A Multicenter, Open-label, Randomized Controlled Clinical Study Comparing the Efficacy and Safety of ctDNA-guided Ribociclib Plus Endocrine Therapy Versus Chemotherapy Followed by Ribociclib Plus Endocrine Therapy as Adjuvant Treatment in Patients With HR+/HER2- Early Breast Cancer

This study is a prospective, multicenter, open-label, randomized controlled clinical trial designed to determine whether ribociclib plus endocrine therapy (ET) is non-inferior to adjuvant chemotherapy followed by ribociclib plus ET in patients with circulating tumor DNA (ctDNA)-negative, hormone receptor-positive/human epidermal growth factor receptor 2-negative (HR+/HER2-) early breast cancer.

开始日期2026-10-01

申办/合作机构

复旦大学

NCT07391774

/ Not yet recruiting临床3期IIT

A Phase III Trial of Rx Therapy Guided by Genomic Risk Assessment For High Anatomic Stage ER-pos/HER2-neg Breast Cancer With RS</=25 (RxFINE-Low)

This phase III trial compares standard of care hormone therapy plus ribociclib to chemotherapy followed by hormone therapy plus ribociclib for the treatment of patients with high anatomic stage breast cancer with low risk of the cancer returning (low risk recurrence). Ribociclib may stop the growth of tumor cells by blocking some of the enzymes needed for cell growth. Hormone therapy, with letrozole, anastrozole or exemestane, lowers the amount of estrogen made by the body. This may help stop the growth of tumor cells that need estrogen to grow. Chemotherapy drugs work in different ways to stop the growth of tumor cells, either by killing the cells, by stopping them from dividing, or by stopping them from spreading. Hormone therapy plus ribociclib may work as well as chemotherapy followed by hormone therapy plus ribociclib for the treatment of high anatomic stage breast cancer with low recurrence risk.

开始日期2026-07-07

申办/合作机构

National Cancer Institute

NCT07618390

/ Not yet recruiting临床2期IIT

A Phase ll, Interventional, Single-arm Study Evaluating the Efficacy and Safety of Inavolisib Plus Ribociclib and Fulvestrant in Chinese Patients With PIK3CA-mutant, HR-positive, HER2-negative Locally Advanced or Metastatic Breast Cancer.

This is a prospective, multicenter, open-label, single-arm phase II investigator-initiated study designed to evaluate the efficacy and safety of inavolisib in combination with ribociclib and fulvestrant as first-line treatment in Chinese patients with PIK3CA-mutant, hormone receptor-positive (HR+), HER2-negative (HER2-), endocrine-resistant metastatic breast cancer (mBC). Approximately 160 patients will be enrolled at around 16 centers in China.
The study consists of a screening period of up to 28 days, a treatment period, and a post-treatment follow-up period.
PIK3CA mutation status must be determined in blood or tumor tissue using polymerase chain reaction (PCR)-based assays or next-generation sequencing (NGS) performed in a local clinical laboratory. Patients with locally confirmed PIK3CA mutations who meet all eligibility criteria will be enrolled and receive study treatment with inavolisib, ribociclib, and fulvestrant. Details of the treatment regimen are provided in the Study Treatment section. Study treatment will continue until radiologically confirmed disease progression as determined by the investigator, unacceptable toxicity, withdrawal of informed consent, or study termination, whichever occurs first.
Patients must have measurable disease according to RECIST v1.1. Patients with bone-only metastases are not eligible, even if the lesions are considered measurable. Locally advanced disease must be unsuitable for surgical resection or other local treatment with curative intent.

开始日期2026-06-01

申办/合作机构

中山大学孙逸仙纪念医院

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100 项与琥珀酸瑞波西利相关的临床结果

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100 项与琥珀酸瑞波西利相关的转化医学

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100 项与琥珀酸瑞波西利相关的专利（医药）

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1,252

项与琥珀酸瑞波西利相关的文献（医药）

2026-12-31·Journal of Pharmaceutical Policy and Practice

Economic evaluation of cyclin-dependent kinases 4 and 6 inhibitors in advanced hormonal receptor-positive and human epidermal growth factor receptor 2 negative breast cancer: a nationwide budget impact analysis

Article

作者: Hamad, Anas ; Shafei, Laila ; Mohamed Ibrahim, Mohamed Izham ; Bojassoum, Salha ; Hisham Al-Ziftawi, Nour ; Elazzazy, Shereen

Background:

Several trials demonstrated improvements in clinical outcomes associated with cyclin-dependent kinase 4 and 6 (CDK4/6) inhibitors in breast cancer patients. The challenge remains regarding their high costs. Ribociclib and Abemaciclib are cost-effective in Qatar. Yet, their affordability was not studied. This budget impact analysis (BIA) is to assess the affordability of adopting CDK4/6 inhibitors in Qatar over five years duration (2024-2028).

Methods:

We ran a BIA to evaluate two scenarios: (1) Increasing abemaciclib's market share from 20% to 60%, replacing both palbociclib and ribociclib. (2) Assuming equal market share for both ribociclib and abemaciclib up to 80%, reducing palbociclib's share. The analysis considered treatment costs, patient population, and disease prevalence. All data were retrieved from the National Center for Cancer Care and Research, and costs were presented in Qatari Riyals (QAR). Sensitivity analyses were run to ensure the robustness of the conclusion. All results were compared to Qatar's budget threshold, which is QAR 453,822.

Results:

Based on a total of 173 patients using CDK4/6 inhibitors, increasing abemaciclib's market share to 60% yielded cumulative savings of QAR 14 million over five years, which is around QAR 14,613 per patient per year. However, equally increasing ribociclib's and abemaciclib's market share to 80% resulted in a modest budget increase, remaining within acceptable thresholds. Sensitivity analyses confirmed the robustness of these findings, showing that cost reductions and higher uptake rates further enhanced savings.

Conclusion:

Abemaciclib is a budget-saving option for HR+/HER2- breast cancer in Qatar, should it replace the market share by up to 60% over five years. In addition, ribociclib and abemaciclib are affordable treatment options if they equally contributes to up to 80% of the market share for the eligible advanced breast cancer patients. The results supported the concept of allocating CDK4/6 inhibitors as they were found to be affordable to the Qatari healthcare system.

