更新于：2024-11-14

Human papillomavirus quadrivalent (types 6, 11, 16, 18) vaccine, recombinant(Emmanuel College, University of Queensland)

四价人乳头瘤病毒疫苗（酿酒酵母）

更新于：2024-11-14

概要

概要

基本信息

药物类型

病毒样颗粒疫苗、预防性疫苗、多价疫苗

+ [1]

别名

Human papillomavirus (types 6, 11, 16, 18) L1 virus-like particle vaccine、Human papillomavirus (types 6, 11, 16, 18) L1 VLP vaccine、Human papillomavirus quadrivalent (types 6, 11, 16, 18) recombinant vaccine

+ [13]

靶点-

作用机制-

治疗领域

肿瘤感染消化系统疾病+ [2]

在研适应症

肛门癌前病变乳头状瘤病毒感染HPV相关癌症+ [10]

非在研适应症

急性缺血性卒中白喉脊髓灰质炎+ [6]

原研机构

Emmanuel College, University of Queensland

在研机构

Merck Sharp & Dohme Corp.Merck Sharp & Dohme BVMerck Sharp & Dohme LLC

+ [1]

非在研机构

Merck Sharp & Dohme Ireland Ltd.

SK bioscience Co., Ltd.

最高研发阶段批准上市

首次获批日期

美国 (2006-06-08),

乳头状瘤病毒感染

最高研发阶段(中国)批准上市

特殊审评-

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关联

103

项与四价人乳头瘤病毒疫苗（酿酒酵母）相关的临床试验

NCT06650956 / Not yet recruitingN/AIIT

Integrated Service Delivery to Improve Adolescent Health and HPV Vaccination in Lao PDR: a Quasi-Experimental Mixed-Methods Study

The goal of this study is to find out if adding HPV vaccination to adolescent health services works to increase HPV vaccine uptake in 10-13-year-old girls in Laos. The study will also look at the effects of adding HPV vaccination on the use of other health services in 10-13-year-old boys and girls.
The main questions the study aims to answer are:
1. Does adding HPV vaccination to adolescent health services increase HPV vaccine uptake in girls aged 10-13 years compared to girls who only receive standard HPV vaccination services?
2. Does adding HPV vaccination to adolescent health services increase the use of other health services in 10-13-year-old adolescent boys and girls compared to adolescents who only receive standard HPV vaccination services?
3. What are the barriers and facilitators to using the combined intervention in Laos?
4. What are the opinions of adolescents, caregivers, healthcare providers, and other stakeholders on the combined intervention?
5. How much does it cost and how well it works to combine HPV vaccination with adolescent health services, as opposed to providing HPV vaccination alone?
Researchers will compare a combined intervention to standard HPV vaccination services to see if the combined intervention works to increase HPV vaccination uptake and the use of other health services. The combined intervention includes HPV vaccination given at schools, health facilities, and through community outreach. It also includes education on sexual and reproductive health, counseling, and other health services. Participants in the combined intervention group will:
1. Receive the HPV vaccine at school or at a health facility.
2. Take part in group discussions about sexual and reproductive health.
3. Take part in individual counseling sessions.
4. Use other health services as needed.
Participants in the comparison group will receive standard HPV vaccination services, including:
• HPV vaccination given at schools, health facilities, and through community outreach.

开始日期2024-11-01

申办/合作机构

Health Ltd.

[+1]

CTRI/2024/08/072040 / Not yet recruiting临床2期IIT

Antibody Response following One Dose of Cervavac® as compared to One Dose of Gardasil® Vaccine in Healthy Girls Aged 9-14 Years: A Non-inferiority, Multicenter, Double-blind, Randomized Controlled trial - Academic HPV Vaccine Trial

开始日期2024-08-30

申办/合作机构

Indian Council of Medical Research

TCTR20240825001 / Enrolling by invitation临床1期IIT

Immunogenicity of Quadrivalent Human Papillomavirus Vaccine in Adolescents after Hematopoietic Stem Cell Transplant: A Pilot Study

开始日期2024-07-25

申办/合作机构-

100 项与四价人乳头瘤病毒疫苗（酿酒酵母）相关的临床结果

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100 项与四价人乳头瘤病毒疫苗（酿酒酵母）相关的转化医学

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100 项与四价人乳头瘤病毒疫苗（酿酒酵母）相关的专利（医药）

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778

项与四价人乳头瘤病毒疫苗（酿酒酵母）相关的文献（医药）

2024-12-31·Human vaccines & immunotherapeutics

High impact of quadrivalent human papillomavirus vaccine across racial/ethnic groups: National Health and Nutrition Examination Survey, 2003–2006 and 2015–2018

Article

作者: Markowitz, Lauri E ; Unger, Elizabeth R ; Querec, Troy D ; Lewis, Rayleen M ; Stefanos, Ruth ; Gargano, Julia W

Human papillomavirus (HPV) causes cervical as well as other cancers. Racial and ethnic disparities in cervical cancer incidence and mortality in the United States are well documented. HPV vaccination has been recommended in the United States since 2006 and is expected to prevent HPV-attributable cancers in all racial/ethnic groups. Quadrivalent HPV vaccine-type (HPV6/11/16/18) and nonvaccine-type cervicovaginal HPV prevalences were estimated from National Health and Nutrition Examination Surveys in 2015-2018 (vaccine era) and 2003-2006 (prevaccine era) data. Prevalence ratios comparing 2015-2018 to 2003-2006 were calculated among sexually experienced Non-Hispanic White (NHW), Non-Hispanic Black (NHB), and Mexican American (MA) females aged 14-24 years. Quadrivalent HPV vaccine-type prevalence declined 82% (CI: 60%-92%) among NHW, 86% (CI: 64%-95%) among NHB, and 100% among MA females, forecasting future reductions in cervical cancer across racial/ethnic groups.

2024-12-31·Human Vaccines & Immunotherapeutics

The 13-year long-term follow-up on the effectiveness and immunogenicity of the quadrivalent human papillomavirus vaccine in Chinese females vaccinated at 20–45 years of age

Article

作者: Xu, Xiaoqian ; Pan, Chenghao ; Wen, Tianmeng ; Qiao, Youlin ; Zhang, Xun ; Zhao, Fanghui ; Hu, Shangying ; Zhao, Huan

TRIAL REGISTRATION:

The LTFU study was registered at the Chinese Clinical Trial Registry, ChiCTR2100052313.

