搭桥”功能，发展为集靶点创新、结构优化与智能激活于一体的高度定制化治疗平台。 ▲ 图6. T细胞衔接器(TCE)通过抗原结合发挥作用 ▼ 表2. T细胞衔接器 (TCE) 上市药物一览 (截至2025年9月) 05 新兴靶点：下一代免疫疗法的希望与挑战随着肿瘤免疫治疗的进展，免疫检查点抑制剂已取得显著疗效，但单一治疗策略面临耐药性和免疫逃逸等挑战。为突破这些局限，研究者积极探索联合免疫靶点或双特异性、三特异性抗体策略，以增强免疫系统对肿瘤的清除能力。以下是几种受关注的创新方案，展示了下一代免疫疗法的希望与挑战。 01 PD-1与CTLA-4：先驱者的新策略将PD-1与CTLA-4同时阻断，标志着肿瘤免疫治疗的重要里程碑。CTLA-4在T细胞启动阶段发挥抑制作用，而PD-1在肿瘤微环境中抑制已激活的T细胞。联合使用可以在不同免疫环节解除抑制，增强抗肿瘤免疫。然而，临床上仍存在耐药性问题，且免疫相关不良事件发生率较高。为此，研究者开发了双特异性抗体，如XmAb20717（Vudalimab），该药物整合了PD-1和CTLA-4的作用机制，正进入临床试验（NCT05005728，NCT05032040），并报告了抗肿瘤活性信号。 02 PD-1与VEGF：当红炸子鸡 PD-1与VEGF联合治疗，尤其是PD-1 x VEGF双特异性抗体，近年来成为肿瘤免疫治疗的热点。VEGF通过促进肿瘤血管异常增生和免疫抑制微环境的形成，助长肿瘤生长。PD-1 x VEGF双抗不仅能抑制VEGF，正常化肿瘤血管，还能通过PD-1抑制解除T细胞的免疫抑制，增强免疫对肿瘤的杀伤力。AK112（Ivonescimab）是PD-1 + VEGF双特异性抗体，已在中国获批上市，主要用于特定类型的非小细胞肺癌（NSCLC）。该药物在多个临床试验中展示了良好的疗效和安全性，进一步验证了PD-1/VEGF双抗在多个癌种中的潜力。 ▲ 图7. Ivonescimab作用机制图 03 PD-1与LAG-3：联合的免疫解放 PD-1与LAG-3联合使用正成为免疫治疗领域的新亮点。LAG-3是一种与PD-1类似的免疫抑制性受体，通过抑制T细胞的活化，促进肿瘤免疫逃逸。联合抑制PD-1和LAG-3可以彻底解除T细胞的抑制，恢复其抗肿瘤活性。Tebotelimab（MGD013）是PD-1与LAG-3的双特异性抗体，已进入I/II期临床试验（NCT03219268），早期试验显示良好的疗效。这一组合疗法有望在临床治疗中发挥重要作用。 04 PD-1与其他靶点：突破耐药机制的双特异性抗体与三特异性抗体新一代双靶点和三靶点抗体正成为肿瘤免疫治疗的重要突破，尤其在解决耐药性方面。PD-1 x IL-2、PD-1 x TGF-β和PD-1 x 4-1BB等双抗组合，分别通过增强T细胞活性、克服基质屏障和加速T细胞增殖，显著提升抗肿瘤效果。这些组合疗法正在快速推进临床试验，展现出解决耐药性和提高治疗响应率的巨大潜力。以CS2009（三特异性抗体）为例，它同时靶向PD-1、CTLA-4和VEGF，改善了T细胞功能、抑制免疫抑制微环境并优化肿瘤血管结构，为肿瘤免疫治疗带来新的突破。 ▼ 表3. PD-1/L1部分双抗药物 05 IO靶点在自体免疫疾病中的潜力自免疾病通常伴随免疫系统的过度激活或失调，而通过靶向免疫检查点（如CTLA-4、PD-1/PD-L1、TIGIT等），可以抑制异常免疫反应，减少免疫系统对自身组织的攻击。这种策略的目的是通过调节免疫系统的活动来缓解自免疾病的症状，减轻患者的病情。然而，使用IO靶点治疗自免疾病也面临一些挑战，尤其是免疫检查点抑制剂（如PD-1/PD-L1抑制剂）可能会引起免疫相关的不良事件（irAEs），甚至加剧某些自免疾病。因此，如何平衡免疫激活和免疫抑制的效果，是该领域研究的一个关键。 ▼ 表4. 部分IO靶点自免相关管线 06 未来展望与挑战：持续进化的免疫治疗蓝图 1) 挑战：耐药性与生物标志物的探索尽管免疫治疗取得了显著进展，但仍面临两大挑战：原发性耐药（初始无应答）和获得性耐药（治疗后出现进展）。现有的生物标志物（如PD-L1表达）对疗效预测的能力有限。因此，开发更可靠、预测性更强的生物标志物，以精准筛选获益人群，是未来研究的关键。2) 联合治疗的未来：从ICI-ICI到多模式协同未来免疫治疗将不再局限于ICI之间的联合，而是趋向于多模式协同治疗，通过结合不同机制的疗法实现“1+1>2”的效果。具体策略包括： ◐ 免疫+化疗或放疗：破坏肿瘤结构、增加抗原释放并清除免疫抑制细胞，为免疫药物创造更有利的微环境。 ◐ 免疫+靶向药物：抑制肿瘤生长并改善免疫微环境，从而增强治疗效果。这种多维抗癌策略通过不同治疗方式的协同作用，提升疗效。3) 其它免疫疗法：协同作用的广阔前景免疫抗体药物是核心，而其他新兴疗法则可成为重要的协同力量： ◐ 细胞疗法：CAR-T在血液肿瘤中成效显著，并正逐步探索实体瘤应用。 ◐ 抗体偶联药物（ADC）：精准递送化疗药物或毒素至癌细胞，与免疫疗法联用具有巨大潜力。 ◐ 寡核苷酸偶联抗体（AOC）：将寡核苷酸精准递送至肿瘤微环境中的免疫细胞或癌细胞，特异性沉默免疫抑制基因，克服传统免疫疗法的耐药性。▶ 总结肿瘤免疫抗体药物已从前沿理念发展为癌症治疗的核心支柱，取得了里程碑式的进展。从CTLA-4抑制剂到PD-1/PD-L1药物，再到新靶点的涌现，每一步突破都为患者带来了新的希望。未来免疫治疗将走向多模式、协同化的“组合交响”，重点将放在克服耐药、优化生物标志物及探索更高效的联合策略，以实现个体化的精准治疗。 Sanyou 10th Anniversary: Analysis of the 2025 and 2018 Double Nobel Prizes Won in the Field of “Tumor Immunology” 01 Introduction: The Rise of Antibody-Based Cancer Immunotherapy In humanity's epic battle against cancer, treatments are undergoing a profound transformation—from the era of traditional surgery, radiotherapy, and chemotherapy to precise molecular targeted therapies, and now to antibody-based cancer immunotherapy, centered on harnessing the body's immune system as its primary defense. The 2025 Nobel Prize in Physiology or Medicine was awarded to Mary Brunkow, Fred Ramsdell, and Shimon Sakaguchi for revealing regulatory T cells' (Tregs) role in peripheral immune tolerance. This foundational work explains how the immune system avoids attacking healthy tissues, spurring cancer immunotherapy development. The insights have sparked antibody drugs to deplete these cells, with many in clinical trials.This award resonates with the 2018 Nobel to James P. Allison and Tasuku Honjo for discovering cancer treatment through inhibiting immune negative regulators, particularly the PD-1 and CTLA-4 pathways. Together, the prizes highlight immune modulation's pivotal role in oncology: 2018 emphasized removing "inhibitory signals" from T cells, while 2025 spotlights Tregs' balancing act in the immune system. Their synergy creates a solid foundation—from basic mechanisms to clinical applications—for contemporary antibody-driven immunotherapy. ▲ Figure 1. Two Nobel Prizes in Physiology or Medicine ▼ Table 1. Brief Comparison of the Two Nobel Prizes in Key Dimensions The Nobel Prize recognition of T-cell regulation highlights the importance of basic immunology in cancer immunotherapy (IO). By understanding the role of Tregs in immune balance, researchers can design targeted Treg inhibitors or enhancers, driving IO’s evolution from single checkpoint blockade to multi-target synergy to address resistance and low response rates. Additionally, IO targets modulate immune system activity, playing opposing roles in tumor immunity and autoimmune diseases—activating immunity for cancer and suppressing it for autoimmune disorders. Cancer immunotherapy has become a global focus in drug development and investment, with the market expected to grow from $13.742 billion in 2024 to $296.01 billion by 2033. This article explores the mechanisms and challenges of immune checkpoint inhibitors (ICIs) and emerging targets (like LAG-3, VEGF), analyzing how Tregs influence immune tolerance and immune evasion, and discusses the critical role of combination therapies in enhancing efficacy. ▲ Figure 2. Global Cancer Immunotherapy Market Size 02 Immune Checkpoint Inhibitors: The Classical “Release the Brakes” Strategy Immune system balance is vital. T cells, the core “fighters” of immunity, require two signals for activation: recognition of the antigen–MHC complex on antigen-presenting cells (APCs) by the T-cell receptor (TCR), and a co-stimulatory signal such as CD28 binding to B7. Meanwhile, the immune system employs multiple “brakes,” known as immune checkpoints, to prevent overactivation and autoimmune damage. Immune checkpoint inhibitors work by releasing these brakes, thereby boosting T-cell activity against cancer cells. 