2026-09-01·Biomaterials advances

Ribociclib-loaded folic acid conjugated chitosan-polycaprolactone hybrid nanoparticles for the management of glioblastoma

Article

作者: Mehra, Neelesh K ; Rajana, Naveen ; Quadros, Mural ; Mehta, Dhwani ; Islam, Md Asrarul ; Sanhueza Chavez, Carlos A ; Mokashi, Meghana ; Kumar, Sunil ; Gupta, Vivek ; Alkyam, Mayssam ; Ravula, Sravani ; Perron, Jeanette C

The objective of the present research investigation is to assess the anti-glioblastoma potential of Ribociclib (Ribo) and Ribociclib-loaded folic acid conjugated chitosan-polycaprolactone nanoparticles (RFCPNPs). Folic acid was conjugated to glycol chitosan by carbodiimide chemistry, and the formation of the conjugation was confirmed by FT-IR and ¹H NMR. RFCPNPs were fabricated by the single emulsification method, and particle size, PDI, surface charge, %EE, and % DL were 127.8 ± 4.37 nm, 0.197 ± 0.012, 5.05 ± 0.1 mV, 70.82 ± 4.25%, and 3.37 ± 0.20%, respectively. The presence of pH-sensitive biological macromolecule, i.e., chitosan, in the carrier system provides pH-sensitivity to RFCPNPs and displays diffusion-controlled release of the Ribo up to 48 h. RFCPNPs exhibited a bi-phasic release pattern, releasing approximately 22.9 ± 3.8%, 23.2 ± 5.8%, and 7.3 ± 1.2% of Ribo within 1 h, and 98.3 ± 1.6%, 86.6 ± 1.5%, and 75.8 ± 5.1% of Ribo were released from RFCPNPs in 48 h in pH 5.5, 6.8, and 7.4 dissolution media, respectively. The half-maximal inhibitory concentration (IC₅₀) of RFCPNPs was found to be 2.7 ± 0.3 and 3.2 ± 0.10 μM in U87 MG and U138 MG cells, which is 8-10-fold-, and 2-3-fold less than the pure Ribo and unconjugated nanoparticles, respectively. The receptor blocking assay demonstrated the significant role of folic acid in the anti-glioblastoma efficacy of the RFCPNPs. RFCPNPs exhibited enhanced ROS generation, apoptosis, and reduced mitochondrial membrane potential of U87 MG cells compared to the pure Ribo. RFCPNPs exhibited approximately 40% apoptotic cells, more than 1.6 times greater than those of the plain drug counterpart. The Ribo and RFCPNPs exhibited 27.1 ± 2.2%, 66.2 ± 1.3% cellular migration inhibition, and 380 ± 46 and 10 ± 4 colonies, respectively. U87 MG spheroids treated with Ribo and RFCPNPs demonstrated 64.3 ± 5.2% and 34.7 ± 11.0% viable cells, respectively. These outcomes suggest that the optimized nanocarrier represents a promising approach for treating glioblastoma.

2026-07-01·INTERNATIONAL JOURNAL OF CARDIOLOGY

Incidence and outcomes of atrial arrhythmia with cyclin dependent kinase 4/6 inhibitors in hormone receptor-positive / human epidermal growth factor receptor 2-negative breast cancer

Article

作者: Herrmann, Joerg ; Hodge, David O ; Davis, Nathaniel E ; Ruddy, Kathryn J ; Tan, Nicholas Y ; Blumenfeld, Sophia

BACKGROUND:

Cyclin-dependent kinase 4/6 (CDK4/6) inhibitors are increasingly used in hormone receptor-positive, HER2-negative (HR+/HER2-) breast cancer, yet emerging data suggest potential cardiotoxicity, including atrial arrhythmias (AA). Understanding incidence and outcomes of AA is essential as indications for CDK4/6 inhibitors expand.

OBJECTIVES:

To evaluate the incidence of new-onset AA and associated outcomes in patients with HR+/HER2- breast cancer treated with CDK4/6 inhibitors.

METHODS:

We conducted a retrospective cohort study of patients who received CDK4/6 inhibitors for HR+/HER2- breast cancer at Mayo Clinic from 2015 to 2024. The primary outcome was incidence of AA (atrial fibrillation, atrial flutter, or atrial tachycardia). Secondary outcomes included cerebrovascular events and all-cause mortality. Fine-Gray subdistribution hazard models and Cox regression models were used to assess risk factors for AA and all-cause mortality, respectively.

RESULTS:

Among 2773 patients, 59% received palbociclib, 28% abemaciclib, and 14% ribociclib. New-onset AA occurred in 42, cumulative incidence at 5 years of 2.1% (95% CI 1.5-2.8%). No significant differences in 5-year AA incidence were observed between agents: 1.5% (95% CI 0.7-2.8%), 2.3 (95% CI 1.6-3.2%), 1.0 (95% CI 0.3-2.6%) (p = 0.49). Multivariable analysis identified age at treatment as the only independent predictor of AA (HR 1.07, 95% CI 1.04-1.09, p < 0.001). New-onset AA was associated with increased mortality (HR 1.56, 95% CI 1.10-2.20, p = 0.012).

CONCLUSIONS:

Patients who receive CDK4/6 inhibitors for breast cancer experience a low but measurable risk of new-onset atrial arrhythmias. There was no significant difference in new-onset AA risk between agents. Prospective studies are needed to define mechanisms and guide monitoring strategies.

1,328

项与琥珀酸瑞波西利相关的新闻（医药）

2026-06-01

·PRNewswire

A combined therapeutic strategy aims to improve disease control in advanced hormone‑sensitive prostate cancer