2024-11-01·Lancet Global Health

The effect of BCG revaccination on the response to unrelated vaccines in urban Ugandan adolescents (POPVAC C): an open-label, randomised controlled trial

Article

作者: Serubanja, Joel ; van Dam, Govert J ; Webb, Emily L ; Kakande, Ayoub ; Kaleebu, Pontiano ; Natukunda, Agnes ; Kabali, Joel ; Nassuuna, Jacent ; Zirimenya, Ludoviko ; Kabagenyi, Joyce ; Kukundakwe, Christine ; Kiwudhu, Fred ; Nkurunungi, Gyaviira ; Namusobya, Loyce ; Oduru, Gloria ; Mutebe, Alex ; Apule, Barbara ; Kabuubi, Prossy N ; Akello, Florence A ; Sewankambo, Moses ; Kizindo, Robert ; Katushabe, Charity ; Ninsiima, Caroline ; Kizza, Moses ; Walusimbi, Bridgious ; Nayebare, Doreen ; Akello, Mirriam ; Kiwanuka, Samuel ; Elliott, Alison M ; Akurut, Hellen ; Nkangi, Ronald ; Nassanga, Beatrice ; Driciru, Emmanuella ; Wajja, Anne ; Kayiwa, John ; Nankabirwa, Christine ; Namutebi, Milly ; Onen, Caroline ; Amongi, Susan ; Cose, Stephen ; Kabami, Grace ; Nyanzi, Ruth ; Amongin, Rebecca ; Tumusiime, Josephine ; Zziwa, Christopher ; Nakazibwe, Esther ; Tumwesige, Pius ; Nsubuga, Denis ; Corstjens, Paul L A M

BACKGROUND:

Immune responses induced by several important vaccines differ between populations, with reduced responses in low-income and rural settings compared with high-income and urban settings. BCG immunisation boosts immune responses to some unrelated vaccines in high-income populations. We aimed to test the hypothesis that BCG revaccination can enhance responses to unrelated vaccines in Ugandan schoolchildren.

METHODS:

We conducted an open-label, randomised controlled trial to compare the effects of BCG revaccination versus no BCG revaccination on the immunogenicity of subsequent unrelated vaccines among adolescents aged 13-17 years who are participants in an urban Ugandan birth cohort study, in which BCG vaccination was documented at birth. Participants were excluded if they had received any of the trial vaccines or related agents when aged 5 years or older. Computer-generated 1:1 randomisation was implemented in REDCap. Participants were excluded if they were concurrently enrolled in other trials; had a clinically significant history of immunodeficiency, or serious psychiatric conditions or moderate to severe acute illnesses; were taking immunosuppressive medications; had allergies to vaccine components, a predisposition towards developing keloid scarring; positive HIV tests or pregnancy tests; were female participants who were lactating; or if they planned to use investigational drugs, vaccines, blood products, or any combination thereof. Trial participants assigned to the BCG revaccination group received the live parenteral BCG-Russia vaccine (Serum Institute of India, Pune, India; 0·1 mL intradermally, right upper arm) at week 0. All participants received yellow fever vaccine (YF-17D; Sanofi Pasteur, Lyon, France; 0·5 mL intramuscularly, left upper arm), live oral typhoid vaccine (Ty21a; PaxVax, London, UK; one capsule per day taken for three alternate days), and quadrivalent virus-like particle human papillomavirus (HPV) vaccine (Merck, Rahway, NJ, USA; 0·5 mL intramuscularly, left upper arm) at week 4; and toxoid vaccines (tetanus-diphtheria; Serum Institute of India; 0·5 mL intramuscularly, left upper arm) and an HPV booster at week 28. An additional HPV vaccination at week 8 was provided to female participants older than 14 years who had not previously been vaccinated. The primary outcomes were yellow fever neutralising antibody titres at 4 weeks post-YF-17D vaccination, Salmonella enterica serovar Typhi (henceforth S Typhi) O-lipopolysaccharide (O:LPS)-specific IgG concentration at 4 weeks post-Ty21a vaccination, and HPV-16 and HPV-18 L1 protein-specific IgG concentration at 4 weeks post-HPV vaccination. Primary outcome assays were conducted at week 8, and at week 52 for tetanus-diphtheria. We conducted an intention-to-treat analysis comparing log-transformed outcomes between trial groups, with results back-transformed to geometric mean ratios (GMRs). The safety population comprised all randomly allocated participants. The trial was registered at the ISRCTN Registry (ISRCTN10482904) and is complete.

FINDINGS:

Between Aug 31 and Oct 12, 2020, we screened 376 potential participants for eligibility. We enrolled and randomly allocated 300 participants to the two groups (151 [50%] to the BCG group and 149 [50%] to the no BCG group). 178 (59%) of 300 participants were male and 122 (41%) were female. 142 (91%) of 151 participants in the BCG group and 139 (93%) of 149 in the no BCG group completed follow-up. There was no effect of BCG revaccination, compared with no BCG revaccination, on the response observed for any vaccine. Yellow fever plaque reduction neutralising reference tests (PRNT₅₀) titres (the reciprocal of the last plasma dilution that reduced by 50%) had a GMR of 0·95 (95% CI 0·75-1·19; p=0·62) and PRNT₉₀ (reciprocal of the last plasma dilution that reduced by 90%) had a GMR of 0·94 (0·74-1·19; p=0·60); IgG to S Typhi O:LPS was 0·99 (0·80-1·23; p=0·94); IgG to HPV-16 was 0·97 (0·69-1·35; p=0·85) and to HPV-18 was 1·03 (0·76-1·40; p=0·83); and toxoid-specific IgG for tetanus was 1·13 (0·87-1·47; p=0·36) and was 1·00 (0·87-1·16; p=0·97) for diphtheria. There were no serious adverse events in either group.

INTERPRETATION:

We found no evidence that BCG revaccination is an effective strategy to improve immunogenicity of other vaccines in this low-income, urban setting.

FUNDING:

UK Medical Research Council.

TRANSLATION:

For the Luganda translation of the abstract see Supplementary Materials section.

380

项与四价人乳头瘤病毒疫苗（酿酒酵母）相关的新闻（医药）

2024-11-12

·Merck

Merck to Present New Data From GARDASIL®9 Studies Reinforcing the Importance of Gender-Neutral HPV Vaccination in Adults Up to Age 45 at the International Papillomavirus Conference (IPVC) 2024

