更新于：2024-11-01

KKLC1

更新于：2024-11-01

基本信息

别名

cancer/testis antigen 83、CT83、CXorf61

+ [5]

简介-

关联

项与 KKLC1 相关的药物

820-TCR

靶点

KKLC1

作用机制

KKLC1抑制剂 [+2]

在研机构

T-Cure Bioscience, Inc.初创企业 [+1]

原研机构

National Cancer Institute

在研适应症

乳腺癌 [+5]

非在研适应症-

最高研发阶段临床1期

首次获批国家/地区-

首次获批日期1800-01-20

821-TCR

靶点

HLA class I抗原 x KKLC1

作用机制

HLA class I抗原调节剂 [+1]

在研机构

T-Cure Bioscience, Inc.初创企业

原研机构

T-Cure Bioscience, Inc.初创企业

在研适应症

实体瘤

非在研适应症-

最高研发阶段临床前

首次获批国家/地区-

首次获批日期1800-01-20

ZI-KL1-1

靶点

KKLC1

作用机制

KKLC1抑制剂

在研机构

Zelluna Immunotherapy AS初创企业

原研机构

Zelluna Immunotherapy AS初创企业

在研适应症

乳腺癌 [+4]

非在研适应症-

最高研发阶段临床前

首次获批国家/地区-

首次获批日期1800-01-20

项与 KKLC1 相关的临床试验

NCT05035407 / Recruiting临床1期IIT

A Phase I Trial of T Cell Receptor Gene Therapy Targeting KK-LC-1 for Gastric, Breast, Cervical, Lung and Other KK-LC-1 Positive Epithelial Cancers

Background:
Researchers have found a new way to treat cancer using T cell therapy. The therapy used in this study is T Cell Receptor (TCR) Gene Therapy Targeting KK-LC-1, a cancer germline antigen that is expressed by certain cancers. This therapy is a type of treatment in which a participant s T cells (a type of immune system white blood cell) are changed in the laboratory to attack cancer cells and given back to the participant. This treatment might help people with KK-LC-1 positive cancers which may include gastric, breast, cervical, lung and other epithelial Cancers. Epithelial cancers are cancers that begin in the cells that line an organ.
Objective:
The purpose of this study is to determine the safety of different doses of KK-LC-1 TCR T cells plus aldesleukin to treat metastatic or refractory/recurrent KK-LC-1 positive cancers.
Eligibility:
Adults aged 18 and older with metastatic or refractory/recurrent KK-LC-1 positive epithelial cancer.
Design:
Participants will be screened with HLA typing (a blood test needed for eligibility) and KK-LC-1 testing of the cancer tumor (to determine if the cancer is KK-LC-1 positive). A new biopsy may be needed if tumor from an outside location is not available for KK-LC-1 testing. Eligible participants will come to the NIH campus to have a screening evaluation which will include physical exam, review of medical history and current medications, blood and heart tests, imaging (X-ray, CT scan, MRI or PET scan), and evaluation of participant s veins that are used for drawing blood.
If the participant is eligible for the study based on the screening evaluation, they will have a baseline evaluation prior to receiving the experimental treatment which may include additional laboratory or imaging tests.
Participants will have a large IV catheter inserted into a vein to undergo a procedure called leukapheresis. Leukapheresis is the removal of the blood by a machine to collect specific white blood cells. The remaining blood is returned to the body. This procedure is needed to collect the cells that will be modified to target the cancer. The cells are grown in the lab and given back to the participant through an injection into the participant's tumor. It takes 11-15 days to grow the cells.
While the cells are growing, the participant will be admitted to the hospital about one week
before the cell infusion to receive 2 types of chemotherapy through an IV catheter over 5 days. The main purpose of the chemotherapy is to make the cells more effective in fighting the cancer tumors. The cells will be given 1-2 days after the last dose of chemotherapy. Within 24 hours after the cell infusion, participants will be given a cell growth factor called aldesleukin through an IV for up to 4 days. Aldesleukin is thought to help the cells live longer in the participant s body. Participants will recover in the hospital until they are well enough to go home, which is usually about 7-12 days after the cell infusion or last dose of aldesleukin.
Participants will have a follow-up visit at approximately 40 days after the date of cell infusion. This visit will be to evaluate the safety of the cell therapy and the response of the cancer to the treatment which will include physical examination, lab tests, and imaging studies. If a participant has stable disease or their cancer has responded to the treatment, they will be seen again at 12 weeks post cell infusion, every 3 months x 3 visits, and then every 6 months x 5 years. If a participant s cancer progresses after this therapy, they will be return to their home doctor for further management.
After receiving cell therapy, participants will be followed on a long-term gene therapy protocol. Participants will have blood drawn periodically to test if the cells have grown or changed. These blood tests will take place immediately before the cells, and then at 3, 6, and 12 months for the first year and possibly annually thereafter based on the results. These tests can be drawn locally and sent to the NIH. After a participant is off the study, they will be contacted by telephone or mailed questionnaire for a total of 15 years after cell therapy....