01 CTLA-4: Challenges and New Strategies for a Pioneer CTLA-4, the first successfully targeted immune checkpoint, inhibits CD28 co-stimulation by binding to B7 molecules on T cells to prevent overactivation. The CTLA-4 inhibitor ipilimumab (Yervoy®), approved by the FDA in 2011 for advanced melanoma, marked a new era in cancer immunotherapy but showed high toxicity. Current strategies—such as localized delivery, novel antibodies (HL12, HL32), low-dose combinations, ADCs, and bispecific antibodies—aim to enhance efficacy, reduce toxicity, and improve synergy with PD-1 inhibitors. ▲ Figure 3. Effects of CTLA-4 Blocking Antibodies 02 PD-1/PD-L1: An Era Milestone and Pathways for Differentiated Innovation PD-1/PD-L1 inhibitors are the cornerstone of cancer immunotherapy, blocking tumor immune evasion and restoring T-cell antitumor activity. Since their approval in 2014, these drugs have achieved remarkable success, though resistance remains a major challenge. To overcome this, next-generation PD-1/PD-L1 therapies are becoming more refined, aiming to enhance efficacy and expand patient benefit. Researchers are developing antibodies that bind distinct PD-1/PD-L1 epitopes and engineering them to boost antibody-dependent cellular cytotoxicity (ADCC) for dual antitumor effects. Meanwhile, Fc-silent antibody designs (such as IgG4/S228P) help avoid unwanted depletion of activated T cells. Combination approaches and localized delivery strategies—pairing PD-1/PD-L1 inhibitors with other checkpoint or targeted therapies, or applying them directly at tumor sites—are also advancing to improve outcomes while minimizing systemic side effects. ▲ Figure 4. Effects of PD-1/PD-L1 Blocking Antibodies 03 Overcoming Tumor Immune Suppression: From Nobel Discoveries to Treg-Targeted Therapies Regulatory T cells (Tregs), known as the "guardians" are key targets in cancer immunotherapy. The 2025 Nobel Prize highlighted their central role in immune tolerance, accelerating related research. Many tumors induce and enrich Tregs to build immune barriers that suppress effector T cell attacks. Thus, precisely modulating or weakening these tumor "recruited" Tregs has become a critical breakthrough for immunotherapy. Antibody drugs that directly target Tregs are among the most focused strategies. They work by recognizing surface molecules unique to Tregs — such as CCR8, CD25, or OX40 — and selectively clearing out the suppressive cells within tumors. For instance, anti-CCR8 antibodies like DT-7012 and CHS-114 are now in clinical trials for solid cancers, while CD25-targeting antibody–drug conjugates (e.g., PF-08046032) precisely remove Tregs without overly disturbing other immune cells. The main challenge is striking the right balance: boosting anti-tumor immunity without tipping the system into autoimmunity. Indirect strategies, including anti-CTLA-4, anti-PD-1/PD-L1, and TIGIT antibodies (like tiragolumab), suppress Treg function while enhancing effector T-cell responses. These approaches are generally safer but often work best in combination with direct Treg-targeting therapies for stronger, more durable antitumor effects. ▲ Figure 5. Antitumor Therapies Targeting Regulatory T Cells (Tregs) 04 TCE Therapy: Precision "Bridging" to Activate Tumor Immunity T-cell Engagers (TCEs) are a groundbreaking innovation in tumor immunotherapy. These bispecific antibodies precisely connect T cells with tumor cells, activating the T cells to directly kill tumors. One end of the TCE binds to CD3 on T cells, while the other attaches to tumor-associated antigens (TAAs) on cancer cells, bypassing traditional immune recognition to rapidly trigger T-cell activation and release cytotoxic particles for efficient tumor destruction. As the technology advances, TCEs are evolving in the following key areas: 1) Target Expansion and Innovation: Early TCEs targeted blood cancers (CD19, BCMA), now extending to solid tumors with novel targets like GPRC5D and Claudin 18.2. 2) Molecular Structure Optimization: Next-gen TCEs mimic natural IgG for longer half-life, support intermittent dosing, and reduce side effects (e.g., CRS) with Fc modifications. 3) Multispecific and Conditional Activation: Trispecific antibodies improve targeting by binding both tumor cells and the tumor microenvironment, while "prodrug" designs activate TCEs only in tumor-rich areas. 4) Strong vs. Weak CD3 Binding: Strong CD3 engagement rapidly activates T cells but increases CRS risk; weak engagement reduces toxicity, particularly in solid tumor treatments.In summary, TCE therapy is evolving from a simple “bridging” tool into a highly customized treatment platform, integrating target innovation, structural optimization, and intelligent activation. ▲ Figure 6. Mechanism of Action of T-cell Engagers (TCEs) via Antigen Binding ▼ Table 2. Approved T-cell Engager (TCE) Therapies (as of October 2025) 05 Emerging Targets: Opportunities and Challenges for Next-Generation Immunotherapies With advances in cancer immunotherapy, checkpoint inhibitors have achieved great success but still face resistance and immune escape. To overcome these challenges, researchers are exploring combination therapies and multi-specific antibodies to enhance tumor clearance—showcasing both the promise and hurdles of next-generation immunotherapies. 