November 12, 2024 3:00 am ET RAHWAY, N.J.--(BUSINESS WIRE)-- Merck (NYSE: MRK), known as MSD outside of the United States and Canada, today announced that new clinical and real-world data for the company’s 9-valent Human Papillomavirus (HPV) vaccine, GARDASIL ® 9 (Human Papillomavirus 9-valent Vaccine, Recombinant), evaluating the burden and incidence of certain HPV-related cancers and diseases, will be presented at the International Papillomavirus Conference (IPVC) 2024 in Edinburgh, UK, from November 12-15. Data to be presented include results from the BROADEN and PROGRESS studies evaluating the prevalence of oral HPV infection and burden of HPV-related oropharyngeal and other head and neck cancers, as well as studies evaluating the age of disease-causal HPV infection among females and highlighting the importance of protecting both females and males from HPV-related cancers and diseases through vaccination. “These data support the value of adult vaccination and strengthen our understanding that disease-causal HPV infection can happen later in life, reinforcing the importance of HPV vaccination for both females and males beginning at age 9,” said Dr. Eliav Barr, senior vice president, head of global clinical development and chief medical officer, Merck Research Laboratories. “While historically the HPV vaccination conversation has focused on preventing certain HPV-related cervical cancers in women, we also continue to see the growing incidence of HPV-related oropharyngeal and other head and neck cancers, particularly in men. In both men and women globally, there are approximately 666,000 new diagnoses of certain HPV-related cancers annually. The breadth of data we are presenting at the conference continues to demonstrate the link between HPV and certain HPV-related cancers in males and females and the role HPV vaccination can play in prevention.” Details on key abstracts for Merck: New Data Analyses of HPV-Related Cancers and Diseases in Women and Men Abstract Title Details Immunogenicity Of 9-Valent HPV (9VHPV) Vaccine In Male Clinical Trial Participants: A Post-Hoc Analysis By Baseline Demographic Characteristics. A. Luxembourg. ID #2172. TOPIC AS02: CLINICAL RESEARCH. CLINICAL SCIENCE ORAL ABSTRACT SESSION 05: HPV VACCINES Sequential Human Papillomavirus Infection Between Anogenital Anatomical Sites In Men. G. Nahhas. Poster #230. Session: 1 Estimating The Age of Acquisition of Disease-Causal HPV Infection Onset In Women Who Develop CIN2+ In England. K. Engelbrecht. Poster #209. Session: 1 Estimating The Age Of Disease-Causal HPV Infection Based On The Natural History Of CIN2+ Among Females In Canada. A. Cherif. Poster #219. Session: 2 Data Assessing Burden of Oral HPV Infection and HPV-Related Head and Neck Cancers in Men and Women Abstract Title Details Oral Human Papillomavirus Prevalence And Genotyping Among Adults In The United Kingdom – PROGRESS Study. O. Ovcinnikova. Poster #229. Session: 1 Oral Human Papillomavirus Incidence Among A General Adult Population In The US: Results From The PROGRESS (Prevalence Of Oral HPV Infection, A Global Assessment) Study. M. Felsher. Poster #228. Session: 1 Preliminary Results Of The BROADEN Study: Burden Of Human Papillomavirus-Related Head And Neck Cancers. T. Waterboer. ID#1292. TOPIC AS03: PUBLIC HEALTH, EPIDEMIOLOGY AND IMPLEMENTATION SCIENCE. ORAL ABSTRACTS SESSION 01: HPV AND HPV-DRIVEN CANCER IN THE HEAD AND NECK The BROADEN-China Study: Increasing Burden of Human Papillomavirus-Related Head and Neck Cancers in China. S. Zhang. ID#2397. TOPIC AS03: PUBLIC HEALTH, EPIDEMIOLOGY AND IMPLEMENTATION SCIENCE. ORAL ABSTRACTS SESSION: PUBLIC HEALTH LATE BREAKING ORAL ABSTRACTS Indication for GARDASIL 9 GARDASIL 9 is a vaccine indicated in females 9 through 45 years of age for the prevention of cervical, vulvar, vaginal, anal, oropharyngeal and other head and neck cancers caused by human papillomavirus (HPV) Types 16, 18, 31, 33, 45, 52, and 58; cervical, vulvar, vaginal, and anal precancerous or dysplastic lesions caused by HPV Types 6, 11, 16, 18, 31, 33, 45, 52, and 58; and genital warts caused by HPV Types 6 and 11 . GARDASIL 9 is indicated in males 9 through 45 years of age for the prevention of anal, oropharyngeal and other head and neck cancers caused by HPV Types 16, 18, 31, 33, 45, 52, and 58; anal precancerous or dysplastic lesions caused by HPV Types 6, 11, 16, 18, 31, 33, 45, 52, and 58; and genital warts caused by HPV Types 6 and 11. The oropharyngeal and head and neck cancer indication is approved under accelerated approval based on effectiveness in preventing HPV-related anogenital disease. Continued approval for this indication may be contingent upon verification and description of clinical benefit in a confirmatory trial. GARDASIL 9 does not eliminate the necessity for vaccine recipients to undergo screening for cervical, vulvar, vaginal, anal, oropharyngeal and other head and neck cancers as recommended by a health care provider. GARDASIL 9 has not been demonstrated to provide protection against diseases caused by: - HPV types not covered by the vaccine - HPV types to which a person has previously been exposed through sexual activity Not all vulvar, vaginal, anal, oropharyngeal and other head and neck cancers are caused by HPV, and GARDASIL 9 protects only against those vulvar, vaginal, anal, oropharyngeal and other head and neck cancers caused by HPV Types 16, 18, 31, 33, 45, 52, and 58. GARDASIL 9 is not a treatment for external genital lesions; cervical, vulvar, vaginal, anal, oropharyngeal and other head and neck cancers; or cervical intraepithelial neoplasia (CIN), vulvar intraepithelial neoplasia (VIN), vaginal intraepithelial neoplasia (VaIN), or anal intraepithelial neoplasia (AIN). Vaccination with GARDASIL 9 may not result in protection in all vaccine recipients Select Safety Information for GARDASIL 9 GARDASIL 9 is contraindicated in individuals with hypersensitivity, including severe allergic reactions to yeast, or after a previous dose of GARDASIL 9 or GARDASIL® [Human Papillomavirus Quadrivalent (Types 6, 11, 16, and 18) Vaccine, Recombinant]. Because vaccinees may develop syncope, sometimes resulting in falling with injury, observation for 15 minutes after administration is recommended. Syncope, sometimes associated with tonic-clonic movements and other seizure-like activity, has been reported following HPV vaccination. When syncope is associated with tonic-clonic movements, the activity is usually transient and typically responds to restoring cerebral perfusion. Safety and effectiveness of GARDASIL 9 have not been established in pregnant women. The most common (≥10%) local and systemic adverse reactions in females were injection-site pain, swelling, erythema, and headache. The most common (≥10%) local and systemic reactions in males were injection-site pain, swelling, and erythema. The duration of immunity of a 2-dose schedule of GARDASIL 9 has not been established. Dosage and Administration GARDASIL 9 should be administered intramuscularly in the deltoid or anterolateral area of the thigh. For individuals 9 through 14 years of age, GARDASIL 9 can be administered using a 2-dose or 3-dose schedule. For the 2-dose schedule, the second dose should be administered 6–12 months after the first dose. If the second dose is administered less than 5 months after the first dose, a third dose should be given at least 4 months after the second dose. For the 3-dose schedule, GARDASIL 9 should be administered at 0, 2 months, and 6 months. For individuals 15 through 45 years of age, GARDASIL 9 is administered using a 3-dose schedule at 0, 2 months, and 6 months. About Merck At Merck, known as MSD outside of the United States and Canada, we are unified around our purpose: We use the power of leading-edge science to save and improve lives around the world. For more than 130 years, we have brought hope to humanity through the development of important medicines and vaccines. We aspire to be the premier research-intensive biopharmaceutical company in the world – and today, we are at the forefront of research to deliver innovative health solutions that advance the prevention and treatment of diseases in people and animals. We foster a diverse and inclusive global workforce and operate responsibly every day to enable a safe, sustainable and healthy future for all people and communities. For more information, visit www.merck.com and connect with us on X (formerly Twitter) , Facebook , Instagram , YouTube and LinkedIn . About Merck’s global commitment to supply and access to HPV vaccines Merck is committed to ensuring adequate global supply and supporting broader, equitable access to our HPV vaccines to help protect against certain HPV-related cancers and diseases. This commitment is enabled through significant capital investments, including more than $2 billion to help increase capacity through additional manufacturing facilities that allowed for a nearly doubling of supply of our HPV vaccines from 2017-2020 and then, supply was doubled again between 2020-2024 to address increasing global demand. As a result, we expect to supply sufficient quantities of our HPV vaccines to meet anticipated demand and will continue to expand supply capacity in the future. Global equitable access to our HPV vaccines is a key part of our efforts and key partnerships help us achieve these goals. In 2024, Merck reaffirmed its commitment to Gavi, the Vaccine Alliance, through an agreement with UNICEF, to supply low- and middle-income countries with over 115 million doses of HPV vaccine by 2025, to appropriately support local immunization programs. Merck has consistently increased our supply commitment to Gavi from 1.7 million doses in 2017 to more than 30 million doses in 2024. Additionally, we are working to ensure continued supply in countries with existing HPV vaccination programs and currently supply approximately 150 National Immunization Programs globally. Forward-Looking Statement of Merck & Co., Inc., Rahway, N.J., USA This news release of Merck & Co., Inc., Rahway, N.J., USA (the “company”) includes “forward-looking statements” within the meaning of the safe harbor provisions of the U.S. Private Securities Litigation Reform Act of 1995. These statements are based upon the current beliefs and expectations of the company’s management and are subject to significant risks and uncertainties. If underlying assumptions prove inaccurate or risks or uncertainties materialize, actual results may differ materially from those set forth in the forward-looking statements. Risks and uncertainties include but are not limited to, general industry conditions and competition; general economic factors, including interest rate and currency exchange rate fluctuations; the impact of pharmaceutical industry regulation and health care legislation in the United States and internationally; global trends toward health care cost containment; technological advances, new products and patents attained by competitors; challenges inherent in new product development, including obtaining regulatory approval; the company’s ability to accurately predict future market conditions; manufacturing difficulties or delays; financial instability of international economies and sovereign risk; dependence on the effectiveness of the company’s patents and other protections for innovative products; and the exposure to litigation, including patent litigation, and/or regulatory actions. The company undertakes no obligation to publicly update any forward-looking statement, whether as a result of new information, future events or otherwise. Additional factors that could cause results to differ materially from those described in the forward-looking statements can be found in the company’s Annual Report on Form 10-K for the year ended December 31, 2023 and the company’s other filings with the Securities and Exchange Commission (SEC) available at the SEC’s Internet site ( www.sec.gov ). Please see Prescribing Information for GARDASIL 9 (Human Papillomavirus 9-valent Vaccine, Recombinant) at https://www-merck-com.libproxy1.nus.edu.sg/product/usa/pi_circulars/g/gardasil_9/gardasil_9_pi.pdf a nd Patient Information/Medication Guide for GARDASIL 9 at https://www-merck-com.libproxy1.nus.edu.sg/product/usa/pi_circulars/g/gardasil_9/gardasil_9_ppi.pdf Media Contacts: Julie Cunningham +1 (617) 519-6264 Muchena Zigomo +1 (267) 309-5591 Investor Contacts: Peter Dannenbaum +1 (732) 594-1579 Damini Chokshi +1 (732) 594-1577 Source: Merck & Co., Inc.

