Calquence Plus Chemoimmunotherapy Reduced the Risk of Disease Progression or Death by 27% Vs. Standard of Care in Patients With Untreated Mantle Cell Lymphoma in ECHO Phase III Trial
Calquence Plus Chemoimmunotherapy Reduced the Risk of Disease Progression or Death by 27% Vs. Standard of Care in Patients With Untreated Mantle Cell Lymphoma in ECHO Phase III Trial
First and only BTK inhibitor to demonstrate favourable overall survival
trend vs. standard-of-care chemoimmunotherapy in this setting
第一個也是唯一一個表現出良好總體存活率的 BTK 抑制劑
在這種環境下趨勢與標準護理化學免疫療法
Positive results from the ECHO Phase III trial showed AstraZeneca's Calquence (acalabrutinib) in combination with bendamustine and rituximab demonstrated a statistically significant and clinically meaningful improvement in progression-free survival (PFS) and showed a favourable trend in overall survival (OS) compared to standard-of-care chemoimmunotherapy (bendamustine plus rituximab) in previously untreated patients with mantle cell lymphoma (MCL).
ECHO三期試驗的陽性結果顯示阿斯利康的 Calquence (acalabrutinib)與苯達莫司汀和利妥昔單抗聯合使用在以前未接受治療的套細胞淋巴瘤(MCL)患者中,與標準護理化學免疫療法(苯達莫司汀加利妥昔單抗)相比,無進展存活率(PFS)有統計學意義且具有臨床意義的改善,並且與標準護理化學免疫療法(苯達莫司汀加利妥昔單抗)相比,總體存活率(OS)呈現出良好的趨勢。
These results will be presented today in a late-breaking oral presentation at the European Hematology Association (EHA) 2024 Hybrid Congress in Madrid, Spain (#LBA3439).
這些結果將於今天在西班牙馬德里舉行的歐洲血液學協會(EHA)2024年混合大會(#LBA3439)的最新口頭報告中公佈。
Results showed the Calquence combination regimen reduced the risk of disease progression or death by 27% compared to standard-of-care chemoimmunotherapy (hazard ratio [HR] 0.73; 95% confidence interval [CI] 0.57-0.94; p=0.016). Median PFS was 66.4 months for patients treated with the Calquence combination (n=299) versus 49.6 months with standard-of-care chemoimmunotherapy (n=299).
結果顯示 Calquence 與標準護理的化學免疫療法相比,聯合方案將疾病進展或死亡的風險降低了27%(危險比 [HR] 0.73;95% 置信區間 [CI] 0.57-0.94;p=0.016)。接受該治療的患者的PFS中位數爲66.4個月 Calquence 聯合療法(n=299)與標準護理化學免疫療法(n=299)的49.6個月對比。
The secondary endpoint of OS showed a favourable trend for the Calquence combination compared to standard-of-care chemoimmunotherapy, further supporting the clinical benefit of this combination (HR 0.86; 95% CI 0.65-1.13; p=0.2743). The OS data were not mature at the time of this analysis and the trial will continue to assess OS as a key secondary endpoint.
操作系統的次要端點顯示出有利的趨勢 Calquence 與標準護理化學免疫療法相比,組合進一步支持了該組合的臨床益處(HR 0.86;95% 置信區間0.65-1.13;p=0.2743)。在本次分析時,操作系統數據尚未成熟,該試驗將繼續評估操作系統作爲關鍵的次要終點。
The ECHO trial enrolled during the pandemic period, and a pre-specified analysis censoring for COVID-19-related deaths was conducted to assess the impact. PFS was further improved in both arms, with the Calquence combination reducing the risk of disease progression or death by 36% (HR 0.64; 95% CI; 0.48-0.84; p=0.0017). Median PFS was not reached among patients treated with the Calquence combination versus 61.6 months for standard-of-care chemoimmunotherapy (HR 0.64, 95% CI, 0.48-0.84; p=0.0017). A favourable trend was seen for OS in this analysis for the Calquence combination (HR 0.75; 95% CI 0.53-1.04; p=0.0797).