开始日期2022-03-08

申办/合作机构

National Cancer Institute

ChiCTR2200057171 / Recruiting早期临床1期IIT

Efficacy and Safety of T Cell Receptor Modified T (TCR-T) Cells in Advanced Pancreatic Cancer, Lung Cancer and Colorectal Cancer Therapy

开始日期2022-03-01

申办/合作机构-

NCT03778814 / Recruiting临床1期IIT

TCR-T Cells Targeting Cancer Cells for Immunotherapy of Lung Cancer and Other Solid Tumors: Phase I Clinical Trial

Tumor organoids and TILs (and/or peripheral T cells) cultures will be established from fresh tissure of lung cancer and other solid tumors. Coculture will be utilized to screen tumor-responsive T cells which are further selected for monoclonal expansion and TCR cloning for engineered reconstitution of TCR-T cells. After verification by multiple in vitro and in vivo studies, a large number of TCR-T cells will be introduced back into the patients via vein, artery or fine needle punctured to the tumor, or combinations. In this phase I study, the safety, tolerance and preliminary efficacy of the TCR-T cell immunotherapy on human will firstly be assessed.

开始日期2018-12-01

申办/合作机构

广州医科大学附属第二医院

100 项与 KKLC1 相关的临床结果

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100 项与 KKLC1 相关的转化医学

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0 项与 KKLC1 相关的专利（医药）

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项与 KKLC1 相关的文献（医药）

2024-05-02·Oncogene

A novel bioinformatic approach reveals cooperation between Cancer/Testis genes in basal-like breast tumors

Article

作者: Okada, Yuki ; Ginestier, Christophe ; Cristofari, Gael ; Meseure, Didier ; Charafe-Jauffret, Emmanuelle ; Benlamara, Sarah ; Nicolas, André ; Vincent-Salomon, Anne ; Djerroudi, Lounes ; Ferry, Laure ; Laisné, Marthe ; Kirsh, Olivier ; Gupta, Nikhil ; Rodgers, Brianna ; Daher, Diana ; Defossez, Pierre-Antoine ; Wicinski, Julien ; Philippe, Claude

AbstractBreast cancer is the most prevalent type of cancer in women worldwide. Within breast tumors, the basal-like subtype has the worst prognosis, prompting the need for new tools to understand, detect, and treat these tumors. Certain germline-restricted genes show aberrant expression in tumors and are known as Cancer/Testis genes; their misexpression has diagnostic and therapeutic applications. Here we designed a new bioinformatic approach to examine Cancer/Testis gene misexpression in breast tumors. We identify several new markers in Luminal and HER-2 positive tumors, some of which predict response to chemotherapy. We then use machine learning to identify the two Cancer/Testis genes most associated with basal-like breast tumors: HORMAD1 and CT83. We show that these genes are expressed by tumor cells and not by the microenvironment, and that they are not expressed by normal breast progenitors; in other words, their activation occurs de novo. We find these genes are epigenetically repressed by DNA methylation, and that their activation upon DNA demethylation is irreversible, providing a memory of past epigenetic disturbances. Simultaneous expression of both genes in breast cells in vitro has a synergistic effect that increases stemness and activates a transcriptional profile also observed in double-positive tumors. Therefore, we reveal a functional cooperation between Cancer/Testis genes in basal breast tumors; these findings have consequences for the understanding, diagnosis, and therapy of the breast tumors with the worst outcomes.

2023-11-01·Journal of cancer research and clinical oncology

Expression of four cancer-testis antigens in TNBC indicating potential universal immunotherapeutic targets.