MEDSIR has presented at the ASCO scientific congress, held in Chicago, the final results of its ZZ‑FIRST study, which support the potential of combining enzalutamide and talazoparib in high‑volume metastatic hormone‑sensitive prostate cancer. The study, which enrolled 54 patients from Spanish centers, evaluates a strategy to intensify standard therapy with the aim of blocking tumor progression before the cancer develops resistance to treatment, a frequent phenomenon in prostate cancer. CHICAGO, June 1, 2026 /PRNewswire/ -- MEDSIR, a leading international oncology research company, has presented the final results of the ZZ‑FIRST study during an oral session at the ASCO 2026 scientific congress, held in Chicago. This study evaluates a therapeutic intensification strategy in patients with advanced prostate cancer. Previously, the study demonstrated relevant treatment response results in more than 70% of cases, reflected by a decrease in PSA (prostate‑specific antigen) levels, a biomarker used in the blood monitoring of prostate cancer. ZZ-FIRST: a new therapeutic strategy Continue Reading Dr. Joaquin Mateo during ZZ-First oral session at ASCO 2026 In the ZZ‑FIRST study, a phase II, multicenter, randomized trial, 54 patients from eight centers across Spain were enrolled. Specifically, the trial included patients with high‑volume metastatic hormone‑sensitive prostate cancer (mHSPC), meaning a high tumor burden at diagnosis and typically a poorer prognosis. For these patients, current treatment is based on androgen deprivation therapy, usually in combination with next‑generation hormonal treatments such as enzalutamide. Since many prostate cancer cells depend on male hormones for growth (androgens such as testosterone), these therapies aim to block these hormonal signals by reducing testosterone levels and inhibiting their downstream effectors. However, over time, some tumors develop resistance and continue to grow despite hormonal blockade, becoming hormone‑resistant. In this context, the ZZ‑FIRST study evaluates the feasibility of intensifying initial treatment with enzalutamide by combining it with talazoparib (a PARP inhibitor, a protein involved in DNA repair) from earlier stages of the disease. By administering both drugs together while the disease is still hormone‑sensitive, the goal is to increase the accumulated DNA damage in tumor cells and promote their destruction before mechanisms of resistance to hormonal therapy emerge. The results presented at ASCO show that patients treated with the experimental combination achieved a radiographic progression‑free survival of 45.3 months, compared with 31.1 months in those treated with enzalutamide alone. This endpoint measures the time from treatment initiation until tumor progression is detected by imaging tests. In addition, patients receiving the combination also showed a longer time to PSA progression and to the development of resistance to hormonal therapy. In addition, adaptive tumor mechanisms were investigated before initiating therapy and during the first weeks of treatment with enzalutamide, providing key information to better understand how resistance develops. The ZZ‑FIRST results indicate that the combination of hormonal therapy with PARP inhibitors may particularly benefit patients whose tumors present certain mutation profiles in DNA repair genes. "Although patients with metastatic disease initially respond to hormonal therapy, the tumor eventually adapts and grows again. Therefore, it is essential to investigate the biological mechanisms that allow the tumor to develop resistance to hormonal treatment and to identify new therapeutic strategies capable of delaying or preventing this process," explained Dr. Joaquín Mateo, principal investigator of the study, oncologist at Vall d'Hebron University Hospital and Head of the Prostate Cancer Group at the Vall d'Hebron Institute of Oncology (VHIO), who presented the results at ASCO. ZZ‑FIRST has received external funding from Pfizer S.L., the Spanish Association Against Cancer (AECC), and the United States Department of Defense (DoD). The drugs used in the study were provided by Pfizer S.L. (talazoparib) and Astellas Pharma Europe Ltd. (enzalutamide). ADELA and CADILLAC: MEDSIR presence at the ASCO congress In addition to the presentation of the ZZ‑FIRST study, MEDSIR also presented the design of other studies during the congress. On the one hand, the company presented, in collaboration with the Menarini Group, the design of the ADELA study, an international phase III trial evaluating the selective estrogen receptor degrader (SERD) elacestrant combined with everolimus versus elacestrant monotherapy. The study includes patients with ER+/HER2‑ tumors who developed an ESR1 gene mutation after progression on prior endocrine therapy and CDK4/6 inhibitors. The trial is being implemented in more than 100 hospitals across nine countries, including Spain, Austria, the Czech Republic, Greece, the United Kingdom, France, Italy, Germany, and Brazil. On the other hand, the CADILLAC study is also noteworthy. This is an international phase II trial evaluating the efficacy and safety of combining the SERD camizestrant with the CDK4/6 inhibitor ribociclib in patients with advanced HR+/HER2‑ breast cancer who have stopped responding to standard treatments. The study, currently ongoing at centers in Spain, Germany, and China, includes 150 patients whose data will be compared with historical records from more than 150 patients receiving conventional therapy. About MEDSIR Founded in 2012, MEDSIR is distinguished by its close collaboration with strategic partners to drive innovation in oncology research. With headquarters in Spain and the United States, the company provides comprehensive management of clinical trials, from study design through to publication, supported by an extensive global network of experts and integrated technology to streamline the process. The company offers support for proof‑of‑concept studies and a strategic approach that allows research partners to benefit from the best of both worlds: industry clinical research and investigator‑driven trials. More information: SOURCE MEDSIR 21% more press release views with Request a Demo