01 PD-1 and CTLA-4: New Strategies for Pioneers Simultaneous blockade of PD-1 and CTLA-4 marked a major milestone in cancer immunotherapy. CTLA-4 suppresses T-cell activation during the priming phase, while PD-1 inhibits activated T cells within the tumor microenvironment. Their combination releases immune inhibition at multiple stages, enhancing anti-tumor immunity. However, resistance and high rates of immune-related adverse events remain challenges. To address this, bispecific antibodies such as XmAb20717 (Vudalimab) have been developed, integrating PD-1 and CTLA-4 mechanisms. The drug has entered clinical trials (NCT05005728, NCT05032040) and shown preliminary anti-tumor activity. 02 PD-1 × VEGF: The Hot Favorite Right Now VEGF promotes tumor angiogenesis and an immunosuppressive microenvironment. PD-1 × VEGF bispecifics inhibit VEGF to normalize tumor vasculature while restoring T-cell activity via PD-1 blockade, thereby enhancing tumor killing. AK112 (Ivonescimab), a PD-1/VEGF bispecific antibody, has been approved in China for specific non–small cell lung cancer (NSCLC) subtypes, demonstrating promising efficacy and safety across multiple clinical studies. ▲ Figure 7. Mechanism of Ivonescimab 03 PD-1 and LAG-3: Combined Checkpoint Blockade PD-1 and LAG-3 combination therapy is emerging as a new focus in immuno-oncology. LAG-3, an inhibitory receptor similar to PD-1, suppresses T-cell activation and promotes tumor immune evasion. Dual blockade of PD-1 and LAG-3 can fully restore T-cell antitumor activity. Tebotelimab (MGD013), a PD-1/LAG-3 bispecific antibody, is in phase I/II trials (NCT03219268) with encouraging early results, showing promise for future clinical application. 04 PD-1 and Other Targets: Bispecific and Trispecific Antibodies to Overcome Resistance Mechanisms Next-generation dual- and tri-specific antibodies are driving breakthroughs in cancer immunotherapy, especially against resistance. Combinations like PD-1 × IL-2, PD-1 × TGF-β, and PD-1 × 4-1BB enhance T-cell activity, overcome stromal barriers, and boost proliferation, markedly improving antitumor efficacy. Tri-specific CS2009, targeting PD-1, CTLA-4, and VEGF, enhances T-cell function, modulates the tumor microenvironment, and normalizes vasculature, showing strong clinical potential. ▼ Table 3. Selected PD-1/L1 Bispecific Antibodies 05 The Potential of IO Targets in Autoimmune Diseases Autoimmune diseases involve excessive or misdirected immune activity. Targeting immune checkpoints such as CTLA-4, PD-1/PD-L1, and TIGIT can help suppress abnormal responses and reduce self-tissue attack, easing symptoms. However, using IO targets also carries risks—checkpoint inhibitors may trigger immune-related side effects or worsen some conditions. Balancing immune activation and suppression remains a key challenge. ▼ Table 4. Pipeline of Selected IO Targeted Drugs 06 Future Outlook and Challenges: The Evolving Blueprint of Immunotherapy 1) Challenges: Resistance and Biomarker Exploration Despite remarkable progress in immunotherapy, two major challenges remain: primary resistance (lack of initial response) and acquired resistance (disease progression after treatment). Current biomarkers, such as PD-L1 expression, have limited predictive power. Therefore, developing more reliable and predictive biomarkers to accurately identify patients who will benefit is a key focus for future research. 2) The Future of Combination Therapy: From ICI-ICI to Multi-Modal Synergy Future immunotherapy will extend beyond combinations of immune checkpoint inhibitors (ICIs) toward multi-modal synergistic approaches that achieve a “1+1>2” effect by integrating therapies with different mechanisms. Key strategies include: ◐ Immunotherapy + Chemotherapy or Radiotherapy: Disrupting tumor structure, increasing antigen release, and eliminating immunosuppressive cells to create a more favorable microenvironment for immune agents. ◐ Immunotherapy + Targeted Therapy: Inhibiting tumor growth while improving the immune microenvironment to enhance overall efficacy.This multi-dimensional approach leverages the synergy of diverse treatments to achieve stronger and more durable anti-cancer effects. 3) Other Immunotherapies: New Frontiers in Synergistic Potential While immune antibody drugs remain the cornerstone, emerging therapies are becoming powerful allies： ◐ Cell therapies such as CAR-T have achieved remarkable success in hematologic cancers and are being explored for solid tumors. ◐ Antibody-drug conjugates (ADCs) precisely deliver chemotherapeutic agents or toxins to cancer cells, offering great potential when combined with immunotherapy. ◐ Antibody-oligonucleotide conjugates (AOCs) enable targeted delivery of oligonucleotides to immune or cancer cells within the tumor microenvironment, selectively silencing immunosuppressive genes and helping to overcome resistance to traditional immunotherapies. ▶ Summary Cancer immunotherapy antibodies have evolved from groundbreaking concepts to become a cornerstone in cancer treatment, achieving milestone progress. From CTLA-4 inhibitors to PD-1/PD-L1 drugs, and the emergence of new targets, each breakthrough brings new hope for patients. The future of immunotherapy will focus on multi-modal, synergistic "combination symphonies," with an emphasis on overcoming resistance, optimizing biomarkers, and exploring more efficient combination strategies to achieve personalized precision treatment. ▶ Reference 1. Hsu CY, Pallathadka H, Jasim SA, et al. Innovations in cancer immunotherapy: A comprehensive overview of recent breakthroughs and future directions. Crit Rev Oncol Hematol. 2025;206:104588. doi:10.1016/j.critrevonc.2024.104588 2. Liu J, Chen Z, Li Y, Zhao W, Wu J, Zhang Z. PD-1/PD-L1 Checkpoint Inhibitors in Tumor Immunotherapy. Front Pharmacol. 