Article

作者: Liu, Baorui ; Li, Lin ; Xie, Li ; Xiao, Jie ; Zhang, Lianru ; Huang, Fengli

OBJECTIVEImmunotherapy is an attractive treatment for breast cancer. Cancer-testis antigens (CTAs) are potential targets for immunotherapy for their restricted expression. Here, we investigate the expression of CTAs in breast cancer and their value for prognosis. So as to hunt for a potential panel of CTAs for universal immunotherapeutic targets.MATERIAL AND METHODSA total of 137 breast cancer tissue specimens including 51 triple-negative breast cancer (TNBC) were assessed for MAGE-A4, MAGEA1, NY-ESO-1, KK-LC-1 and PRAME expression by immunohistochemistry. The expression of PD-L1 and TILs was also calculated and correlated with the five CTAs. Clinical data were collected to evaluate the CTA's value for prognosis. Data from the K-M plotter were used as a validation cohort.RESULTSThe expression of MAGE-A4, NY-ESO-1 and KK-LC-1 in TNBC was significantly higher than in non-TNBC (P = 0.012, P = 0.005, P < 0.001 respectively). 76.47% of TNBC expressed at least one of the five CTAs. Patients with positive expression of either MAGE-A4 or PRAME had a significantly extended disease-free survival (DFS). Data from the Kaplan-Meier plotter confirm our findings.CONCLUSIONSMAGE-A4, NY-ESO-1, PRAME and KK-LC-1 are overexpressed in breast cancer, especially in TNBC. Positive expression of MAGE-A4 or PARME may be associated with prolonged DFS. A panel of CTAs is attractive universal targets for immunotherapy.

2023-08-01·Journal for ImmunoTherapy of Cancer

Single-cell sequencing on CD8⁺TILs revealed the nature of exhausted T cells recognizing neoantigen and cancer/testis antigen in non-small cell lung cancer

Article

作者: Kishi, Hiroyuki ; Matsushita, Hirokazu ; Adachi, Katsutoshi ; Takahashi, Yusuke ; Doi, Kiyoshi ; Stratford, Richard ; Masago, Katsuhiro ; Fukuyama, Takashi ; Clancy, Trevor ; Miura, Daiki ; Demachi-Okamura, Ayako ; Shinohara, Shuichi ; Muraoka, Daisuke ; Hamana, Hiroshi ; Yamashita, Yoshiko ; Kuroda, Hiroaki ; Matsui, Takuya ; Watanabe, Fumiaki ; Nishida, Reina ; Sugita, Yusuke ; Fukushima, Yasunori ; Onoue, Kousuke ; Tanaka, Yuki ; Komuro, Hiroyasu ; Takashima, Chieko ; Onoguchi, Kazuhide ; Yamaguchi, Rui ; Iwata, Hisashi ; Ohki, Takashi ; Shigematsu, Yoshiki

BackgroundCD8+tumor infiltrating lymphocytes (TILs) are often observed in non-small cell lung cancers (NSCLC). However, the characteristics of CD8+TILs, especially T-cell populations specific for tumor antigens, remain poorly understood.MethodsHigh throughput single-cell RNA sequencing and single-cell T-cell receptor (TCR) sequencing were performed on CD8+TILs from three surgically-resected lung cancer specimens. Dimensional reduction for clustering was performed using Uniform Manifold Approximation and Projection. CD8+TIL TCR specific for the cancer/testis antigen KK-LC-1 and for predicted neoantigens were investigated. Differentially-expressed gene analysis, Gene Set Enrichment Analysis (GSEA) and single sample GSEA was performed to characterize antigen-specific T cells.ResultsA total of 6998 CD8+T cells was analyzed, divided into 10 clusters according to their gene expression profile. An exhausted T-cell (exhausted T (Tex)) cluster characterized by the expression ofENTPD1(CD39),TOX,PDCD1(PD1),HAVCR2(TIM3) and other genes, and by T-cell oligoclonality, was identified. The Tex TCR repertoire (Tex-TCRs) contained nine different TCR clonotypes recognizing five tumor antigens including a KK-LC-1 antigen and four neoantigens. By re-clustering the tumor antigen-specific T cells (n=140), it could be seen that the individual T-cell clonotypes were present on cells at different stages of differentiation and functional states even within the same Tex cluster. Stimulating these T cells with predicted cognate peptide indicated that TCR signal strength and subsequent T-cell proliferation and cytokine production was variable but always higher for neoantigens than KK-LC-1.ConclusionsOur approach focusing on T cells with an exhausted phenotype among CD8+TILs may facilitate the identification of tumor antigens and clarify the nature of the antigen-specific T cells to specify the promising immunotherapeutic targets in patients with NSCLC.