临床结果临床2期临床3期

2026-06-01

·BiG生物创新社

明明III期阳性，为什么 FDA 还是犹豫了？

阿斯利康寄予厚望的口服 SERD 药物 camizestrant，最新进展看起来有些矛盾。一方面，这不是一个没有数据支撑的项目。SERENA-6 是一项阳性 III 期研究，阿斯利康已向 FDA 提交 NDA，FDA 也曾授予该适应症突破性疗法认定。另一方面，FDA 在 2026 年 4 月 ODAC 会议后并未顺利放行，咨询委员会以 6:3 的结果认为其 benefit-risk 尚不足以支持批准；5月27日，FDA 又延长 PDUFA 审评时间，以评估公司补充提交的长期疗效分析。这件事有意思的地方在于，争议并不主要来自一个常规问题：药物有没有活性？Camizestrant 作为口服 ER antagonist / SERD，其机制逻辑并不难理解；SERENA-6 也确实达到了主要终点。真正把它卡住的，是一个更前沿、也更难被监管接受的问题：当 ctDNA 提前捕捉到 ESR1 突变，但患者尚未发生影像学进展时，是否应该提前换药？换句话说，FDA 要评估的不是单一分子的成败，而是一种新的治疗范式：治疗决策是否可以从“疾病进展后换药”，前移到“分子耐药信号出现时换药”。Camizestrant 暴露出的，也不是 SERD 赛道的简单降温，而是精准治疗进入动态监测阶段后的新门槛：药企不仅要证明药物能作用于靶点，还要证明在更早的分子耐药阶段改变治疗，确实能带来足够明确、可解释、并被监管接受的临床获益。 01 SERENA-6真正想证明的不只是camizestrant有效要理解FDA的犹豫，先要理解SERENA-6的设计。在 HR+/HER2- 晚期乳腺癌中，芳香化酶抑制剂（AI）联合 CDK4/6 抑制剂是重要的一线内分泌治疗组合。ESR1 突变常被视为 AI 治疗压力下出现的耐药机制之一。传统做法通常是等到患者影像学进展后，再进入下一线治疗。但 SERENA-6 试图把治疗动作提前：患者在接受 AI + CDK4/6 抑制剂治疗期间，通过 ctDNA 监测发现 ESR1 突变；如果尚未影像学进展，就随机切换为 camizestrant + CDK4/6 抑制剂，或继续原来的 AI + CDK4/6 抑制剂。 SERENA-6的临床设计这意味着，SERENA-6 的核心创新不是又做了一个口服 SERD，而是把 ESR1 突变从一个解释耐药的 biomarker，变成一个触发治疗切换的决策点。这一步非常关键。因为在精准治疗里，找到 biomarker 只是第一层；证明在 biomarker 出现的那个时间点进行干预，能带来患者真正获益，才是第二层。SERENA-6 想证明的正是第二层。FDA 的疑问也集中在这里：这项研究是否足以证明，提前换药优于等到影像学进展后再换药？ 02 FDA 真正质疑的是“提前换药”的临床含义 FDA 的核心观点可以概括为一句话：SERENA-6 证明了一个 PFS 差异，但还没有充分证明“在 ESR1 突变出现时提前换药”这一策略本身具有明确长期获益。在 ODAC 文件中，FDA 明确指出，目前尚无药物获批用于在 ESR1 突变被检测到、但患者尚未影像学进展时切换治疗。SERENA-6 没有直接比较“ESR1 突变出现时换药”与“继续原方案直到影像学进展后再换药”哪一种更好。也就是说，试验回答的是提前切换后的 PFS 是否改善，却没有完全回答提前切换是否比标准序贯策略更优。尚无药物用于1.5L治疗这也是为什么 FDA 特别关注对照组。SERENA-6 中，对照组患者继续 AI + CDK4/6 抑制剂后，在疾病进展或死亡前仍有一段中位治疗时间。FDA 的担心是：如果这些患者在原治疗下还能获益，提前换药是否意味着没有充分利用当前治疗线？这个问题在肿瘤慢病化背景下越来越重要。对于治疗窗口较短、疾病快速进展的肿瘤，提前干预的逻辑更容易被接受。但在 HR+ 乳腺癌这样治疗序列较长的疾病中，监管方会更关心整个治疗旅程，而不是单个时间点的 PFS 差异。因此，camizestrant 的监管争议，本质上是序贯治疗问题：什么时候换药，换药后能否延长总治疗获益，是否减少后续化疗，是否改善生活质量，是否最终体现为更长生存。 03 PFS 阳性为什么仍然不够？ SERENA-6 达到了 PFS 主要终点，但 FDA 对这个 PFS 的解释保持谨慎。关键在于，SERENA-6 的 PFS 起点并不是传统意义上的一线治疗开始，也不是影像学进展后进入二线治疗，而是“检测到 ESR1 突变并随机化”这一新时间点。FDA 在 briefing document 中明确表示，这种从 ESR1 突变检测时开始计算的 PFS，是一个新的起点；其临床意义是否等同于传统 PFS，并不确定。 Camizestrant达到PFS 主要终点这不是统计学问题，而是临床解释问题。如果一个患者在 ctDNA 中检测到 ESR1 突变，但影像学上仍稳定，那么这个患者究竟处于“必须马上换药”的状态，还是仍可继续从当前治疗获益？如果提前换药后 PFS 延长，这个延长究竟代表真实延迟进展，还是部分来自更早定义治疗起点？这些问题会直接影响监管对 PFS 的信任程度。 FDA 对 PFS2（从随机分组/开始治疗，到患者在下一线治疗后再次疾病进展或死亡的时间）也持保留态度。PFS2 理论上可以帮助判断后续治疗旅程是否被改善，但 FDA 认为，在 SERENA-6 中，后续治疗选择、地区可及性、研究者判断等因素都会影响 PFS2 的可解释性；同时，对照组患者进展后并未允许 crossover 到 camizestrant + CDK4/6 抑制剂，这使得它无法清晰回答“提前换药是否优于进展后换药”。 OS 则是更有力、但目前仍不成熟的证据。FDA 文件提到，SERENA-6 的 OS 数据尚不成熟，最终 OS 分析预计要到 2028 年左右，且统计把握度有限。换句话说，如果未来 OS 或更完整的长期获益数据足够有说服力，可能会缓解部分争议；但在当前时点，FDA 仍认为证据链不够完整。 04 安全性不是唯一核心但会放大不确定性这次 FDA 争议不能简单归因于安全性。ODAC 和 FDA 的讨论重心更多集中在试验设计、终点解释和长期获益不确定性上。但安全性仍然重要，因为当获益解释本身存在争议时，任何额外风险都会被放大。 FDA 文件提到，camizestrant 与心率降低、QT 延长相关；当与可能延长 QT 的药物，如 ribociclib，联用时，可能增加心律失常风险。文件还提到，开发项目中曾有患者在 camizestrant 与 ribociclib 联用剂量下出现 bradycardia、QT prolongation 和 Torsades de Pointes。 Camizestrant可能有心律失常风险这并不意味着 camizestrant 的安全性不可管理，也不意味着心脏风险就是审评延长的唯一原因。更准确的理解是：当主要获益来自一个监管尚未完全认可的新治疗时点和新 PFS 语境时，监管方会要求更清晰的 benefit-risk 平衡。如果一个治疗策略能够明确延长 OS，或显著延迟化疗、改善生活质量，安全性风险的接受度会更高；但如果获益仍主要依赖一个临床意义尚待解释的 PFS，安全性信号就会让 FDA 更难快速作出正面判断。 05 ESR1 赛道没有结束但竞争门槛变了 Camizestrant 的审评延长，并不是ESR1或oral SERD赛道失败。更稳健的判断是：这个赛道正在从“分子竞争”进入“治疗路径竞争”。过去，oral SERD/ER antagonist 的主要叙事是：能否更好降解或抑制 ER，能否覆盖 ESR1 突变，能否替代注射给药的 fulvestrant。但在 CDK4/6 抑制剂已经深度改变 HR+ 乳腺癌治疗格局之后，单纯讲“更强分子”已经不够。真正的问题变成：它应该放在哪一线？用于什么患者？在 ESR1 突变刚出现时用，还是进展后用？是否继续 CDK4/6 抑制剂？主要终点如何被监管接受？阿斯利康仍在推进 camizestrant 的其他 III 期项目，包括更广泛治疗场景下的 SERENA-4、CAMBRIA-1 和 CAMBRIA-2 等研究。这个事实本身说明，当前争议不是机制被完全否定，而是 SERENA-6 所代表的“ctDNA 触发提前换药”路径还需要更强证据。 Camizestrant的其他III期研究这对整个 ESR1 领域都有启发。未来能跑出来的项目，未必只是活性最强的分子，而是能把biomarker、治疗线、联合方案、对照组、终点和监管沟通整合得最清楚的项目。换句话说，精准治疗的难点已经从“找到突变”升级为“证明在正确时间点改变治疗，真的改变患者结局”。Camizestrant 卡在 FDA 门口，真正提示的是这个新门槛。结语这个悬念不只属于阿斯利康短期看，camizestrant 的美国审评仍有悬念。FDA 延长审评时间，意味着它仍在评估阿斯利康提交的补充分析；ODAC 的投票也只是咨询意见，并不等于最终监管结论。但从产业视角看，这个案例的意义已经超出单一药物。随着 ctDNA、MRD 和动态 biomarker 逐渐进入肿瘤临床开发，药企会越来越频繁地面对同一个问题：能不能在影像学进展之前，用分子信号提前改变治疗？这个方向当然有吸引力。它代表更早发现耐药、更早调整治疗、更少等待疾病恶化。但监管不会因为逻辑优美就自动接受。它需要试验证明：提前干预不是提前消耗治疗线，而是让患者获得更长、更可解释、更有临床意义的获益。所以，camizestrant 的故事不是SERD 行不行这么简单。它真正提出的问题是：精准治疗进入动态监测时代后，临床开发能否跟上 biomarker 的速度？最终，精准治疗的下一道门槛，可能不是找到突变，而是证明在突变出现的那个时间点改变治疗，真的让患者走得更远。 Reference 1. AstraZeneca. US FDA decision date extended for SERENA-6 filing of camizestrant to enable review of additional data. 27 May 2026. 2. FDA. Oncologic Drugs Advisory Committee Meeting, April 30, 2026: Combined FDA and Applicant ODAC Briefing Document for camizestrant, NDA 220359. 3. https://www.astrazeneca.com/content/dam/az/PDF/2026/eq1/Q1-2026-results-presentation.pdf 4. Reuters. US FDA extends review of AstraZeneca's experimental breast cancer pill. 27 May 2026. 5. https://x.com/ryanhuey/status/1929264918068347121 共建Biomedical创新生态圈！如何加入BiG会员？