ECHO試驗是在大流行期間註冊的,並對與COVID-19相關的死亡進行了預先指定的分析審查,以評估其影響。兩個領域的PFS都得到了進一步改善, Calquence 組合可將疾病進展或死亡的風險降低36%(HR 0.64;95% 置信區間;0.48-0.84;p=0.0017)。在接受該治療的患者中,PFS中位數未達到 Calquence 標準護理化學免疫療法的組合對比爲61.6個月(HR 0.64,95% 置信區間,0.48-0.84;p=0.0017)。在這項分析中,操作系統呈現出有利的趨勢 Calquence 組合(HR 0.75;95% 置信區間0.53-1.04;p=0.0797)。
Michael Wang, MD, Puddin Clarke Endowed Professor, Director of Mantle Cell Lymphoma Program of Excellence, Co-Director of Clinical Trials at MD Anderson Cancer Center in Houston, US and principal investigator in the trial, said: "For people living with mantle cell lymphoma, a typically aggressive form of non-Hodgkin's lymphoma, the ECHO results offer promise of a new, effective treatment option for adults older than 65, who represent the majority of MCL patients. The improved progression-free survival seen in patients treated with the Calquence combination compared to chemoimmunotherapy demonstrate its potential to change the standard of care as the only BTK inhibitor in this first-line setting."
醫學博士、普丁·克拉克特許教授、套細胞淋巴瘤卓越項目主任、美國休斯敦MD 安德森癌症中心臨床試驗聯合主任、該試驗首席研究員王邁克爾說:“對於套細胞淋巴瘤(一種典型的侵襲性非霍奇金淋巴瘤)患者來說,ECHO的結果有望爲65歲以上的成年人提供一種新的、有效的治療選擇,他們代表大多數 MCL 患者。接受該療法治療的患者的無進展存活率得到改善 Calquence 與化學免疫療法相比,組合療法表明,作爲一線環境中唯一的BTK抑制劑,它有可能改變護理標準。”
Susan Galbraith, Executive Vice President, Oncology R&D, AstraZeneca, said: "The ECHO trial data demonstrate important progress in improving outcomes for patients with mantle cell lymphoma. The 16.8 months of additional time patients can live without their disease progressing is highly clinically meaningful, together with a trend to improvement in overall survival. We therefore believe Calquence plus chemoimmunotherapy will be an important new option for patients living with this disease."
阿斯利康腫瘤學研發執行副總裁蘇珊·加爾佈雷思說:“ECHO的試驗數據表明,在改善套細胞淋巴瘤患者預後方面取得了重要進展。患者可以在不進展的情況下延長16.8個月的存活時間,這具有很高的臨床意義,而且總體存活率也有改善的趨勢。因此,我們相信 Calquence 另外,化學免疫療法將是這種疾病患者的重要新選擇。”
Summary of Results: ECHO
結果摘要:ECHO
|
Calquence plus bendamustine and rituximab (n = 299) |
Placebo plus bendamustine and rituximab (n = 299) | |
|---|---|---|
|
Median PFS (months) |
Calquence plus bendamustine and rituximab (n = 299) 66.4 |
Placebo plus bendamustine and rituximab (n = 299) 49.6 |
|
PFS HR (95% CI) |
Calquence plus bendamustine and rituximab (n = 299) 0.73 (0.57-0.94) | |
|
PFS p-value |
Calquence plus bendamustine and rituximab (n = 299) 0.0160 | |
|
OS HR (95% CI) |
Calquence plus bendamustine and rituximab (n = 299) 0.86 (0.65-1.13) | |
|
OS p-value |
Calquence plus bendamustine and rituximab (n = 299) 0.2743 | |
|
Censoring for COVID-19 deaths | ||
|
Median PFS |
Calquence plus bendamustine and rituximab (n = 299) NR |
Placebo plus bendamustine and rituximab (n = 299) 61.6 |
|
PFS HR (95% CI) |
Calquence plus bendamustine and rituximab (n = 299) 0.64 (0.48-0.84) | |
|
PFS p-value |
Calquence plus bendamustine and rituximab (n = 299) 0.0017 | |
|
OS HR (95% CI) |
Calquence plus bendamustine and rituximab (n = 299) 0.75 (0.53-1.04) | |
|
OS p-value |