项与 KKLC1 相关的新闻（医药）

2024-07-03

·生物制品圈

看Octet如何把小分子互作“玩”出花样？（内含福利）

在生命科学研究领域，了解小分子与蛋白质之间的相互作用对于新药发现、疾病治疗及生物过程研究具有至关重要的意义。然而，这些应用往往因技术限制而充满挑战。基于生物层干涉（BLI）技术的Octet® 非标记分子互作系统具有高通量、高灵敏度、以及对DMSO等有机溶剂不敏感等优点，已成为小分子药物开发过程中的中坚力量。近年来，应用Octet®发表的小分子互作相关文章已经占到国内文献的1/3左右，且不仅有量，更加有质！现在，就让我们一同欣赏这些小分子研究的精彩成果，感受Octet®技术在揭示分子奥秘方面的卓越成就。 Science 脂肪肝新靶点[1] 中国医学科学院基础医学研究所肝细胞脂肪代谢对预防非酒精性脂肪性肝病（NAFLD）和其他慢性代谢性疾病具有重要意义。中国医学科学院基础医学研究所黄波团队研究发现，糖原合成使用其中间代谢物尿苷二磷酸葡萄糖（UDPG）来拮抗脂肪生成，从而引导小鼠和人肝细胞将葡萄糖碳储存为糖原。在这项机制研究中，发现UDPG通过SLC35F5转运进入高尔基体后，诱导蛋白酶S1P的泛素化降解，从而阻断活性形式SREBP1c的生成，最终抑制脂肪酸的合成。通过Octet®对小鼠和人的脂肪酸合成过程中关键酶（S1P）与UDPG结合这一重要步骤进行了验证，并提供了结合的直观证据（图1）。而S1P突变后与UDPG结合能力变弱，脂肪合成增加（图2）。研究还利用Octet®检测点突变结合界面的氨基酸残基位点后的S1P与UDPG的结合，进一步验证S1P-UDPG复合物结构解析的结果。图1：通过SA传感器固化小鼠（a）和人（b）的S1P蛋白分别与不同浓度UDPG结合解离曲线图2：S1P蛋白关键氨基酸突变(N438A or T593A)后，小鼠（c-d）和人（e）S1P蛋白与不同浓度UDPG结合解离曲线原文大量Pulldown以及CO-IP数据，但作者仍选择用Octet®非标记分子互作系统来证明S1P与UDPG直接相互作用，可见Direct Binding是趋势。 Science子刊 Octet® 检测<100Da小分子[2][3] 山东大学硫化氢(H2S)是一种重要的内源性分子，具有抗氧化特性。山东大学娄红祥/常文强组发现基因Cys4编码胱硫氨酸β合成酶(CBS)，是白色念珠菌中主要的H2S合成酶。敲除Cys4基因的白色念珠菌导致低致病性，提示CBS是一个很有前途的抗真菌靶点。Aminooxy-acetic acid (AOA)是一种小分子CBS抑制剂，在口咽念珠菌病(OPC)小鼠模型中具有良好的疗效，提示CBS具有作为对抗真菌感染治疗靶点的潜力。该成果发表于Science子刊。图2. Octet® RED96结果：将Cys4固化在SSA传感器上，与AOA进行结合解离，发现AOA亲和力为55µM。该小分子分子量小于<100Da! 本研究中检测的氨基氧乙酸AOA 仅有91Da，通过Octet® 依然可以灵敏的检测出准确的结果。 Nature子刊小分子药物筛选[4] 中国医科大学盛京医院醛脱氢酶1（ALDH1）是乳腺癌症干细胞的标志物（BCSC），其酶活性调节肿瘤干性。识别控制ALDH+细胞的上游靶点可能抑制三阴性乳腺癌症TNBC肿瘤。本文发现KK-LC-1细胞通过与FAT1结合并随后促进其泛素化决定了TNBC ALDH+的干性。采用计算和Octet® 互作筛选的方法，发现Z8398787730（Z8）作为一个小分子可以结合KK-LC-1，通过激活Hippo途径机制抑制TNBC肿瘤生长，并降低TNBC ALDH+细胞的干性和活力。这些发现确定了抑制ALDH+细胞中的KK-LC-1-FAT1-Hippo-ALDH1A1通路作为TNBC的潜在治疗手段TNBC肿瘤生长，并降低TNBC ALDH+细胞的干性和活力。这些发现确定了抑制ALDH+细胞中的KK-LC-1-FAT1-Hippo-ALDH1A1通路作为TNBC的潜在治疗手段。图2. (A) 用Octet® 单浓度筛选KK-LC-1抑制剂（145个）；(B) 用Octet® 进行Z8的多浓度亲和力测定，亲和力为4.3μM；(C) Z8的分子结构 Octet® 不仅可以用于小分子亲和力验证，由于其高通量和易学易用的特性，还可以用于小分子筛选。生物层干涉（BLI）技术可以实现对相互作用更加定量化地测定，非常适合亲和力比较低的化合物检测。在传统的方法中，化合物解离快、有洗涤等步骤，使得结合的小分子被洗掉后易产生假阴性结果；另外传统方法多数需要标记，可能会改变靶点分子的构象，也会产生假阳性结果。SPR技术容易受到溶剂效应影响，也不适合一些溶解性差的小分子。对比之下，生物层干涉（BLI）技术的非标记和实时检测可以克服传统方法的弊端，使得小分子相互作用检测结果更加真实可靠！ -参考文献- [1] Hepatic glycogenesis antagonizes lipogenesis by blocking S1P via UDPG.Science,2024 [2] Inhibition of fungal pathogenicity by targeting the H2Ssynthesizing enzyme cystathionine β-synthase. Sci. Adv. 8, eadd5366 (2022) [3] Science Advances | 山东大学娄红祥/常文强发现胱氨酸β-合成酶可作为对抗真菌感染的潜在治疗靶点 [4] KK-LC-1 as a therapeutic target to eliminate ALDH+ stem cells in triple negative breast cancer. Nature Communications | (2023) 14:2602