2026-05-30

·生物通

巴林通过基于价值的定价推动药品政策改革与医疗卫生可持续性

巴林的医疗卫生体系通过一系列政府主导的改革与投资逐步发展，建立了初级与三级医疗服务，并在“全民健康（Health for All）”倡议下提供免费医疗服务。本文从政策视角探讨巴林的药品监管、定价策略与框架、医药市场与支出情况，并以乳腺癌和糖尿病（diabetes mellitus）为案例，同时分析关键挑战与未来政策重点，包括基于价值的定价和医疗卫生体系发展。2015年至2022年间，卫生支出占国内生产总值（GDP）的平均比例估计为4.44%，范围为3.84%至4.98%，其中2022年最低，为3.84%。由于本地制造能力有限，药品预算的大部分被用于药品进口。2024年药品进口额达到4.6426亿美元，2023年人均卫生支出约为1175.82美元。价格审查政策已通过药品追踪追溯系统（track-and-trace system）以及持证代理商监管等措施帮助降低成本。目前，有两类主要疾病对医疗卫生体系构成挑战：其一为乳腺癌，巴林在海湾合作委员会（GCC）地区属于发病率最高的国家之一，2020年每10万人中发病44.2例；其二为糖尿病，2024年患病率为22.1%，由此带来显著的直接成本并加剧预算压力。为改善可及性与可负担性，关键政策举措包括将卫生技术评估（Health Technology Assessment, HTA）纳入决策和价格谈判、促进本地制造，以及结合数据驱动政策实施基于价值的定价。该文发表于《Discover Health Systems》，是一篇聚焦巴林药品政策与卫生体系可持续性的政策分析文章。研究背景在于，巴林虽已通过长期政府主导改革建立覆盖初级医疗与三级医疗的服务体系，并在“全民健康”框架下提供广泛公共医疗保障，但其医药市场规模受人口规模和产业基础限制，药品供应高度依赖进口，本地制造能力不足，专利药占比较高，因而医疗财政承压明显。与此同时，巴林卫生支出虽处于海湾合作委员会（GCC）国家常见区间，但面对乳腺癌与糖尿病等高负担慢性病时，药品支出、创新疗法可及性与预算可持续性之间的矛盾更加突出。正因如此，围绕药品监管、价格形成机制、仿制药与生物类似药替代、卫生技术评估（Health Technology Assessment, HTA）以及基于价值的定价（value-based pricing, VBP）的制度优化，成为开展本项研究的现实依据。研究人员围绕巴林药品监管体系、国家卫生监管局（National Health Regulatory Authority, NHRA）定价框架、医药市场结构与卫生支出、乳腺癌与糖尿病两类重点疾病负担，以及未来政策重点进行了系统梳理。研究显示，巴林已形成较为完备的药品注册与价格管理制度，以外部参考定价（External Reference Pricing, ERP）为核心，并结合内部参考定价（Internal Reference Pricing, IRP）和到岸成本（cost, insurance, and freight, CIF）规则实施药品定价；同时通过条码化与全链条追溯制度、持证代理制度等措施强化药品质量与供应链安全。在疾病负担层面，乳腺癌和糖尿病构成当前最重要的财政与服务压力来源，前者需要持续投入高成本肿瘤创新药物与筛查资源，后者则因高患病率带来庞大的直接医疗成本。研究最终指出，巴林未来若要兼顾药物可及性、可负担性与医保财政稳定，应进一步扩大仿制药和生物类似药使用，推动HTA制度化嵌入价格谈判与报销决策，并逐步向VBP模式过渡，以支持卫生体系的长期可持续发展。从研究设计看，本文主要采用政策综述与卫生体系分析方法，综合梳理巴林药品监管制度、NHRA药品定价指南、医药市场与宏观卫生支出数据，并选取乳腺癌与2型糖尿病作为疾病案例进行财政和服务负担分析。文中涉及的样本或数据来源主要包括国家法规文件、NHRA公开数据、巴林肿瘤中心（BOC）药房2023年药物消耗数据、初级卫生保健成本数据、2015年卫生部（MOH）数据支持的糖尿病疾病成本研究，以及GCC与国际组织公开统计资料。一、Introduction 论文首先介绍巴林卫生体系的发展脉络。研究人员指出，巴林作为GCC成员国中人口规模较小的国家，医疗体系是在长期政府投资与制度改革基础上建立起来的，已形成初级与三级医疗并存、公共医疗覆盖较广的服务格局。人口规模较小虽然影响了药品市场容量，但卫生支出占GDP比例更多反映国家收入水平与财政优先序。由于本地制药工业有限，巴林主要依赖药品进口，仅有少数本地企业生产维生素、糖浆和部分注射制剂。文章同时指出，巴林药品制度具有较强适应性，药品审批受美国食品药品监督管理局（FDA）和海湾地区监管批准经验影响，价格形成主要依赖ERP并常结合IRP，这为后续讨论药品价格治理和VBP转型奠定了制度背景。二、Pharmaceutical regulation in Bahrain 在“巴林的药品监管”部分，研究人员梳理了区域与国家双层监管结构。海湾中央药品注册委员会（GCC-DR）负责区域层面的药品审批协调，而NHRA则依据2009年第38号法律于2010年成立，负责政府与私营部门的独立卫生监管。文中指出，NHRA依托国际标准与科学证据开展监管，其职责涵盖医疗机构和卫生专业人员许可、药品注册与定价、制药工厂许可、临床试验审批以及纪律处分等。研究通过2023年新增743项药品申请、累计注册药品4211种的数据表明，巴林药品市场虽然规模有限，但监管体系较完整、市场准入流程较规范。三、NHRA’s pricing framework and policy 在“NHRA的定价框架与政策”部分，论文详细总结了巴林药品定价机制。研究人员指出，NHRA自2013年发布《药品定价指南》后持续更新，2022年版本进一步扩展了定义、定价机制以及价格谈判与企业申诉规则，并体现了海湾卫生委员会（Gulf Health Council）统一价格实施方向。具体而言，药品定价以CIF为基础，并按固定汇率换算为巴林第纳尔后计算零售价格。创新药的CIF价格可依据原产国证明（COO）出厂价加运保费、全球最低CIF价格，或与巴林已注册相似治疗或化学属性药物价格比较确定。首个仿制药进入市场后，原研药价格下调20%；若原研药晚于仿制药上市，则须遵循最低适用价格规则。研究还指出，仿制药和生物类似药通过阶梯式降价机制推动竞争。首个仿制药价格在原研药降价基础上进一步下调，第二、第三及之后进入市场的仿制药继续逐步降价。对于复方制剂、不同规格和不同包装，也存在成体系的比例降价规则。这些规则显示，巴林当前药品定价政策主要目标在于区域价格对齐、控制零售价格和提升市场可负担性，但其核心仍是参考定价和成本加成逻辑，而非正式的VBP框架。四、Pharmaceutical market and spending 在“医药市场与支出”部分，研究人员结合注册、价格修订、供应链监管和宏观支出数据说明巴林医药市场特征。