疫苗上市批准加速审批

2024-11-07

·Endpoints

Soft RSV sales reveal a vaccine market failing to catch post-Covid momentum

Coming out of Covid, the vaccine market appeared to experience a renaissance as the innovations of the pandemic unleashed new products and a new impetus to prevent infections. But just a few years later, the sector is facing headwinds in China, a weakening market for RSV vaccines in the West, and an incoming White House that’s allied itself with a leading vaccine skeptic, Robert F. Kennedy Jr. Kennedy, a longtime anti-vaccine advocate, is expected to have a significant hand in the Trump administration’s drug and food policy, and the campaign has talked about having him lead a review of vaccine safety. That political development has spooked investors. On Wednesday morning, the day after the election, shares of major vaccine developers fell, including a 2.9% dip for GSK and 5% for Moderna. In the hours after the election, Kennedy said he doesn’t plan to try and take vaccines off the market — an idea that would be difficult in any case, given how the FDA functions. “If vaccines are working for somebody, I’m not going to take them away,” he told NBC News. “People ought to have choice and that choice ought to be informed by the best information.” But Kennedy’s possible elevation is almost certain to grow a trend of vaccine hesitancy in the US, which has seen some rates of childhood vaccination decline even before the Covid-19 pandemic disrupted some routine preventive healthcare. On Wednesday, in an interview at the Financial Times’ Global Pharma and Biotech Summit in London, GSK CEO Emma Walmsley said transparency is key to rebuilding faith in vaccines. “You don’t just shout, ‘Trust us,'” she said. “You bring the facts forward, and I hope science and truth will prevail.” The uncertainty over the Trump administration’s health policies comes amid trouble in China. Merck has wrestled with a broader corruption crackdown that’s put a damper on sales of Gardasil , and GSK said the economic slowdown there has impacted vaccine volumes. After a rapid launch of the RSV vaccines approved last year, this year has shown far weaker sales. Pfizer’s third-quarter sales dropped 5%, while GSK had a massive 73% decline compared to the third quarter of 2023. Moderna, which had its adult vaccine approved over the summer, reported just $10 million in revenue , well below the other two pharmas. The figures validate pessimism heading into the vaccination campaign after the CDC slightly narrowed its RSV recommendations over the summer , and executives at all three vaccine manufacturers pointed to the revised recommendations as impacting the market in the second season. Vaccine prescription data through the last week of October showed continued decline for both GSK and Pfizer's RSV shots, with roughly 1.5 million total inoculations, compared with four million through the same period in 2023, according to Jefferies. Moderna is capturing just 1% of the market share, leaving analysts to conclude that this year will be “negligible” for the company. And GSK adjusted its guidance for vaccine sales, expecting low single-digit decline in 2024 after originally forecasting low-to-mid single-digit growth. Moderna CEO Stéphane Bancel said Thursday that pharmacies and patients are prioritizing Covid and flu vaccines this fall, suggesting more RSV shots could come at the beginning of the new year. "I think it will be quite interesting to see what happens in Q1 potentially, and does the shape of a curve of RSV look different than what we saw in the previous season," he said. That the once-beaming RSV opportunity — which public health experts have hailed as a great breakthrough — could slide so quickly is alarming to vaccine makers and investors. Advisors to the CDC don’t seem to be itching to swiftly expand the recommended age groups either, holding firm on its new guidance when the Advisory Committee on Immunization Practices convened in October. There have been a few bright spots. Moderna on Thursday surprised investors by exceeding Covid-19 vaccine sales estimates for the third quarter and posting a profit. Bancel said that earlier FDA approval of the updated vaccines allowed the company to better meet demand. And Pfizer is seeing stabilizing demand for their Covid-19 shots. CEO Albert Bourla told investors recently that he expects the company will stop segmenting out its Covid business, equipped with a more sure sense of demand moving forward. "We will stop separating our business to Covid/non-Covid because it's Pfizer business," he said.