临床结果临床终止临床2期临床1期

2024-06-25

·PipelineReview

CDR-Life Announces Pipeline Expansion of Highly Tumor-Targeted T Cell Engagers

CDR813 and CDR505 programs further broaden pipeline of cancer-specific targeted therapies ZÜRICH, Switzerland I June 25, 2024 I CDR-Life Inc. today announced an expansion of its pipeline of novel T cell engagers (TCE) with the addition of CDR813 and CDR505. CDR813 is a highly potent and selective TCE candidate targeting tumors expressing PRAME (preferentially expressed antigen in melanoma) in HLA-A*02:01 patients. PRAME is a clinically validated pan-cancer target expressed in a broad set of tumors including non-small cell lung cancer (NSCLC), endometrial cancer, melanoma and ovarian cancer, but not in normal tissue. A bi-valent and bi-specific antibody-based TCE, CDR813 targets a PRAME peptide presented on tumor cells by the HLA-A*02 complex and the CD3 receptor on T-cells with unparalleled potency and specificity. CDR505 is a TCE targeting KK-LC-1, a novel HLA-A*01 target relevant in common cancer populations not yet addressed by other T cell receptor (TCR) therapeutics. While most TCE programs target the HLA-A02 haplotype, CDR505 targets KK-LC-1/HLA-A*01, expanding the potential of TCEs to benefit a large patient population with high unmet need. Preclinical data on CDR505 was presented at the American Association for Cancer Research (AACR) Annual Meeting in April 2024. “With our continued investment in building a broad pipeline of unique, potent and highly cancer-targeted therapies, we are expanding the promise of our differentiated T cell engager platform to treat a range of solid tumors,” said Christian Leisner, Ph.D., Chief Executive Officer at CDR-Life. “Importantly, the CDR813 and CDR505 programs are geared toward populations with significant unmet medical need, increasing our reach to benefit more patients.” About CDR-Life CDR-Life is developing powerful T-cell engagers (TCE) to eradicate hard-to-treat solid tumors. Our integrated antibody-based TCE platform unlocks access to a wide range of cancer antigens. We are leveraging this platform to advance a pipeline of potent and selective TCE therapeutics targeting intracellular and surface tumor antigens. With a team of proven drug development experts and backed by leading cross-Atlantic investors, we are working to empower patients’ own immune systems to eliminate tumors. SOURCE: CDR-Life