NHRA在药品注册和续注册过程中实施结构化价格管理，若原产国或参考市场价格下降，或生产信息改变，价格可被重新评估。为防止假药流入，巴林已建立国家级条码与追溯系统，实现受监管药品供应链全流程可追踪。根据相关法令，仅有NHRA授权的本地持证代理可进口并分销获批药品。文中数据显示，2024年巴林药品进口额约4.6426亿美元，2023年人均卫生支出约1175.82美元；2015年至2022年卫生支出占GDP平均为4.44%。2021年药品销售额估计为5.28亿美元，相当于GDP的1.32%，其中专利处方药占总药品支出的57%，仿制处方药约占总市场33%，处方药销售总体占全部药品销售约90%。这些结果表明，巴林药品市场对进口和专利药依赖度高，是卫生财政可持续性的关键制约因素。五、Breast cancer in Bahrain: Incidence, services, and cost challenges 在“巴林乳腺癌：发病、服务与成本挑战”部分，研究人员指出，癌症是巴林仅次于心血管疾病的第二大死亡原因，而乳腺癌（breast cancer, BC）是女性中负担尤为突出的恶性肿瘤。文中依据历史登记数据表明，巴林女性乳腺癌年龄标化发病率长期处于GCC较高水平，2000年为每10万人58.2例，2010年为44.4例，2020年为44.2例。研究进一步总结了服务体系建设：1994年巴林开始实行癌症强制报告，2005年对40岁及以上女性实施乳腺X线摄影筛查，2019年成立巴林肿瘤中心（BOC），增强了先进诊断、治疗和移植服务能力；复杂病例此前常需政府资助转诊海外。为缓解人力短缺，巴林自2000年起支持本国肿瘤科医师海外培训，并在初级医疗机构扩展乳腺筛查设备与咨询服务。研究还提到，下一代测序（Next-generation sequencing, NGS）面板已用于多基因检测，以支持风险预测和个体化治疗选择。在成本层面，2019年成立的国家肿瘤委员会（National Tumour Board, NTB）为多学科病例评审平台，强调遵循国家综合癌症网络或英国国家卫生与临床优化研究所指南，并兼顾成本效益管理。随着患病负担上升，巴林也尝试通过引入仿制药和生物类似药降低部分治疗成本。尽管如此，乳腺癌防治仍对财政造成显著压力。文章引用初级卫生保健成本数据说明，癌症筛查服务成本高于心血管疾病或糖尿病风险筛查；在药物支出方面，BOC药房2023年数据显示，Pembrolizumab 100 mg年度成本最高，约720万美元，而Ribociclib 200 mg片剂为使用频率最高的药物之一。研究据此说明，保障创新肿瘤药物可及性虽具有重要临床意义，但也显著加重了公共预算负担。六、Diabetes mellitus in Bahrain: prevalence, costs, and policy priorities 在“巴林糖尿病：流行、成本与政策优先序”部分，研究人员指出，糖尿病（diabetes mellitus）在巴林及整个海湾地区均已成为重大公共卫生问题，其高流行与社会经济发展、生活方式改变及肥胖增加密切相关。文中显示，2024年巴林成人糖尿病患病率为22.1%，较2011年的19.5%进一步上升。面对这一趋势，政府将预防作为优先方向，通过卫生部（MOH）提供免费的健康宣传、专科门诊和专业人员培训；巴林糖尿病协会（BDS）也通过患者及家庭教育、咨询与宣教支持相关工作。关于经济负担，研究援引2019年发表、基于2015年MOH数据的首项患病率基础疾病成本研究，指出2型糖尿病总成本估计为2.8115亿美元，占GDP的0.9%；其中直接医疗成本为2.779亿美元，患者年均成本为3084美元，因缺勤产生的间接成本为326万美元。研究并强调，直接医疗成本占2015年卫生总支出的15.3%，占MOH预算的22.0%，说明糖尿病已构成显著的财政压力。文章还总结了巴林在创新治疗准入方面的进展，例如司美格鲁肽（Semaglutide）和恩格列净（Empagliflozin）均已获批，其中部分制剂在特定情况下可免费提供，反映出巴林在控制疾病负担与引入新疗法之间寻求平衡。七、Key challenges and future policy priorities 在“关键挑战与未来政策重点”部分，研究人员归纳了巴林药品政策改革的核心难题。首先，市场结构性问题突出，包括进口依赖、本地生产薄弱、专利药主导以及仿制药促进政策有限或执行情况不明。其次，药品注册所需文件与认证要求较为复杂，可能延缓市场准入并削弱价格竞争。再次，尽管巴林已建立系统化ERP与CIF导向定价框架，但尚无证据表明VBP已正式纳入定价或报销流程，特别是在高价生物制剂和专科药品领域。NHRA 2021―2025战略强调监管强化、合规、安全监督、绩效指标和数据系统建设，但并未明确提出VBP模型。研究进一步指出，GCC层面的改革路线图已提出从以数量为基础的模式向基于价值的医疗卫生（value-based healthcare）框架转型，但实施程度在各成员国之间不一。当前主要障碍包括卫生技术数据系统不足、技术专长有限，以及政府、药企、支付方和卫生专业人员之间的协同不足。为解决这些问题，路线图建议扩展遗传数据库和筛查项目、实施风险分担协议、协调HTA与真实世界证据（real-world evidence）收集，以及建立长期数字卫生平台和VBP机制。论文据此强调，HTA能力建设是实现VBP和高质量卫生资源配置的关键前提，而巴林虽尚未正式将HTA和VBP嵌入现行NHRA定价体系，但已将HTA能力建设和循证决策整合作为持续改革的重要方向。综合讨论部分，论文认为，巴林已经形成一个受监管的药品市场，具备结构化定价指南、ERP、药品注册控制以及条码化与序列化要求，这些制度有助于促进药品质量、安全与区域价格一致性。但在慢性病高负担背景下，采购效率、处方行为和价格决策透明性仍有进一步优化空间。文章强调，应把政策重点放在高患病率疾病领域，尤其是肿瘤和糖尿病治疗中扩大仿制药与生物类似药使用，以在不损害结局的前提下降低药物支出；通过系统化电子处方审计强化成本效益导向处方；更广泛、正式地应用HTA支撑透明、循证的定价与报销决策；并通过改进需求预测和药物经济学（pharmacoeconomics）评估提升采购效率。整体上，这些政策组合有望改善药品可负担性、维持医疗可及性，并支持卫生预算的长期可持续性。结论部分可译为：巴林已建立受监管的药品市场，并以结构化定价指南、外部参考定价、产品注册管控以及条码和序列化要求为支撑。这些措施促进了药品质量、安全性和区域价格协调。未来仍可进一步优化采购效率和处方实践。鉴于慢性疾病负担显著，政策优先事项应聚焦高患病率疾病。在肿瘤和糖尿病照护中扩大仿制药和生物类似药的使用，可在不影响结局的情况下减少药物支出。引入系统化电子处方审计可增强对成本效益处方的遵循。更广泛且正式地使用卫生技术评估（HTA），可支持透明、循证的定价与报销决策。改进需求预测与药物经济学评估可提升采购效率。这些行动将有助于提高可负担性、维持可及性，并支持卫生预算的长期可持续性。