Calquence plus bendamustine and rituximab (n = 299) 0.0797 | |
|
Calquence 再加苯達莫司汀和利妥昔單抗 (n = 299) |
安慰劑加苯達莫司汀和利妥昔單抗 (n = 299) | |
|---|---|---|
|
PFS 中位數 (月) |
Calquence 再加苯達莫司汀和利妥昔單抗 (n = 299) 66.4 |
安慰劑加苯達莫司汀和利妥昔單抗 (n = 299) 49.6 |
|
PFS 小時(95% 置信區間) |
Calquence 再加苯達莫司汀和利妥昔單抗 (n = 299) 0.73 (0.57-0.94) | |
|
PFS p 值 |
Calquence 再加苯達莫司汀和利妥昔單抗 (n = 299) 0.0160 | |
|
OS HR(95% 置信區間) |
Calquence 再加苯達莫司汀和利妥昔單抗 (n = 299) 0.86 (0.65-1.13) | |
|
操作系統 p 值 |
Calquence 再加苯達莫司汀和利妥昔單抗 (n = 299) 0.2743 | |
|
審查 COVID-19 死亡人數 | ||
|
PFS 中位數 |
Calquence 再加苯達莫司汀和利妥昔單抗 (n = 299) NR |
安慰劑加苯達莫司汀和利妥昔單抗 (n = 299) 61.6 |
|
PFS 小時(95% 置信區間) |
Calquence 再加苯達莫司汀和利妥昔單抗 (n = 299) 0.64 (0.48-0.84) | |
|
PFS p 值 |
Calquence 再加苯達莫司汀和利妥昔單抗 (n = 299) 0.0017 | |
|
OS HR(95% 置信區間) |
Calquence 再加苯達莫司汀和利妥昔單抗 (n = 299) 0.75 (0.53-1.04) | |
|
操作系統 p 值 |
Calquence 再加苯達莫司汀和利妥昔單抗 (n = 299) 0.0797 | |
NR=Not reached
nr=未到達
The safety and tolerability of Calquence was consistent with its known safety profile, and no new safety signals were identified. Grade 3 or higher adverse events (AEs) due to any cause occurred in 88.9% (n=264) of patients treated with the Calquence combination and 88.2% (n=262) of patients treated with standard-of-care chemoimmunotherapy, including Grade 3 or higher atrial fibrillation in 3.7% (n=11) and 1.7% (n=5) of patients, Grade 3 or higher hypertension in 5.4% (n=16) and 8.4% (n=25), Grade 3 or higher major bleeding in 2.0% (n=6) and 3.4% (n=10), and Grade 3 or higher infections in 41.1% (n=122) and 34.0% (n=101), respectively. Serious AEs and Grade 5 events were balanced across arms (69% [n=205] versus 62% [n=184], and 12.1% [n=36] versus 10.1% [n=30], respectively). AEs leading to discontinuation were observed in 10.4% (n=31) and 6.4% (n=19) of patients for the Calquence combination and placebo arms respectively. AEs related to COVID-19 were seen in the trial, including Grade 5 events which occurred in 9.4% (n=28) of patients treated with the Calquence combination and 6.7% (n=20) of patients treated with standard-of-care chemoimmunotherapy.
的安全性和耐受性 Calquence 與其已知的安全特徵一致,沒有發現新的安全信號。在接受該治療的患者中,88.9%(n=264)發生因任何原因引起的3級或更高的不良事件(AE) Calquence 在接受標準護理化學免疫療法治療的患者中,有 88.2%(n=262)組合,包括 3.7%(n=11)和 1.7%(n=5)患者的 3 級或以上心房顫動,5.4%(n=16)和 8.4%(n=25)的 3 級或更高血壓,2.0%(n=6)和 3.4%(n=10)),三級或以上感染率分別爲41.1%(n = 122)和34.0%(n = 101)。嚴重的AE和5級事件在各臂之間保持平衡(分別爲69% [n = 205] 和62% [n = 184],12.1% [n = 36] 對10.1% [n = 30])。在10.4%(n=31)和6.4%(n=19)的患者中觀察到導致停藥的不良反應 Calquence 分別是組合和安慰劑組。試驗中發現了與 COVID-19 相關的不良事件,包括在 9.4%(n=28)接受該治療的患者中發生的 5 級事件 Calquence 聯合治療和接受標準護理化學免疫療法治療的患者的 6.7%(n=20)。
Additional AstraZeneca data at EHA
In addition to these compelling data, AstraZeneca data at EHA 2024 shows how the Company is advancing a diverse and innovative pipeline spanning multiple modalities including next-generation T cell engagers, cell therapy and antibody drug conjugates, to enable the creation of novel combination regimens across a range of blood cancers.