AACR会议

2024-05-07

·生物制品圈

BioNTech 2024年一季度业绩暴跌85%，计划年底前进行至少10项潜在的注册试验

2024年5月6日，BioNTech发布2024年第一季度业绩报告：总营收1.876亿欧元（约2.02亿美元），同比下降85%（2023年同期为12.7亿欧元，约14亿美元）；净亏损3.151亿欧元，而去年同期的净利润为5.022亿欧元。对于业绩暴跌，公司将其归咎于地方性COVID-19疫苗市场需求下降，销售前景低迷。不过，尽管第一季度收入急剧下降，但公司首席执行官Ugur Sahin在周一的声明中表示积极，转而关注BioNTech的产品线和即将到来的里程碑。Sahin表示：“在过去的几周里，我们报告了我们的个性化和现成的基于mRNA的候选药物的积极初步数据，”这进一步证明了公司核心技术的强大潜力。2024年，BioNTech计划开发一种适应变异株的COVID-19疫苗，并推进肿瘤学项目。公司在肿瘤学的策略是构建具有协同作用机制的化合物类的投资组合，包括免疫调节剂、靶向治疗以及个体化和现成的mRNA疫苗，涉及各类实体瘤和治疗阶段的项目。公司计划在2024年底前进行至少10项潜在的注册试验，并计划从2026年开始在肿瘤学领域进行第一波市场首次亮相。到2030年，公司预计将获得10个获批的癌症适应症。BioNTech首席财务官Jens Holstein表示，为了给这些潜在的批准和上市奠定基础，公司将在未来几年内扩大其业务，以实现“肿瘤学的商业准备”。今年3月，该公司任命了新的首席商务官Annemarie Hanekamp，其将于7月1日接替现任首席营销官兼首席商务官Sean Marett。此外，BioNTech还任命了一位美国总经理，他已经“开始在该国建立商业运营”。具体来说，公司在肿瘤学的管线亮点包括ADC药物，如BNT323/DB-1303、BNT325/DB-1305及BNT326/YL202；双特异性候选抗体BNT311/GEN1046（acasunlimab）、抗VEGF-A候选抗体BNT327/PM8002；癌症候选疫苗BNT116、BNT122；细胞治疗项目BNT211。BNT116是一种静脉注射的基于mRNA-LNP的癌症疫苗，由六种编码NSCLC中经常表达的肿瘤相关抗原（TAA）的mRNA（MAGE A3、CLDN6、KK-LC-1、PRAME、MAGE A4、MAGE C1）组成。该疫苗一项随机对照2期临床试验（NCT05557591）正在进行中，以评估BNT116联合cemiplimab与单独使用cemiplimab作为晚期NSCLC患者的一线治疗。另外，BNT116的1期试验初步结果在今年4月的AACR年会上公布了。BNT122是一种个体化的新抗原特异性免疫疗法（iNeST），是由BioNTech与罗氏集团成员基因泰克公司合作开发。其目前正在进行4项临床试验，分别用于治疗晚期黑色素瘤、辅助治疗结直肠癌、治疗实体瘤和辅助治疗胰腺导管腺癌。展望今年全年，BioNTech预计集团总收入在25亿欧元（27亿美元）至31亿欧元（33亿美元）之间。公司表示，几乎所有预期的2024年收入都将在年底到来。参考资料：[1]BioNTech Misses Q1 Earnings, Revenue on Lower COVID-19 Sales.BioSpace.Published: May 06, 2024 By Tristan Manalac.[2]BioNTech plots first wave of cancer launches in 2026 as COVID vaccine sales continue to disappoint.Fierce pharma.By Fraiser KansteinerMay 6, 2024 10:44am.[3]BioNTech 2024年一季报材料.识别微信二维码，添加生物制品圈小编，符合条件者即可加入生物制品微信群！请注明：姓名+研究方向！版权声明本公众号所有转载文章系出于传递更多信息之目的，且明确注明来源和作者，不希望被转载的媒体或个人可与我们联系(cbplib@163.com)，我们将立即进行删除处理。所有文章仅代表作者观点，不代表本站立场。

疫苗财报信使RNA免疫疗法AACR会议