疫苗

2024-11-07

·生物制品圈

癌症疫苗佐剂在临床试验中的比较

摘要：癌症治疗在提高总体生存率方面取得了长足进步；然而，逃避免疫系统继续是治疗已建立疾病负担个体的挑战。由于刺激对癌症的免疫反应存在困难，可能需要使用具有不同机制的组合佐剂。这些佐剂与其他佐剂或其他治疗的组合已显示出协同效应，以强大和持久的免疫反应的形式，证明了进一步发展的重要性。本综述讨论了免疫逃逸的复杂性，具有不同作用机制的佐剂的应用，以及临床试验中用于癌症免疫疗法的佐剂。 1、引言佐剂是现代时代疫苗的重要组成部分，并已成功用于增强针对疫苗特异性抗原的先天和适应性免疫反应。总体而言，佐剂可分为传递系统和免疫刺激剂。传递系统可以是微粒、脂质颗粒到乳液。相比之下，免疫刺激剂是来自病原体的成分，如CpG DNA和脂多糖。许多颗粒传递系统模仿病原体的大小和组成，并被抗原呈递细胞吞噬，导致MHC呈递和细胞/体液免疫的激活。而免疫刺激剂通过模式识别受体（PRRs）靶向各种信号通路。PRRs包括一系列Toll样受体（TLRs）、视黄酸诱导基因I样受体（RLRs）和寡聚化结构域样受体（NLRs）。这些信号通路的激活导致增强的先天免疫反应和细胞因子释放。Apostolico等人提供了现有佐剂及其各自作用模式的总结。为了在临床上获得所需的免疫反应，已经评估了各种佐剂和佐剂的组合。除了有效性外，这些佐剂的安全性同样重要。佐剂可能导致局部和全身毒性，从给药部位发红到发热和恶心不等。此外，可能发生严重和罕见的免疫毒性问题，需要对佐剂和疫苗候选物进行彻底的临床评估。Petrovsky等人总结了与各种佐剂相关的毒性问题。这些佐剂支持一系列疫苗候选物。主要地，疫苗平台可分为非活性、减毒活、核苷酸基、类毒素、亚单位/重组/多糖疫苗和基于病毒载体的疫苗。根据抗原的免疫原性，疫苗候选物可能包含或不包含佐剂。针对流感、HPV、肺炎等的疫苗已从包含佐剂中受益。然而，水痘、麻疹/腮腺炎/风疹和脊髓灰质炎疫苗不包含任何佐剂。我们对疫苗和佐剂的大部分了解来自传染病模型。然而，正在进行大量研究以开发有佐剂的治疗性癌症疫苗。本综述将重点关注FDA批准的和正在评估用于治疗性癌症疫苗和组合免疫疗法的实验性佐剂。 1.1 佐剂日益增长的认识将佐剂用于增强疫苗的免疫反应被誉为疫苗研究中最重要的进展之一。铝盐，通常称为“Alum”，是第一种与疫苗一起使用的佐剂，至今仍是最常用的佐剂之一。Alum最初由Glenny等人在1926年在伦敦发现。20世纪80年代，随着重组DNA的出现，佐剂技术取得了进步，这标志着佐剂研究的开始。然而，仍有许多工作要做。直到1990年代，才批准了第一个使用非Alum佐剂的许可疫苗（Fluad）。随着癌症治疗中免疫疗法的兴起，正在研究各种佐剂，并且许多有佐剂的癌症疫苗目前正在临床开发中。其中一些佐剂已经获得了商业许可，如Poly-ICLC（Hiltonol）、Montanide ISA-51、Imiquimod和CpG ODN。Montanide ISA-51和Poly-ICLC已被用于研究目的，但尚未获得商业用途的人类使用批准。Imiquimod已获得FDA批准作为用于生殖器疣的局部乳膏。CpG 1018目前是FDA批准的商业疫苗Heplisav-B的一部分。 1.2 免疫系统的逃逸先天免疫系统在抗肿瘤免疫中起着至关重要的作用，通过推动坏死肿瘤细胞死亡。垂死的细胞表达损伤相关分子模式（DAMPs），吸引树突细胞，这些细胞最终成熟并刺激T细胞途径以消除更多的癌细胞。p53是一种肿瘤抑制基因，会在响应压力信号（例如，DAMPs和干扰素）时激活，有助于细胞凋亡、细胞周期停滞和细胞退化。在许多癌症中（约占所有人类癌症的50%，在晚期/更具侵略性的癌症中约占80%），p53突变可以克服这些免疫抑制机制并继续增殖，通常使它们对化疗产生抗性。了解不同逃逸途径背后的机制为癌症治疗中新靶点和治疗方法铺平了道路。在癌症中，免疫编辑包括三个不同的阶段：消除、平衡和逃逸。在消除期间，急性炎症刺激促炎细胞因子（例如，IL-12和IFN-γ）的释放，这触发免疫系统通过自然杀伤（NK）细胞、细胞毒性T细胞和巨噬细胞识别和摧毁癌前和恶性细胞。肿瘤细胞通过招募免疫抑制因子或减少免疫原性发展出抗性变体。一旦癌细胞无法被宿主的免疫系统识别和消除，就达到了最后阶段，逃逸，肿瘤进展发生。在这一逃逸阶段，从急性炎症过渡到慢性炎症，导致抑制性免疫检查点（例如，CTLA-4和PD-1）的上调。免疫抑制细胞的入侵，如调节性T细胞（Tregs）和肿瘤相关巨噬细胞（TAMs），以及免疫抑制细胞因子（例如，TGF-β和IL-10）的释放，形成了一个复杂的肿瘤微环境（TME），能够逃避免疫系统。 1.3 免疫检查点抑制剂当前的角色和局限性免疫检查点抑制剂(ICIs)已成为癌症免疫疗法的主流，为其化疗对应物提供了特异性，同时对许多肿瘤类型保持了广泛的活性。在许多情况下，ICIs已成为晚期和转移性疾病（例如，晚期胆道癌(BTC)和晚期肾细胞癌）的标准护理。它们在临床试验中显示出有希望的抗肿瘤效果，同时保持了可接受的安全性。当化疗和免疫检查点抑制剂联合使用时，会创造出协同效应，但最佳剂量和给药顺序存在变异性。大多数临床试验同时给予化学疗法和ICIs，但也有临床前和临床数据支持化疗诱导可以改变肿瘤微环境(TME)并优化其进行ICI治疗。目前，有三种联合疗法已被批准作为一线治疗，全部针对非小细胞肺癌(NSCLC)。这些包括(a)卡铂+紫杉醇+贝伐珠单抗+阿特珠单抗，(b)顺铂/卡铂+培美曲塞+帕博利珠单抗，和(c)卡铂+紫杉醇/白蛋白紫杉醇+帕博利珠单抗。然而，TME的改变可以促进免疫检查点抑制剂的抗性，并且所有癌症患者的临床结果并不一致。