2021;12:731798. Published 2021 Sep 1. doi:10.3389/fphar.2021.731798 3. Nova One Advisor. Cancer immunotherapy market size, share & trends analysis report, by product, by application, by distribution, by end use, by region: Global industry analysis, size, share, growth, trends, regional outlook, and forecast 2024-2033. Nova One Advisor website. Published April 2025. 4. Grand View Research. Asia Pacific cancer immunotherapy market outlook, 2024 - 2030. Grand View Research. Published 2024. Accessed September 21, 2025. 5. Yin Q, Wu L, Han L, et al. Immune-related adverse events of immune checkpoint inhibitors: a review. Front Immunol. 2023;14:1167975. Published 2023 May 25. doi:10.3389/fimmu.2023.1167975 6. Babamohamadi M, Mohammadi N, Faryadi E, et al. Anti-CTLA-4 nanobody as a promising approach in cancer immunotherapy. Cell Death Dis. 2024;15(1):17. Published 2024 Jan 8. doi:10.1038/s41419-023-06391-x 7. Waldman AD, Fritz JM, Lenardo MJ. A guide to cancer immunotherapy: from T cell basic science to clinical practice. Nat Rev Immunol. 2020;20(11):651-668. doi:10.1038/s41577-020-0306-5 8. Pasqualotto E, Moraes FCA, Chavez MP, et al. PD-1/PD-L1 Inhibitors plus Chemotherapy Versus Chemotherapy Alone for Resectable Non-Small Cell Lung Cancer: A Systematic Review and Meta-Analysis of Randomized Controlled Trials. Cancers (Basel). 2023;15(21):5143. Published 2023 Oct 26. doi:10.3390/cancers15215143 9. Parvez A, Choudhary F, Mudgal P, et al. PD-1 and PD-L1: architects of immune symphony and immunotherapy breakthroughs in cancer treatment. Front Immunol. 2023;14:1296341. Published 2023 Dec 1. doi:10.3389/fimmu.2023.1296341 10. Cheng W, Kang K, Zhao A, Wu Y. Dual blockade immunotherapy targeting PD-1/PD-L1 and CTLA-4 in lung cancer. J Hematol Oncol. 2024;17(1):54. Published 2024 Jul 27. doi:10.1186/s13045-024-01581-2 11. Esfandiari A, et al. T-cell engaging bispecific antibodies in cancer therapy: limitations, challenges, and opportunities. Mol Ther. 2024. 12. Labrijn AF, et al. T cell-engaging bispecific antibodies in cancer immunotherapy. Nat Rev Clin Oncol. 2022. 13. Mazor Y, et al. Diversifying the T cell-engaging bispecific antibody platform. Nat Rev Drug Discov. 2021. 14. Cech P, Skórka K, Dziki L, Giannopoulos K. T-Cell Engagers-The Structure and Functional Principle and Application in Hematological Malignancies. Cancers (Basel). 2024;16(8):1580. Published 2024 Apr 20. doi:10.3390/cancers16081580 15. Cheng B, Lv J, Xiao Y, Song C, Chen J, Shao C. Small molecule inhibitors targeting PD-L1, CTLA4, VISTA, TIM-3, and LAG3 for cancer immunotherapy (2020-2024). Eur J Med Chem. 2025;283:117141. doi:10.1016/j.ejmech.2024.117141 16. Luke JJ, Patel MR, Blumenschein GR, et al. The PD-1- and LAG-3-targeting bispecific molecule tebotelimab in solid tumors and hematologic cancers: a phase 1 trial. Nat Med. 2023;29(11):2814-2824. doi:10.1038/s41591-023-02593-0 17. Chao MP, Takimoto CH, Feng DD, et al. Therapeutic Targeting of the Macrophage Immune Checkpoint CD47 in Myeloid Malignancies. Front Oncol. 2020;9:1380. Published 2020 Jan 22. doi:10.3389/fonc.2019.01380 18. Gomes de Morais AL, Cerdá S, de Miguel M. New Checkpoint Inhibitors on the Road: Targeting TIM-3 in Solid Tumors. Curr Oncol Rep. 2022;24(5):651-658. doi:10.1007/s11912-022-01218-y 19. Hodi FS, Chapman PB, Sznol M, et al. Safety and efficacy of combination nivolumab plus ipilimumab in patients with advanced melanoma: results from a North American expanded access program (CheckMate 218). Melanoma Res. 2021;31(1):67-75. doi:10.1097/CMR.0000000000000708 20. Xu J, Shen J, Gu S, et al. Camrelizumab in Combination with Apatinib in Patients with Advanced Hepatocellular Carcinoma (RESCUE): A Nonrandomized, Open-label, Phase II Trial.Clin Cancer Res. 2021;27(4):1003-1011. doi:10.1158/1078-0432.CCR-20-2571 21. Fitzgerald KN, Lee CH, Voss MH, et al. Cabozantinib Plus Nivolumab in Patients with Non-Clear Cell Renal Cell Carcinoma: Updated Results from a Phase 2 Trial. Eur Urol. 2024;86(2):90-94. doi:10.1016/j.eururo.2024.04.025 1 推荐阅读三优十周年｜TCE药物-重塑免疫治疗版图的新力量三优十周年｜神经系统疾病治疗进展三优十周年｜AI-STAL 智能超万亿分子库发展历程三优十周年｜打造全球顶尖的原创新药创新工场三优十周年｜抗体治疗50年风雨江湖三优十周年｜针对宠物疾病的单克隆抗体药物三优十周年｜CAR-T细胞治疗现状挑战与未来三优十周年｜服务篇-体外药效筛选解决方案三优十周年｜AI-STAL篇-Anticalin靶向蛋白库三优十周年｜靶点篇-自身免疫疾病靶点介绍创新前沿｜三优生物类器官产学研联盟启航中和抗体“硬核出击”，斩断CHIKV病毒感染链三优十周年｜服务篇-靶点至PCC药物研发三优十周年｜靶点篇-六大恶性肿瘤靶点介绍创新前沿｜2025ADC热门靶点与技术创新启示关于三优生物三优生物是一家以“让天下没有难做的创新生物药”为使命，以超万亿分子库和智能科技驱动的生物医药高科技企业。公司致力于打造全球顶尖的原创新药创新工场。公司以智能超万亿分子库（AI-STAL）为核心；以干湿结合、国际领先的创新生物药智能化及一体化研发平台为依托；以多样化的业务模式推动全球创新药物的研发及产业化。公司总部位于中国上海，在亚洲、北美洲、欧洲等多地建立了业务中心，形成了全球化的业务网络，现有投产及布局的研发及GMP场地20000多平方米。公司已与全球2000多家药企、生技公司等建立了良好的合作关系，已赋能1200多个新药研发项目；已完成50多个合作研发项目，其中10多个协同研发项目已推至IND及临床研发阶段。公司已申请130多项发明专利，其中30多项发明专利已获得授权，并获得了国家级高新技术企业、上海市专精特新、ISO9001、ISO27001等10余项资质及体系认证。 1 推荐阅读三优十周年｜TCE药物-重塑免疫治疗版图的新力量三优十周年｜神经系统疾病治疗进展三优十周年｜AI-STAL 智能超万亿分子库发展历程三优十周年｜打造全球顶尖的原创新药创新工场三优十周年｜抗体治疗50年风雨江湖三优十周年｜针对宠物疾病的单克隆抗体药物三优十周年｜CAR-T细胞治疗现状挑战与未来三优十周年｜服务篇-体外药效筛选解决方案三优十周年｜AI-STAL篇-Anticalin靶向蛋白库三优十周年｜靶点篇-自身免疫疾病靶点介绍创新前沿｜三优生物类器官产学研联盟启航中和抗体“硬核出击”，斩断CHIKV病毒感染链三优十周年｜服务篇-靶点至PCC药物研发三优十周年｜靶点篇-六大恶性肿瘤靶点介绍创新前沿｜2025ADC热门靶点与技术创新启示关于三优生物三优生物是一家以“让天下没有难做的创新生物药”为使命，以超万亿分子库和智能科技驱动的生物医药高科技企业。公司致力于打造全球顶尖的原创新药创新工场。公司以智能超万亿分子库（AI-STAL）为核心；以干湿结合、国际领先的创新生物药智能化及一体化研发平台为依托；以多样化的业务模式推动全球创新药物的研发及产业化。公司总部位于中国上海，在亚洲、北美洲、欧洲等多地建立了业务中心，形成了全球化的业务网络，现有投产及布局的研发及GMP场地20000多平方米。公司已与全球2000多家药企、生技公司等建立了良好的合作关系，已赋能1200多个新药研发项目；已完成50多个合作研发项目，其中10多个协同研发项目已推至IND及临床研发阶段。公司已申请130多项发明专利，其中30多项发明专利已获得授权，并获得了国家级高新技术企业、上海市专精特新、ISO9001、ISO27001等10余项资质及体系认证。