EHA的其他阿斯利康數據
除了這些令人信服的數據外,阿斯利康在EHA 2024上的數據還顯示了該公司如何推進涵蓋多種模式的多元化創新產品線,包括下一代T細胞結合劑、細胞療法和抗體藥物偶聯物,從而能夠針對一系列血液癌開發新的組合方案。
Results from the ongoing Phase I, dose-escalation trial of AZD0486, a novel CD19xCD3 T cell engager, showed durable responses in patients with heavily pretreated relapsed/refractory follicular lymphoma with a median follow up of 11 months. Complete response rates of 84% were seen at doses of AZD0486 of 2.4 mg and above. Data also showed how cytokine release syndrome (CRS) events were effectively mitigated by the double step-up dosing schedule and no immune effector cell-associated neurotoxicity syndrome (ICANS) events were observed.
正在進行的新型 CD19xCD3 T 細胞參與者 AZD0486 的 I 期劑量遞增試驗的結果顯示,經過大量預治療的復發/難治性濾泡淋巴瘤患者出現持久的反應,中位隨訪時間爲 11 個月。在 2.4 mg 及以上劑量的 AZD0486 劑量下,完全緩解率爲 84%。數據還顯示,加倍給藥計劃是如何有效緩解細胞因子釋放綜合徵(CRS)事件的,並且未觀察到免疫效應細胞相關神經毒性綜合徵(ICANS)事件。
In an oral presentation, preliminary data was shared from an investigator-initiated trial of AstraZeneca's first haematology cell therapy, GC012F (AZD0120), in patients with transplant-eligible high-risk, newly diagnosed multiple myeloma. Early results showed that GC012F had an overall response rate of 100%, a minimal residual disease-negative stringent complete response rate of 95%, and was well tolerated. Grade 1-2 CRS was experienced by 27% (6/22) of patients and no ICANS or neurotoxicity was observed. GC012F is a novel BCMAxCD19 dual-targeting autologous chimeric antigen receptor T therapy (CAR-T) created using the next-day FasTCAR manufacturing platform pioneered by Gracell Biotechnologies, a wholly owned subsidiary of AstraZeneca.
在口頭陳述中,分享了研究人員發起的阿斯利康首個血液學細胞療法 GC012F(AZD0120)試驗的初步數據,該試驗針對符合移植條件的高風險、新診斷的多發性骨髓瘤患者。早期結果顯示,GC012F 的總體緩解率爲 100%,殘留的疾病陰性嚴格完全緩解率爲 95%,並且耐受性良好。27%(6/22)的患者經歷了1-2級CRS,沒有觀察到ICANS或神經毒性。GC012F 是一種新型的bcmaxCD19雙靶向自體嵌合抗原受體T療法(CAR-T),使用阿斯利康全資子公司格雷賽爾生物技術公司首創的次日FastCar製造平台開發。
Notes
注意事項
Mantle cell lymphoma
MCL is a rare and typically aggressive form of non-Hodgkin lymphoma (NHL), often diagnosed as a late-stage disease, resulting when B-lymphocytes mutate into malignant cells within a region of the lymph node known as the mantle zone.1,2 While MCL patients initially respond to treatment, patients do tend to relapse.3 MCL comprises about 3-6% of non-Hodgkin lymphomas, with an annual incidence of 0.5 per 100,000 population in Western countries; in the US, it is estimated that approximately 4,000 new patients are diagnosed with MCL each year.3,4 It is estimated that there are more than 27,500 people living with MCL worldwide.5,6
套細胞淋巴瘤
MCL 是一種罕見且典型的侵襲性非霍奇金淋巴瘤 (NHL),通常被診斷爲晚期疾病,當 B 淋巴細胞在淋巴結的一個被稱爲地幔區的區域內突變爲惡性細胞時導致。1,2 雖然 MCL 患者最初會對治療產生反應,但患者往往會復發。3 MCL約佔非霍奇金淋巴瘤的3-6%,在西方國家,每10萬人口的年發病率爲0.5例;在美國,估計每年約有4,000名新患者被診斷出患有MCL。3,4 據估計,全球有超過27,500人患有MCL。5,6
ECHO