化疗和ICIs在免疫学上冷的肿瘤中的局限性，即缺乏T细胞浸润到肿瘤中，将需要替代方法，如治疗性疫苗。例如，在转移性去势抵抗性前列腺癌中，ICI的客观反应率在没有程序性细胞死亡配体1(PD-L1)的肿瘤患者中为3%，在表达PD-L1的肿瘤患者中为5%，而 sipuleucel-T(Provenge)在改善更大患者群体的总体生存方面更为有效。 1.4 预防性和治疗性疫苗预防性疫苗传统上被用来降低病原体感染的可能性或严重程度，而治疗性疫苗最近被探索用于免疫具有预先存在的免疫敏感状况的个体，以产生免疫反应，减少或根除预先存在的状况。自从铝盐首次引入以来，佐剂已被纳入季节性流感和儿童传染病的预防性疫苗中。最近，预防性疫苗的角色已扩展到由人乳头瘤病毒(HPV)和乙型肝炎病毒引起的癌症。佐剂被描述为主要表现为病原体相关分子模式(PAMPs)或损伤相关分子模式(DAMPs)，它们刺激上皮细胞和树突细胞的病原体识别受体(PRRs)。值得注意的是，单磷酸脂A(MPL)和胞嘧啶磷酸鸟苷(CpG)这些刺激Toll样受体(一种PRR)的佐剂已经包含在Cervarix™和Heplisav™等商业疫苗中。这些疫苗被认为是预防性的，因为它们预防了可能导致某种癌症的病毒感染。在Cervarix™的情况下，它可以预防与HPV 16型和18型相关的感染，是一种二价预防性疫苗。而Gardasil®(四价)和Gardasil® 9(九价)分别针对四种和九种不同的HPV类型。Gardasil®和Gardasil® 9都包含硫酸铝羟基磷酸盐作为佐剂。另一方面，基于蛋白质/肽的、核苷酸基的和活体载体基的疫苗正在进行临床评估，作为治疗性HPV疫苗。治疗性HPV疫苗使用念珠菌皮肤试验试剂或CpG 1826作为佐剂，以改善T细胞反应。相比之下，sipuleucel-T(Provenge™)、BCG Theracys™(TICE)和Talimogene Laherparepvec(T-vec™)被视为治疗性疫苗，因为它们试图减少相应癌症的转移性肿瘤的生长。与预防性疫苗类似，治疗性癌症疫苗使用佐剂来增强免疫反应，但使用患者特定的肿瘤抗原。图1提供了佐剂癌症疫苗作用机制的一般示意图。Sipuleucel-T由来自患者的自体外周血单核细胞(PBMCs)组成，这些细胞从患者体内取出，并使用一种重组融合蛋白PA2024在体外激活，该蛋白由前列腺抗原与粒细胞-巨噬细胞集落刺激因子(GM-CSF)融合而成[27] GM-CSF与前列腺抗原协同作用，通过激活患者的抗原呈递细胞(APCs)来识别它们的肿瘤细胞，从而增强免疫反应。与多西他赛(平均生存期：2-3个月)相比，Sipuleucel-T在延长总体生存方面是有效的(大约四个月)，但像多西他赛一样，它并不增加患有前列腺癌个体的无进展生存率。此外，评估Sipuleucel-T与安慰剂的所有III期试验都显示，总体生存延长了四个月，死亡风险降低了33%，并且与安慰剂相比，T细胞刺激的中位比率增加了八倍。Theracys™，另一种治疗性疫苗，自2009年以来一直作为非肌层浸润性膀胱癌治疗的重要组成部分。这种细菌衍生的佐剂最初被研究用于结核病的疫苗开发。从那时起，它在膀胱癌治疗中保持了有用的作用，并且由于不同的地区维持的“祖先”株BCG的不同菌株可能存在效力、效力和不良事件特征的差异。T-vec™是一种改良的溶瘤性单纯疱疹病毒，用于治疗黑色素瘤。经过工程改造的病毒对黑色素瘤具有高度特异性，并通过引发免疫反应来启动抗肿瘤作用。这种注射剂与编码GM-CSF的序列共同配方，以更好地将APCs招募到肿瘤部位。GM-CSF是一种细胞因子和已知的造血因子，它特别促进树突细胞的功能，并改善细胞毒性T细胞向肿瘤块的迁移。在这些治疗中，进一步推测疗效（定义为肿瘤块的减少和防止进一步转移）与肿瘤浸润性淋巴细胞的浓度强烈相关。图1. 带佐剂癌症疫苗作用机制的一般示意图 1.5 B细胞调节除了刺激抗原特异性的T细胞反应外，癌症疫苗也应该努力向B细胞呈现肿瘤特异性抗原，以产生抗体，实现持久的免疫。肿瘤浸润的B淋巴细胞已成为治疗靶点，帮助那些对T细胞靶向治疗（例如，免疫检查点抑制剂）无反应的患者。它们通过促进T细胞、产生免疫球蛋白，甚至直接杀死癌细胞来帮助减缓肿瘤进展。肿瘤浸润的B淋巴细胞还为三级淋巴结构提供了基础，这些结构允许细胞毒性T淋巴细胞的浸润和更好的患者结果。不同的佐剂可以帮助增强B细胞反应以增强体液免疫，或者针对患有B细胞淋巴瘤的患者的肿瘤特异性B细胞。癌细胞上的Toll样受体可以被触发以引起肿瘤抑制、凋亡、转移抑制和抗肿瘤免疫。例如，CpG ODN是一种Toll样受体(TLR) 9配体，可以因其表达TLR-9而导致恶性B细胞的细胞死亡。TLR-9在许多其他类型的癌症中（例如，前列腺、乳腺、肾细胞癌）过度表达，并且与无进展生存期减少和预后较差相关，使其成为一个很好的靶点。在一项针对表达NY-ESO-1的肿瘤患者的临床试验中，接受多聚IC（TLR-3配体）治疗的患者中有79%在接种疫苗后产生了NY-ESO-1特异性IgG。Toll样受体作为癌症疫苗的靶点在临床试验中显示出前景，因为它们利用了直接靶向癌细胞的能力，同时也激活了抗原呈递细胞(APCs)。 B细胞调节为佐剂在刺激适应性免疫中的作用提供了全面的视野。然而，这条途径在临床上实现期望的治疗反应方面发挥了边缘作用。佐剂的主要焦点仍然是增强细胞免疫并产生细胞毒性反应。 1.6 增强CD8+浸润随着像Provenge™这样的治疗性癌症疫苗的成功，研究人员已经应用了利用个体固有的免疫反应对抗其他癌症（如胰腺癌和乳腺癌）的原则。基本原理本质上是刺激专业的APCs成熟并通过主要组织相容性复合物(MHCs)呈现特定的肿瘤相关抗原。