免疫疗法细胞疗法临床研究

2025-10-31

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ESMO 2025中国之声：FRUSICA-2研究发布，呋喹替尼联合信迪利单抗为晚期肾癌二线治疗带来新希望

*仅供医学专业人士阅读参考FRUSICA-2研究精彩亮相ESMO2025肾细胞癌（RCC）是常见的泌尿系统恶性，晚期患者预后普遍较差。近年来，靶向、免疫治疗的应用极大地改善了患者的一线治疗获益，然而一旦疾病发生进展，后续的治疗选择有限。尤其在中国，晚期RCC的二线治疗目前仍以酪氨酸激酶抑制剂（TKI）或哺乳动物雷帕霉素靶蛋白（mTOR）抑制剂单药治疗为主，存在未满足临床需求。FRUSICA-2 Ⅲ期研究[1]旨在评估呋喹替尼联合信迪利单抗对比现有标准疗法，用于晚期RCC二线治疗的疗效与安全性。近日，FRUSICA-2 Ⅲ期研究在2025年欧洲肿瘤内科学会（ESMO）大会上以口头报告形式隆重发布（摘要号2592MO），成为本次会议的一大亮点。医学界肿瘤频道特邀中国医学科学院肿瘤医院邢念增教授就该研究的背景、设计、主要结果及其对临床实践产生的影响进行专业解读，帮助临床医生更好地理解这一治疗方案，为未来临床实践提供循证依据，进一步改善晚期RCC患者的生存预后。专家简介邢念增教授国家中心/中国医学科学院肿瘤医院副院长泌尿外科主任医师、博士研究生及博士后导师泌尿系统肿瘤细胞和基因治疗北京市重点实验室主任全国人大代表中央保健委员会会诊专家首届“国家杰出医师”国家“有突出贡献中青年专家”，“百千万人才工程”国家级人才，国家卫生健康突出贡献中青年专家。享受国务院特殊津贴。国之名医。吴杨医学药学奖获得者。担任中国医师协会泌尿外科医师分会会长、北京医学会泌尿外科分会候任主任委员、Endourological Society 委员，UroPrecison杂志主编、 J of Urology 编委、《中华医学杂志》副总编、《中华泌尿外科杂志》副总编、《中华腔镜泌尿外科杂志》副总编、《临床泌尿外科杂志》副总编国家重点研发计划首席科学家。国内外发表学术论文400余篇。主编专著23部。晚期肾癌二线治疗困局：靶向耐药与肿瘤异质性下的生存挑战邢念增教授指出，肾癌已成为全球公共卫生领域的一个重大挑战。据统计，2022年全球新发病例数超过43.4万例，每年因肾癌导致的死亡人数约为15.6万[2]。在中国，肾癌每年约造成2.4万人死亡，占全国所有癌症死亡病例的0.9%[3]。RCC占据了肾脏恶性肿瘤的90%，且转移性RCC患者的预后不佳，5年生存率仅为12%[4]。在晚期RCC患者中，传统放、化疗的疗效并不理想，患者生存预后不佳。尽管靶向治疗和免疫治疗的引入显著提高了RCC一线治疗的疗效，客观缓解率（ORR）可达到42%-71.6%，无进展生存期（PFS）延长至11.6-23.9个月[5-11]，但在二线治疗中，仍以TKI、mTOR抑制剂单药治疗为主，其ORR仅为1.0%至23%，中位PFS仅为4.0至8.3个月[11-14]，疗效有限，难以满足患者的治疗需求。更为棘手的是，接受二线治疗的患者大多数已经历过一线TKI治疗的失败，这些患者的肿瘤细胞通常表现出复杂的耐药机制和显著的异质性，亟需更有效的治疗策略以改善这类患者的预后。机制协同，疗效显著：呋喹替尼联合信迪利单抗创晚期RCC二线治疗新纪录邢念增教授表示，FRUSICA-2是一项II/III期临床研究，其中本次ESMO会议公布的数据来自其III期研究，这是一个随机、开放标签、阳性对照试验，旨在评估呋喹替尼联合信迪利单抗对比现有标准疗法（阿昔替尼或依维莫司）在局部晚期或转移性RCC患者二线治疗中的疗效与安全性。研究纳入既往接受过一线VEGFR-TKI治疗失败或不耐受的晚期RCC患者（n=234），按1:1随机分配至实验组和对照组。主要研究终点为盲态独立阅片委员会（BIRC）评估的PFS，次要终点为研究者评估的PFS、ORR、DCR等。该研究在此次ESMO大会首次公布的研究数据显示呋喹替尼联合信迪利单抗用于RCC的二线治疗，疗效优异，安全性良好，引发广泛关注。经BIRC评估，联合组的中位PFS长达22.2个月，而对照组仅为6.9个月[HR=0.373(95% CI: 0.256, 0.544);p< 0.0001]，使疾病进展或死亡风险显著降低了63%。在晚期RCC治疗领域，能够在中位PFS上突破20个月的治疗方案，此前仅见于一线治疗。呋喹替尼与信迪利单抗联合方案在二线治疗中取得如此卓越的疗效，展现出接近一线标准治疗的巨大潜力，有望为晚期RCC患者的二线治疗提供更具希望的新选择。联合组的ORR高达60.5%，是对照组（24.3%）的2.5倍（OR=4.622，p<0.0001）。这一数据表明，联合治疗方案能够更有效地抑制肿瘤生长，使更多患者获得病情缓解的机会，为患者带来了更多的生存希望。联合组的中位DoR达到了23.7个月，相较于对照组单药治疗的11.3个月，延长了12.4个月。说明呋喹替尼联合信迪利单抗这一靶免治疗方案一旦起效，就能够为患者带来更为持久的临床获益。尽管采用了联合治疗方案，但其安全性整体可控，并未出现新的非预期安全性信号。这意味着患者在接受治疗的过程中，能够在有效控制病情的同时，不良反应可管可控，保障了治疗的耐受性和依从性，为长期治疗奠定了基础。邢念增教授在深入分析该研究取得成功的关键因素时指出，本研究在lb期数据表现出色，ORR达到60%，中位PFS达15.9个月。这些优异的前期数据为Ⅲ期试验的设计提供了坚实的科学依据，保障了研究的科学性和可靠性。在该研究的研究设计中，对照组选用了当前二线标准治疗（阿昔替尼或依维莫司），具有高度的临床可比性，为后续的临床决策提供了强有力的证据支持。药物机制层面，呋喹替尼通过抑制VEGFR信号通路，有效阻断肿瘤血管生成，并可改善肿瘤免疫微环境。该药物靶点精准，脱靶毒性小，疗效和安全性已在多种已获批的实体瘤适应症中得到验证。与信迪利单抗联合使用，能够协同增效，实现抗血管生成与免疫治疗的双重机制互补，显著提升抗肿瘤效果，展现出广阔的临床应用前景。这种机制上的协同效应，是联合治疗取得成功的重要基础。此外，本研究采用亚组分析，纳入了程序性死亡配体-1（PD-L1）表达水平等因素。结果显示，呋喹替尼联合信迪利单抗的疗效与PD-L1表达情况无关，即无论PD-L1表达水平如何，该联合治疗方案均显示出优于当前二线标准治疗的疗效。说明该联合方案具备广泛的适用人群，有望让更多患者从中获益。邢念增教授表示，FRUSICA-2研究的成果，将对临床实践产生深远而积极的影响。其突出的疗效数据有望促进呋喹替尼联合信迪利单抗成为晚期RCC二线治疗的标准方案。这一研究进展有望为临床医生及患者提供更科学、有效的治疗选择，进一步改善患者的预后。晚期RCC二线治疗：多因素考量，精准制定方案邢念增教授强调，晚期RCC患者在接受一线治疗发生耐药后，如何选择合适的二线治疗方案一直是临床关注的重点问题。CSCO肾癌专家委员会达成共识，在任何情况下，评估患者是否符合临床试验入组条件应作为二线治疗决策的首要步骤。若患者无法进入临床试验，则需系统回顾其一线治疗情况，包括所用方案、治疗持续时间、最佳缓解时间以及是否出现特定不良反应等，这些信息是制定二线治疗方案的重要依据。了解一线治疗的药物作用机制以及耐药机制是选择二线药物的关键，有助于筛选出作用机制不同或可逆转耐药的药物。以FRUSICA-2研究为例，在该研究开展之时，中国的晚期RCC一线治疗仍以靶向药物单药治疗为主，免疫联合治疗在一线中的应用直至2024年才获批准。而且以TKI类药物为代表的一线靶向治疗方案，因其高级别的循证医学证据支持、口服给药的便捷性以及便于长期管理等特点，目前仍是临床广泛应用的优选方案。FRUSICA-2研究通过联合应用不同机制的药物，有效克服TKI耐药，显著提高了二线治疗的疗效，延长患者的生存期。在选择二线治疗方案时，依据权威指南和高级别临床证据（如Ⅲ期随机对照试验）是重要原则。例如FRUSICA-2Ⅲ期研究的阳性结果，为呋喹替尼联合信迪利单抗在晚期RCC二线治疗中的应用提供了坚实证据，使该联合方案有望成为新的临床标准选择之一。安全性及耐受性同样是制定二线治疗方案时不可忽视的重要因素，直接影响治疗完成度和患者生活质量。应全面评估不同治疗方案常见及罕见不良反应，并结合患者的具体身体状况和耐受能力，选择更为匹配、安全性更优的方案。