ECHO is a randomised, double-blind, placebo-controlled, multi-centre Phase III trial evaluating the efficacy and safety of Calquence plus bendamustine and rituximab compared to standard of care chemoimmunotherapy (bendamustine and rituximab) in adult patients at or over 65 years of age (n=635) with previously untreated MCL.7 Patients were randomised 1:1 to receive either Calquence or placebo administered orally twice per day, on 28 day treatment cycles, plus bendamustine on days 1 and 2 and rituximab on day 1 of each cycle. After six cycles of induction therapy, all patients continued Calquence or placebo in combination with bendamustine and rituximab, patients receive Calquence or placebo plus maintenance rituximab for two years and then either Calquence or placebo only until disease progression.7
回聲
ECHO 是一項隨機、雙盲、安慰劑對照、多中心 III 期試驗,旨在評估 Calquence 與標準治療化學免疫療法(苯達莫司汀和利妥昔單抗)相比,對65歲或以上(n=635)且以前未經治療的MCL的成年患者,加用苯達莫司汀和利妥昔單抗。7 患者以 1:1 的隨機分配,接受其中任一項 Calquence 或安慰劑,每天口服兩次,治療週期爲28天,在每個週期的第1天和第2天加上苯達莫司汀,在每個週期的第1天加上利妥昔單抗。經過六個週期的誘導治療,所有患者均繼續治療 Calquence 或安慰劑與苯達莫司汀和利妥昔單抗聯合使用,患者獲得 Calquence 或者安慰劑加維持利妥昔單抗兩年,然後要麼是 Calquence 或僅在疾病進展之前使用安慰劑。7
The primary endpoint is PFS assessed by an Independent Review Committee and key secondary endpoints include OS, overall response rate (ORR), duration of response (DoR) and time to response (TTR).7 The trial includes 27 countries across North and South America, Europe, Asia and Oceania.7
主要終點是獨立審查委員會評估的PFS,關鍵的次要終點包括操作系統、總響應率(ORR)、反應持續時間(DoR)和反應時間(TTR)。7 該試驗包括北美和南美、歐洲、亞洲和大洋洲的27個國家。7
The ECHO trial enrolled patients from May 2017 to March 2023, continuing through the COVID-19 pandemic. Patients with blood cancer remain at a disproportionately high risk of severe outcomes from COVID-19, including hospitalisation and death compared to the general population.8
ECHO 試驗從 2017 年 5 月到 2023 年 3 月招收了患者,一直持續到 COVID-19 大流行期間。與普通人群相比,血液癌患者出現 COVID-19 嚴重後果(包括住院和死亡)的風險仍然高得不成比例。8
Calquence
Calquence (acalabrutinib) is a next-generation, selective inhibitor of Bruton's tyrosine kinase (BTK). Calquence binds covalently to BTK, thereby inhibiting its activity.9 In B-cells, BTK signalling results in activation of pathways necessary for B-cell proliferation, trafficking, chemotaxis and adhesion.
Calquence
Calquence (acalabrutinib)是布魯頓酪氨酸激酶(BTK)的下一代選擇性抑制劑。 Calquence 與 BTK 共價結合,從而抑制其活性。9 在 B 細胞中,BTK 信號傳導可激活 B 細胞增殖、運輸、趨化性和粘附所需的途徑。
Calquence has been used to treat more than 80,000 patients worldwide and is approved for the treatment of CLL and small lymphocytic lymphoma (SLL) in the US and Japan, approved for CLL in the EU and many other countries worldwide and approved in China for relapsed or refractory CLL and SLL. Calquence is also approved in the US, China and several other countries for the treatment of adult patients with MCL who have received at least one prior therapy. Calquence is not currently approved for the treatment of MCL in Japan or the EU.