MHC-I呈现肿瘤相关抗原会产生激活CD8+ T细胞并迁移到肿瘤部位的反应，这些反应在有佐剂存在时会增强。在激活CD8+ T细胞方面有效的佐剂包括GM-CSF、PolyIC、咪喹莫特、CpG寡脱氧核苷酸和皂苷（例如，ISCOMATRIX）。治疗前CD8+ T细胞的浸润是某些类型癌症（例如，基底样乳腺癌）的一个有利的预后指标，并且与更好的总体生存相关。然而，患者需要CD8+ T细胞存在于肿瘤内，这些治疗才能有效。此外，尝试向患者输注这些T细胞通常会导致低肿瘤穿透。克服这些障碍的一个选择是使用佐剂辅助的CD8+ T细胞浸润到TME中。一项针对胰腺导管腺癌(PDAC)的临床试验，众所周知是非免疫原性肿瘤，在接受低剂量环磷酰胺和含有GM-CSF的疫苗的患者中，T细胞的浸润和肿瘤微环境中三级淋巴结构的发展。同样，Poly (I: C)，特别是PICLC（聚赖氨酸和羧甲基纤维素的组合），在临床前试验中显示出增强CD8+ T细胞浸润到肿瘤并减少生长。总的来说，提高CD8+ T细胞浸润的治疗可能与其他可用的治疗协同作用，包括免疫检查点抑制剂、过继细胞疗法和治疗性疫苗。特别地，免疫检查点抑制剂抵消了肿瘤上调免疫检查点（例如，PD-1 & CTLA-4）的表达，导致免疫抑制细胞（例如，T调节细胞&肿瘤相关巨噬细胞）的激活。结合能够增加肿瘤浸润细胞的治疗和免疫检查点抑制剂，确保一旦这些免疫抑制途径被关闭，将有足够的肿瘤浸润细胞（CD8+ T细胞）来摧毁癌细胞。 2 、方法这篇综述将总结利用佐剂进行癌症疫苗的正在进行的临床研究的进展。对于这篇综述，我们进行了clinicaltrials.gov的搜索。搜索词汇包括癌症作为疾病状态，加上“疫苗”作为额外词汇。没有在搜索中包括“佐剂”这个词，因为在讨论疫苗佐剂时，这个词并不总是被包含在内，而且“佐剂”这个词通常在讨论癌症治疗的各个阶段时使用。这个术语也可能容易与“新辅助疗法”混淆，后者定义了在传统癌症治疗前给予的治疗，以缩小肿瘤。我们的搜索通过包括在美国进行的试验，并且查看那些招募中、通过邀请注册、活跃/非招募中和已完成的试验进行了进一步的缩小。包括了I、II、III和IV期的所有试验，并且进一步缩小到只包括那些已经发布了结果的试验。这次搜索产生了182项试验，所有这些试验都由研究人员进行了纳入或排除的评估（见图2）。没有在治疗组中包括疫苗佐剂的试验，不是研究癌症治疗的疫苗，那些不是研究癌症患者的试验都被排除了。评估的47项试验中没有研究疫苗佐剂。33项试验不是在研究癌症疫苗；4项试验不是在评估癌症患者（见图2）。每项试验分别评估了BCG、AS15和tasquinimod作为佐剂。由于它们为每种佐剂只提供了一个数据点，因此这三项试验也被排除了。排除了研究IL-2和IFN-γ作为疫苗的试验。然而，那些研究这些细胞因子作为与其他疫苗结合的佐剂的试验被包括在内。总的来说，我们最终评估包括了94项临床试验。包括的临床试验的总结见表1。图2. 临床试验纳入和排除的流程图 3 、疫苗用于血液恶性肿瘤的使用临床试验经常评估免疫疗法对血液恶性肿瘤的作用。这是由于证据表明，在干细胞移植后，免疫反应可以成功地根除白血病细胞。与在另一个器官中的实体瘤活检相比，血液恶性肿瘤的反应通常更容易报告，因为血液样本和/或骨髓活检相对容易。虽然目前FDA批准的唯一癌症疫苗是用于前列腺癌的，但是有各种癌症疫苗正在进行临床试验，研究血液恶性肿瘤的治疗。大多数在clinicaltrials.gov上发布结果的筛选试验研究了多发性骨髓瘤，与其他形式的血液恶性肿瘤相比，如急性白血病、淋巴瘤或骨髓增生异常综合征。这可以归因于过去几年在多发性骨髓瘤治疗方面的快速进展。大多数研究血液恶性肿瘤的试验处于I期或II期；有一项针对多发性骨髓瘤的试验正在研究MAGE-A3和NY-ESO-1，这些试验与GM-CSF佐剂结合，这是一项II/III期试验。这些试验中没有一个报告了疗效结果；目前只有安全数据可用。需要注意的是，一些针对血液恶性肿瘤的疫苗使用了一些不能应用于实体瘤的机制；例如，Gress等人的试验利用了捐赠者的免疫系统来对抗患者的癌细胞。 4 、临床试验中联合佐剂的使用癌症研究集中在利用个体的免疫系统通过疫苗识别肿瘤相关抗原(TAAs)。肿瘤已经变得非常擅长逃避免疫系统，并通过表达抑制性共刺激受体如CTL-4和PD-1等机制诱导T细胞耐受，并通过释放免疫抑制因子（例如，TGF-β和IL-10）和免疫抑制细胞的侵袭（例如，调节性T细胞(Tregs)和肿瘤相关巨噬细胞(TAMs)）来创造一个免疫原性差的微环境。肿瘤通过这些不同机制创造这些微环境并逃避免疫系统的能力，导致了在那些有显著肿瘤负担的个体中疫苗单疗法的不成功。然而，当特定的佐剂与疫苗结合时，它们有潜力放大免疫反应并延长抗体的寿命。不完全弗氏佐剂(IFA)是一种免疫增强剂，通过持续的抗原释放刺激B细胞和T细胞的产生，并由于其在注射部位形成抗原库的能力，在许多疫苗中作为传递系统使用。通常IFA（例如，Montanide ISA-51）与免疫刺激剂如Poly (I: C)等佐剂结合使用，Poly (I: C)是一种TLR-3配体，激活CTL和Th1反应。在过去十年中，许多以肿瘤学为重点的临床试验专注于这些佐剂的安全性和有效性作为其主要结果，通过监测不良事件和通过免疫分析测量肿瘤抗原特异性免疫。这些试验中一些有希望的组合是IFA与Poly(I: C)、白细胞介素2 (IL-2)和粒细胞-巨噬细胞集落刺激因子(GM-CSF)的组合，GM-CSF是一种炎症性细胞因子，以两种商业产品sargramostim和molgramostim的形式提供。