100 项与琥珀酸瑞波西利相关的药物交易

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外链

KEGG	Wiki	ATC	Drug Bank
-	琥珀酸瑞波西利	L01XE	DB11730

研发状态

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10 条最早获批的记录,

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适应症	国家/地区	公司	日期
晚期乳腺癌	加拿大	Novartis Pharmaceuticals Canada, Inc.	2018-03-02
转移性乳腺癌	加拿大	Novartis Pharmaceuticals Canada, Inc.	2018-03-02
HR阳性/HER2阴性乳腺癌	美国	Novartis Pharmaceuticals Corp.	2017-03-13

未上市

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适应症	最高研发状态	国家/地区	公司	日期
晚期 HER2 阳性乳腺癌	临床3期	美国	Novartis AG	2022-03-28
晚期 HER2 阳性乳腺癌	临床3期	葡萄牙	Novartis AG	2022-03-28
晚期 HER2 阳性乳腺癌	临床3期	西班牙	Novartis AG	2022-03-28
早期乳腺癌	临床3期	-	Novartis Pharmaceuticals Corp.	2018-03-31
HER2 阴性乳腺癌	临床3期	意大利	Novartis Pharmaceuticals Corp.	2018-02-02
6型髓鞘减少脑白质营养不良	临床3期	意大利	Novartis Pharmaceuticals Corp.	2018-02-02
局部晚期乳腺癌	临床3期	意大利	Novartis Pharmaceuticals Corp.	2018-02-02
乳腺癌	临床3期	美国	Novartis Pharmaceuticals Corp.	2017-06-07
晚期癌症	临床3期	美国	Novartis Pharmaceuticals Corp.	2016-11-30
晚期癌症	临床3期	阿根廷	Novartis Pharmaceuticals Corp.	2016-11-30

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临床结果

适应症

分期

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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