Calquence 已在全球範圍內用於治療80,000多名患者,在美國和日本獲准用於治療CLL和小淋巴細胞淋巴瘤(SLL),在歐盟和全球許多其他國家批准用於CLL,在中國批准用於復發或難治性CLL和SLL。 Calquence 美國、中國和其他幾個國家也批准用於治療先前至少接受過一次治療的成年MCL患者。 Calquence 目前未獲批准用於日本或歐盟的MCL治療。
As part of an extensive clinical development programme, Calquence is currently being evaluated as a single treatment and in combination with standard-of-care chemoimmunotherapy for patients with multiple B-cell blood cancers, including CLL, MCL, diffuse large B-cell lymphoma and follicular lymphoma.
作爲廣泛臨床開發計劃的一部分, Calquence 目前正在評估爲一種單一療法,並與標準護理化學免疫療法相結合,適用於多種B細胞血液癌患者,包括CLL、MCL、瀰漫性大B細胞淋巴瘤和濾泡性淋巴瘤。
AstraZeneca in haematology
AstraZeneca is pushing the boundaries of science to redefine care in haematology. Our goal is to help transform the lives of patients living with malignant, rare and other related haematologic diseases through innovative medicines and approaches that are shaped by insights from patients, caregivers and physicians.
阿斯利康在血液學中的應用
阿斯利康正在突破科學界限,重新定義血液學護理。我們的目標是通過以患者、護理人員和醫生的見解爲基礎的創新藥物和方法,幫助改變惡性、罕見和其他相關血液病患者的生活。
In addition to our marketed products, we are spearheading the development of novel therapies designed to target underlying drivers of disease across six scientific platforms. Our recent acquisitions of Alexion, with expertise in rare, non-malignant blood disorders, and Gracell Biotechnologies Inc., focused on cell therapies for haematologic malignancies, expand our haematology pipeline and enable us to reach more patients with high unmet needs through the end-to-end development and delivery of novel therapies.
除了已上市的產品外,我們還帶頭開發了旨在通過六個科學平台針對疾病潛在驅動因素的新療法。我們最近收購了擁有罕見非惡性血液疾病專業知識的Alexion和專注於血液系統惡性腫瘤細胞療法的Gracell Biotechnologies Inc.,擴大了我們的血液學產品線,使我們能夠通過端到端開發和交付新療法來接觸更多需求未得到滿足的患者。
AstraZeneca in oncology
AstraZeneca is leading a revolution in oncology with the ambition to provide cures for cancer in every form, following the science to understand cancer and all its complexities to discover, develop and deliver life-changing medicines to patients.
腫瘤學領域的阿斯利康
阿斯利康正在引領一場腫瘤學革命,其目標是爲各種形式的癌症提供治療方法,遵循科學來了解癌症及其所有複雜性,發現、開發並向患者提供改變生活的藥物。
The Company's focus is on some of the most challenging cancers. It is through persistent innovation that AstraZeneca has built one of the most diverse portfolios and pipelines in the industry, with the potential to catalyse changes in the practice of medicine and transform the patient experience.
該公司的重點是一些最具挑戰性的癌症。正是通過持續創新,阿斯利康建立了業內最多樣化的產品組合和管道之一,有可能催化醫學實踐的變革並改變患者體驗。
AstraZeneca has the vision to redefine cancer care and, one day, eliminate cancer as a cause of death.
阿斯利康的願景是重新定義癌症治療,並有朝一日消除癌症的死因。
AstraZeneca
AstraZeneca (LSE/STO/Nasdaq: AZN) is a global, science-led biopharmaceutical company that focuses on the discovery, development, and commercialisation of prescription medicines in Oncology, Rare Diseases, and BioPharmaceuticals, including Cardiovascular, Renal & Metabolism, and Respiratory & Immunology. Based in Cambridge, UK, AstraZeneca's innovative medicines are sold in more than 125 countries and used by millions of patients worldwide. Please visit astrazeneca.com and follow the Company on social media @AstraZeneca.
阿斯利康
阿斯利康(倫敦證券交易所/STO/納斯達克股票代碼:AZN)是一家以科學爲主導的全球生物製藥公司,專注於腫瘤學、罕見疾病和生物製藥(包括心血管、腎臟與代謝以及呼吸與免疫學)中處方藥的發現、開發和商業化。阿斯利康的創新藥物總部位於英國劍橋,銷往超過125個國家,全球有數百萬患者使用。請訪問 astrazeneca.com 並在社交媒體上關注該公司 @AstraZeneca.
References
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譯文內容由第三人軟體翻譯。