同时，加强不良反应的预防与全程管理，保障患者治疗顺利和生活质量。药物可及性与经济因素也是影响治疗方案选择的实际问题，医生需要考虑治疗方案是否已在国内获批相应适应症、是否纳入医保报销范围，并结合患者的经济承受能力，制定切实可行的个体化治疗策略。总之，为一线治疗耐药后的晚期RCC患者制定二线方案是一个需整合多方面因素的临床决策过程。只有充分考虑上述各个关键因素，将临床试验机会、前线治疗方案、耐药机制分析、证据指南推荐、安全耐受评估以及药物经济药物经济学因素系统结合，才能为患者提供真正精准、个性化的治疗选择，最终提升治疗效果、改善生活质量和生存预后。未来，随着研究的不断深入和新型药物的不断涌现，晚期RCC的二线治疗格局有望迎来更多突破，为患者带来新的希望。总结与展望FRUSICA-2的III期研究结果在ESMO 2025大会上重磅发布，为晚期RCC二线治疗带来了重要突破。该研究采用呋喹替尼联合信迪利单抗方案，在PFS、ORR及DoR等关键指标上显著优于标准治疗组，且安全性可控，展现出接近一线治疗的疗效潜力。这一成果不仅为临床提供了更优的治疗选择，也有望推动国内外指南更新，改变晚期RCC二线治疗格局。展望未来，随着对肿瘤异质性和耐药机制研究的不断深入，以及生物标志物指导下的精准治疗发展，晚期RCC二线将朝着更加个体化、高效化的方向迈进。同时，随着药物可及性与经济性的持续优化，更多患者将能够从创新治疗方案中获益。FRUSICA-2研究的成功，是中国创新药研发实力的彰显，也为全球肾癌治疗领域贡献了中国智慧。期待该研究进一步推动国际多中心合作，为更多患者带来希望。参考文献：[1].Dingwei Y , Zhisong H , Yuanyuan Q,et al.Fruquintinib (FRUQ) plus sintilimab (SIN) versus axitinib (AXI) or everolimus (EVE) monotherapy as 2L treatment in pts with locally advanced or metastatic renal cell carcinoma (RCC).2025 ESMO 2592MO.[2].Ferlay J, Ervik M, Lam F, Laversanne M, Colombet M, Mery L, Piñeros M, Znaor A, Soerjomataram I, Bray F (2024).[3].Global Cancer Observatory: Cancer Today. Lyon, France: International Agency for Research on Cancer. Available from: https://gco.iarc.who.int/today, accessed [DD Month YYYY].[4].Zheng RS, Chen R, Han BF, et al. [Cancer incidence and mortality in China, 2022]. Zhonghua Zhong Liu Za Zhi. 2024 Mar 23;46(3):221-231. Chinese. doi: 10.3760/cma.j.cn112152-20240119-00035. PMID: 38468501.[5].Motzer RJ, Tannir NM, McDermott DF,et al. Nivolumab plus Ipilimumab versus Sunitinib in Advanced Renal-Cell Carcinoma. N Engl J Med. 2018 Apr 5;378(14):1277-1290.[6].Motzer RJ, Penkov K, Haanen J,et al. Avelumab plus Axitinib versus Sunitinib for Advanced Renal-Cell Carcinoma. N Engl J Med. 2019 Mar 21;380(12):1103-1115.[7].Rini BI, Plimack ER, Stus V,et al. Pembrolizumab plus Axitinib versus Sunitinib for Advanced Renal-Cell Carcinoma. N Engl J Med. 2019 Mar 21;380(12):1116-1127.[8].Choueiri TK, Powles T, Burotto M, et al. Nivolumab plus Cabozantinib versus Sunitinib for Advanced Renal-Cell Carcinoma. N Engl J Med. 2021 Mar 4;384(9):829-841.[9].Lee CH, Shah AY, Rasco D,et al. Lenvatinib plus pembrolizumab in patients with either treatment-naive or previously treated metastatic renal cell carcinoma (Study 111/KEYNOTE-146): a phase 1b/2 study. Lancet Oncol. 2021 Jul;22(7):946-958.[10].Yan XQ, Ye MJ, Zou Q,et al. Toripalimab plus axitinib versus sunitinib as first-line treatment for advanced renal cell carcinoma: RENOTORCH, a randomized, open-label, phase III study. Ann Oncol. 2024 Feb;35(2):190-199.[11].Xinan S,et al.First-line benmelstobart plus anlotinib versus sunitinib in advanced renal cell carcinoma: Subgroup analysis from the phase 3 ETER100 trial.2024 ESMO, Abstract LBA76.[12].Motzer RJ, Escudier B, Oudard S,et al. Efficacy of everolimus in advanced renal cell carcinoma: a double-blind, randomised, placebo-controlled phase III trial. Lancet. 2008 Aug 9;372(9637):449-56.[13].Motzer RJ, Escudier B, Tomczak P,et al. Axitinib versus sorafenib as second-line treatment for advanced renal cell carcinoma: overall survival analysis and updated results from a randomised phase 3 trial. Lancet Oncol. 2013 May;14(6):552-62.[14].Choueiri TK, Escudier B, Powles T,et al. Cabozantinib versus everolimus in advanced renal cell carcinoma (METEOR): final results from a randomised, open-label, phase 3 trial. Lancet Oncol. 2016 Jul;17(7):917-927.本资料由和黄医药提供支持本资料旨在促进医药信息的沟通和交流，而非广告宣传。本资料内容不能以任何方式取代专业的医疗指导，也不应被视为诊疗建议。若您想了解更多有关疾病知识的信息，请咨询医疗卫生专业人士。*此文仅用于向医疗卫生专业人士提供科学信息，不代表平台立场。