NCT02555189 (CTgov)	临床1/2期	转移性去势抵抗性前列腺癌	52	Multigated Acquisition Scan+Enzalutamide+Ribociclib (Phase I: 200 mg Ribociclib + Enzalutamide)	蓋淵遞襯蓋網襯廠製廠 = 醖鹽夢鬱糧襯蓋顧鬱願醖願獵觸夢艱簾鹹醖艱 (憲積膚餘簾鬱鹽鑰醖膚, 淵構製製夢觸簾製築簾 ~ 選獵廠鹽衊範築衊範襯) 更多	-	2026-04-22
				Multigated Acquisition Scan+Enzalutamide+Ribociclib (Phase I: 400 mg Ribociclib + Enzalutamide)	蓋淵遞襯蓋網襯廠製廠 = 鹽夢網窪蓋窪願網淵鏇醖願獵觸夢艱簾鹹醖艱 (憲積膚餘簾鬱鹽鑰醖膚, 觸艱網壓鹹鹽觸積膚鏇 ~ 鏇遞夢蓋鬱範選繭鏇壓) 更多
NCT02985125 (CTgov)	临床1/2期	转移性胰腺腺癌	12	LEE011+everolimus (Phase I - Dose Level 1)	遞範獵築鬱構壓簾鹽鏇(顧繭襯蓋鬱鹽鏇蓋廠願) = 獵鏇艱獵衊艱顧觸網顧觸醖鹹積膚憲鏇蓋網遞 (淵範積齋衊齋獵構獵構, 範淵簾積範膚鏇觸鬱顧 ~ 鬱鑰簾顧壓構廠鹽糧淵) 更多	-	2026-04-07
				LEE011+everolimus (Phase I - Dose Level 2)	遞範獵築鬱構壓簾鹽鏇(顧繭襯蓋鬱鹽鏇蓋廠願) = 淵繭壓廠構衊憲憲襯襯觸醖鹹積膚憲鏇蓋網遞 (淵範積齋衊齋獵構獵構, 餘鑰鬱獵獵獵夢觸獵壓 ~ 鹽窪鏇齋膚鏇糧膚蓋艱) 更多
NCT02712723 (FELINE, CTgov)	临床2期	ER阳性/HER2阴性乳腺癌	121	Placebo+Letrozole (Placebo + Letrozole)	憲築醖簾夢積壓簾艱構 = 衊鹹鏇糧獵願遞鏇蓋艱築憲選願觸憲鏇壓簾齋 (遞夢鑰憲壓願壓鏇範膚, 繭製範積獵顧網窪窪壓 ~ 膚積範製築衊鑰鬱獵醖) 更多	-	2026-03-11
				Letrozole+Ribociclib (Ribociclib 600 mg + Letrozole)	憲築醖簾夢積壓簾艱構 = 夢蓋壓窪鬱鹽艱繭鹽鏇築憲選願觸憲鏇壓簾齋 (遞夢鑰憲壓願壓鏇範膚, 獵鬱觸選膚獵簾構願鹹 ~ 憲願願鹹蓋窪膚鑰醖獵) 更多
ESGO2026	临床1/2期	卵巢浆液性腺癌	70	Ribociclib + letrozole	鹹膚範餘遞憲鏇夢膚糧(築淵觸蓋鏇網糧鬱遞製) = 積餘簾積繭築壓襯鹹蓋積鏇襯鏇艱鬱廠鑰鹹選 (鹽製憲醖築艱積鬱簾壓 ) 更多	积极	2026-02-28
				Ribociclib + letrozole	鹹膚範餘遞憲鏇夢膚糧(築淵觸蓋鏇網糧鬱遞製) = 繭齋範衊顧齋壓獵餘餘積鏇襯鏇艱鬱廠鑰鹹選 (鹽製憲醖築艱積鬱簾壓 )
NCT03673124 (CTgov)	临床2期	复发性低级别输卵管浆液性腺癌 \| 卵巢癌 \| 浆液性囊腺癌	51	Letrozole+Ribociclib	築鹹選選襯鏇築鬱繭糧 = 獵淵廠鹽構壓齋鬱壓網壓網顧衊簾遞鹹糧鹹鹹 (鹹膚顧築淵遞網衊鬱醖, 範鏇繭鹹糧衊鑰襯獵餘 ~ 醖築鹽蓋醖膚衊選糧鹽) 更多	-	2025-12-23
NCT03701334 (BT CRC 1602, SABCS2025)	临床1/2期	AR阳性/ER阳性/HER2阴性乳腺癌 AR-positive	21	ribociclib+bicalutamide	壓夢餘鑰範構鏇築構廠(積淵選獵淵觸製淵鏇鹹) = 廠蓋艱網積窪遞膚選願鹽艱餘蓋遞糧選鹹顧廠 (餘鬱簾淵衊鹹築範襯蓋, 0.097 ~ 0.535) 更多	积极	2025-12-12
SABCS2025	N/A	HR阳性/HER2阴性乳腺癌辅助 HR+ \| HER2-	197	Ribociclib	顧願遞築築襯遞顧簾窪(製鹽繭築顧齋積選襯壓) = 範簾遞蓋醖觸餘鏇鬱築構膚壓鑰構繭築淵衊鬱 (鏇繭淵選鏇壓淵糧廠築, 17.57) 更多	积极	2025-12-11
				Abemaciclib	顧願遞築築襯遞顧簾窪(製鹽繭築顧齋積選襯壓) = 齋觸積鏇鹽獵膚顧積蓋構膚壓鑰構繭築淵衊鬱 (鏇繭淵選鏇壓淵糧廠築, 22.26) 更多
NCT03285412 (LEADER, SABCS2025)	临床2期	ER阳性/HER2阴性乳腺癌 ER+ \| HER2-	152	Ribociclib 400mg plus aromatase inhibitor	積醖鏇衊醖窪鬱蓋簾膚(鏇襯襯醖鹹獵餘積繭願) = 艱繭鏇窪鹹鹹夢鹹夢選襯範構顧廠糧觸衊壓蓋 (餘餘鬱鑰夢繭淵選鏇鏇 ) 更多	积极	2025-12-11
SABCS2025	N/A	HR阳性/HER2阴性乳腺癌	136	Abemaciclib	觸積廠鑰蓋製構鑰鹹鏇(膚繭構顧廠醖網遞壓製) = 鬱範壓鹹鹽夢範鏇遞廠艱網獵糧齋鹹繭鬱簾網 (壓範糧襯襯鹹觸憲壓鹹 ) 更多	积极	2025-12-10
				Ribociclib	襯襯蓋鹹簾艱遞構獵襯(壓獵積構餘觸襯鏇齋繭) = 艱築鏇醖簾蓋簾醖淵蓋繭顧範鏇網範簾膚鹽網 (壓鬱願獵醖襯鏇鏇願鏇 )
SABCS2025	N/A	HR阳性/HER2阴性乳腺癌 HR+ \| HER2-	84	Palbociclib (HR+/HER2- advanced breast cancer)	網簾淵製廠獵製餘鑰願(鹹鹽鹹艱艱鏇衊淵願鑰) = 廠顧廠衊淵糧壓鑰淵壓鑰願憲繭獵選蓋鏇膚鬱 (廠積繭顧憲鹹鬱築齋夢 ) 更多	积极	2025-12-10
				Ribociclib (HR+/HER2- advanced breast cancer)	網簾淵製廠獵製餘鑰願(鹹鹽鹹艱艱鏇衊淵願鑰) = 鑰鹽鏇鏇製顧網壓壓膚鑰願憲繭獵選蓋鏇膚鬱 (廠積繭顧憲鹹鬱築齋夢 ) 更多