临床3期免疫疗法放射疗法

2025-10-31

·优恩蒙国际

卡博替尼的功效作用，老挝卡博替尼仿制药，靶向药中的万金油

卡博替尼(Cabozantinib)是由美国Exelixis生物制药公司研发的一款广谱、多靶点抗肿瘤药物。一般的抗肿瘤药物的靶点有1-3个，而卡博替尼靶点多达9个以上，因此也被称为靶向药中的“万金油”。卡博替尼(Cabozantinib),俗称XL184,是一个多靶点的广谱抗癌药，卡博替尼被称之为靶向药中的“混世魔王”。目前研究发现卡博替尼能作用的靶点：MET、VEGFR1/2/3、ROS1、RET、AXL、NTRK、KIT等至少9个作用机制卡博替尼是一种酪氨酸激酶抑制剂，它能抑制多种受体酪氨酸激酶的活性，包括血管内皮生长因子受体（VEGFR）、肝细胞生长因子受体（MET）和微血管相关蛋白受体（RET）等。这些受体在癌症生长、转移和血管生成中起重要作用，卡博替尼的作用可阻断它们的信号传导，从而抑制肿瘤细胞的生长和扩散适应症和用途：卡博替尼是肾癌患者的一线治疗药物；在非小细胞肺癌患者中，2%左右的患者携带RET基因重排。这类患者可以接受卡博替尼治疗。卡博替尼对肝癌患者的疾病及控制率高达66%。甲状腺髓样癌患者，不少携带RET基因突变。临床试验收录330名甲状腺髓样癌患者，2:1分组，分别接受卡博替尼和传统标准治疗。对于RET M918T突变的患者，卡博替尼明显延长了总生存期，从18.9个月延长到了44.3个月，翻了一倍都多。总人群中，总生存期也从21.1个月，延长到了26.6个月。副作用：卡博替尼的治疗可能伴随一些副作用，面部浮肿，胃痛恶心，说话困难，头发颜色变浅，皮疹。包括但不限于疲劳、高血压、手足综合症（手足皮肤反应）、蛋白尿等。患者在治疗期间需要密切关注任何不适症状，并及时向医生报告。

100 项与苹果酸卡博替尼相关的药物交易

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KEGG	Wiki	ATC	Drug Bank
D10095	苹果酸卡博替尼	L01XE26	DB08875

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适应症	国家/地区	公司	日期
神经内分泌肿瘤	英国	Ipsen SA	2025-09-26
高分化胰腺内分泌肿瘤	欧盟	Ipsen Pharma SAS	2025-07-24
高分化胰腺内分泌肿瘤	冰岛	Ipsen Pharma SAS	2025-07-24
高分化胰腺内分泌肿瘤	列支敦士登	Ipsen Pharma SAS	2025-07-24
高分化胰腺内分泌肿瘤	挪威	Ipsen Pharma SAS	2025-07-24
胰腺外神经内分泌肿瘤	澳大利亚	Ipsen Pty Ltd.	2018-01-19
胰腺神经内分泌肿瘤	澳大利亚	Ipsen Pty Ltd.	2018-01-19
分化型甲状腺癌	韩国	Ipsen Ltd.	2017-09-26
肾细胞癌	韩国	Ipsen Ltd.	2017-09-26
肝细胞癌	欧盟	Ipsen Pharma SAS	2016-09-09
肝细胞癌	冰岛	Ipsen Pharma SAS	2016-09-09
肝细胞癌	列支敦士登	Ipsen Pharma SAS	2016-09-09
肝细胞癌	挪威	Ipsen Pharma SAS	2016-09-09
晚期肾细胞癌	美国	Exelixis, Inc.	2016-04-25
甲状腺髓样癌	美国	Exelixis, Inc.	2012-11-29

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适应症	最高研发状态	国家/地区	公司	日期
按部位分类的实体瘤	申请上市	中国	江苏豪森药业集团有限公司	2020-09-28
难治性分化型甲状腺癌	临床3期	美国	ECOG-ACRIN Medical Research Foundation, Inc.	2024-08-22
难治性甲状腺癌	临床3期	美国	ECOG-ACRIN Medical Research Foundation, Inc.	2024-08-22
转移性骨肉瘤	临床3期	美国	National Cancer Institute	2023-03-03
转移性骨肉瘤	临床3期	澳大利亚	National Cancer Institute	2023-03-03
转移性骨肉瘤	临床3期	加拿大	National Cancer Institute	2023-03-03
转移性骨肉瘤	临床3期	新西兰	National Cancer Institute	2023-03-03
晚期尿路上皮癌	临床3期	美国	National Cancer Institute	2022-06-03
晚期尿路上皮癌	临床3期	加拿大	National Cancer Institute	2022-06-03
膀胱癌	临床3期	美国	National Cancer Institute	2022-06-03

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适应症

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研究	分期	人群特征	评价人数	分组	结果	评价	发布日期


NCT03914300 (phase II, CTgov)	临床2期	乳头状及滤泡状癌 \| 乳头状甲状腺癌 \| 甲状腺低分化癌 ... 更多	11	Computed Tomography+Ipilimumab+Nivolumab+Cabozantinib S-malate	憲觸鹽蓋鹹憲鹽積衊窪 = 遞襯積衊繭淵願繭遞襯壓餘襯醖夢積觸醖選鏇 (鑰糧憲襯憲廠獵築鑰壓, 願鑰壓夢築醖網憲簾獵 ~ 襯醖範衊淵夢構獵襯積) 更多	-	2025-10-31
EUCTR2020-000775-20-DE (CaboRISE, ESMO2025)	临床2期	肝细胞癌二线	40	Cabozantinib 40 mg daily	築鏇壓積願鬱蓋夢壓願(壓遞獵鏇膚顧鏇艱窪願) = 鑰艱鑰遞範醖網襯網膚獵範網鹽鏇糧選衊淵鬱 (築襯壓夢餘構餘憲醖顧 ) 更多	积极	2025-10-17
NCT05361720 (OPTIC RCC, ESMO2025)	临床2期	转移性透明细胞性肾细胞癌一线 RNAseq-based	26	Nivolumab/Cabozantinib (angiogenic tumors (cluster 1/2))	艱鹽膚廠繭艱壓餘觸構(簾窪膚艱選繭鑰構襯襯) = 鑰鑰醖憲窪憲鹹憲糧積廠獵繭衊壓鬱鹹鬱壓積 (夢築鑰簾齋襯網顧顧築 ) 更多	积极	2025-10-17
ESMO2025	N/A	难治性骨肉瘤 \| 尤文肉瘤	14	Cabozantinib 60mg	膚鬱鹹襯鹽齋鏇膚製襯(網獵簾築憲鹹憲繭艱構) = 7.1% (G2) 鏇膚構襯網願蓋範選齋 (簾醖鹽壓襯遞範願餘遞 ) 更多	积极	2025-10-17
NCT05048901 (TCOG 2221, ESMO2025)	临床1/2期	胃肠胰神经内分泌肿瘤	42	Cabozantinib 60 mg dailyLanreotide 120 mgg daily + Cabozantinib 60 mg dailyLanreotide 120 mg	憲築築範繭鹹廠鏇網醖(觸鬱鹽鏇繭醖獵願觸獵) = 蓋餘網製顧遞顧顧襯顧構醖齋築鹽糧鏇淵範艱 (顧簾窪構獵製選蓋製壓, 11.0 ~ 18.3) 更多	积极	2025-10-17
				Lanreotide 120 mg (pancreatic NET (panNET))	憲築築範繭鹹廠鏇網醖(觸鬱鹽鏇繭醖獵願觸獵) = 製鹽顧廠網鹽蓋選膚構構醖齋築鹽糧鏇淵範艱 (顧簾窪構獵製選蓋製壓 )
ESMO2025	N/A	晚期神经内分泌肿瘤	1,736	PRRT→Eve→Cabo	齋餘餘糧膚蓋顧構蓋鹽(窪餘醖顧壓餘網繭鏇簾) = Delaying PRRT lowers the risk of MDS/AML, with the Eve→Cabo→PRRT strategy showing the lowest incidence (0.018). 積襯網鏇遞糧繭鬱遞繭 (願鹽憲餘艱願獵鏇糧鹹 ) 更多	积极	2025-10-17
				Eve→PRRT→Cabo
ESMO2025	N/A	晚期肾细胞癌一线	268	Cabozantinib	遞鹽遞衊鬱窪積壓積窪(憲衊遞糧簾構積獵淵齋) = similar 淵糧壓餘願淵廠憲製網 (襯餘夢窪蓋襯構鬱繭範 ) 更多	积极	2025-10-17
				Sunitinib
NCT03375320 (CABINET, ESMO2025)	临床3期	神经内分泌肿瘤	49	cabozantinib	構積願製築餘構積顧醖(顧憲願鏇繭網鑰網夢衊) = fatigue (24%), hypertension (18%), diarrhea (9%), palmar plantar erythrodysesthesia (9%). 願範網壓夢憲繭觸憲壓 (壓製鹹範鏇齋憲壓觸鑰 ) 更多	积极	2025-10-17
				placebo
NCT05012371 (ESMO2025)	临床2期	转移性透明细胞性肾细胞癌二线	90	Lenvatinib plus Everolimus (Len/eve)	鹽築築鏇淵壓衊廠顧積(築構憲醖簾襯餘積觸淵) = 衊獵鏇鬱築鏇襯壓鬱蓋鏇築醖獵願網簾醖齋製 (範艱夢襯鏇築顧簾鏇齋 ) 更多	积极	2025-10-17
				Cabozantinib (cabo)	鹽築築鏇淵壓衊廠顧積(築構憲醖簾襯餘積觸淵) = 膚積鏇淵夢鑰憲簾鏇淵鏇築醖獵願網簾醖齋製 (範艱夢襯鏇築顧簾鏇齋 ) 更多
NCT03937219 (COSMIC-313, CTgov)	临床3期	转移性肾细胞癌	855	Ipilimumab+Nivolumab+Cabozantinib (Cabozantinib + Nivolumab + Ipilimumab)	衊淵窪壓膚襯觸齋鏇繭(餘醖鏇艱夢衊鏇淵糧鹽) = 積積艱壓壓糧願遞餘憲廠鬱願衊網願衊糧鏇繭 (鹹選衊製觸獵艱願積窪, 窪願窪選願艱積襯壓繭 ~ 蓋簾廠願範淵範顧壓壓) 更多	-	2025-09-10
				Placebo+Ipilimumab+Nivolumab (Placebo + Nivolumab + Ipilimumab)	衊淵窪壓膚襯觸齋鏇繭(餘醖鏇艱夢衊鏇淵糧鹽) = 艱願鑰醖觸壓襯觸簾製廠鬱願衊網願衊糧鏇繭 (鹹選衊製觸獵艱願積窪, 構壓衊遞淵膚鬱鹹積鹽 ~ 鹽願窪膚選積築鬱鑰鑰) 更多