理想的佐剂将在不牺牲安全性的情况下增加疗效。GM-CSF和IFA都已显示出这些特性。在临床试验中，GM-CSF和IFA的组合在启动肿瘤抗原特异性免疫方面表现良好，并且在不与其他药物一起使用时，3-4级事件的发生率为零（表1）。尽管这些药物非常有效，但在治疗个体中免疫反应的持久性通常限制在不到六个月。然而，在一项包括III-IV期黑色素瘤患者的II期临床试验中，将GM-CSF添加到IL-2和IFA中，比单独使用IL-2和IFA的组合，有更多的患者在24个月内具有肿瘤抗原特异性免疫（80% vs 12.5%）。表1 临床试验中癌症疫苗佐剂的比较 95% 置信区间的上限未达到观察进展时间而非无进展生存期（PFS） CP = 环磷酰胺 RT = 放射治疗 GYN = 妇科肿瘤 GBM = 胶质母细胞瘤 CsA = 环孢素 RCC = 肾细胞癌 D/R + 供体/受体 NR = 未报告另一项针对黑色素瘤患者的III期临床试验显示，将IL-2和IFA（不完全弗氏佐剂）结合使用，总体生存率（17.8个月）和无进展生存期（2.2个月）均高于单独使用IL-2（OS：11.1个月；PFS：1.6个月）。在一项II期临床试验中，IFA（Monatide ISA-51）与GM-CSF（沙格司他）和IL-2（阿尔德莱星）结合使用，评估了26名晚期黑色素瘤患者。接受阿尔德莱星和含有IFA和GM-CSF的疫苗治疗的患者，在周围血淋巴细胞（PBLs）中显示42%的细胞毒性T淋巴细胞反应，在哨兵淋巴结（SINs）中为80%，而接受仅含IFA的阿尔德莱星和疫苗的个体中，PBLs为11%，SINs为13%。不完全弗氏佐剂（例如Montanide ISA-51）也显示出与Poly(I: C)等其他佐剂结合使用的潜力。一项I期临床试验针对III-IV期妇科癌症患者，比较了三组的效果（a）疫苗，（b）疫苗+蒙塔尼德，（c）疫苗+蒙塔尼德+Poly(I: C)。观察结果显示，接受疫苗+蒙塔尼德+Poly(I:C)的患者，在16周时可检测到血清免疫球蛋白G（IgG）水平（72.7%，与疫苗+蒙塔尼德的46.2%相比）和CD8+ T细胞反应（90.9%，与疫苗+蒙塔尼德的69.2%相比）。尽管许多临床试验支持佐剂的组合使用，但有时试验可能会传达相互矛盾的结果。例如，一项II期临床试验研究了IFA和咪喹莫特在高风险黑色素瘤患者中的效果，发现接受含有单一佐剂（IFA或咪喹莫特）的疫苗的个体比接受组合佐剂疫苗的个体有更高的免疫反应率。当前研究表明，将具有不同机制和免疫学靶点的佐剂结合使用，可以增加肿瘤抗原特异性免疫、总体生存率和无进展生存率。 5、疫苗与其他治疗药物的联合使用研究人员还探索了将疫苗与其他治疗药物结合使用，以克服与免疫反应相关的挑战。T细胞耗竭发生在长期暴露于抗原（癌细胞）的情况下，这会导致PD-1的持续表达，最终导致T细胞失活或无反应。单克隆抗体，特别是免疫检查点抑制剂，阻断导致免疫抑制效应的受体（例如PD-1）或配体（例如PD-L1），以保持T细胞的激活状态。Le等人评估了纳武利尤单抗联合疫苗用于IV期胰腺癌的效果；对中位总生存率或中位无进展生存率没有显著影响，并且与更高级别的3-4级不良事件的发生率相关。免疫检查点抑制剂似乎在与传统化疗联合使用时，能有效地增加进展时间和总生存率；然而，当并排比较时，传统化疗似乎优于单独使用免疫检查点抑制剂。例如，在IV期胰腺癌的情况下，传统化疗有更高的总生存率（14.7个月）和无进展生存率（5.55个月），而不是伊匹单抗和疫苗（OS：9.38个月；PFS：2.40个月）。在III-IV期套细胞淋巴瘤的临床试验中，当CpG疫苗用于激活自体造血干细胞，除了标准诱导治疗外，观察到疾病中位进展时间（TTP）为6.9年，一年总生存率为87.5%，两年为68.8%。免疫检查点抑制剂提供了许多成功临床试验的有希望的数据；然而，利用免疫检查点抑制剂增强癌症患者免疫反应的联合疗法正在进一步评估中。另一个联合治疗的例子是与赫赛汀的联合。赫赛汀（曲妥珠单抗）是一种单克隆抗体，用于治疗HER2阳性乳腺癌以及表达HER2基因的胃和食管癌。赫赛汀专门结合癌细胞上的HER2受体，阻止它们接收生长信号，有效减缓或停止这些细胞的生长。除了阻断这些受体外，赫赛汀还提醒免疫系统摧毁附着在抗体上的细胞。然而，赫赛汀单药治疗的响应持续时间和疾病进展时间少于一年，使其成为联合治疗的更好候选药物。一项II期临床试验研究了赫赛汀与NeuVax和GM-CSF的联合使用，发现将NeuVax与赫赛汀结合使用是安全的，并没有增加心脏毒性。然而，在疾病无进展生存（在平均25.7个月的随访中）方面，接受赫赛汀、NeuVax和GM-CSF的患者与仅接受赫赛汀和GM-CSF的患者之间没有临床差异。然而，三阴性乳腺癌（TNBC）的一部分患者在接受联合治疗时显示出临床效益，并在III期临床试验中进一步研究。在这个涉及758名患者的多中心、随机、双盲III期试验中，在接受NeuVax（54.1%复发率）和不接受（29.2%复发率）的组之间，没有发现疾病无进展生存的临床意义（平均随访16.8个月）。赫赛汀耐药性可能是这些试验失败的原因，未来的试验可能需要评估其他药物和佐剂，以克服HER2基因表达的复杂性。在过去十年的许多临床试验中，环磷酰胺与传统化疗药物、免疫检查点抑制剂和GM-CSF的联合使用被研究。高剂量的环磷酰胺用作免疫抑制剂，用于治疗自身免疫性疾病和恶性肿瘤。然而，在低剂量下，环磷酰胺具有免疫刺激作用，增强IL-2、IFN-γ和IL-17的水平，并减少Tregs。研究的最大领域集中在将环磷酰胺与GM-CSF结合使用。环磷酰胺通常在临床试验中实现了启动免疫反应的主要结果。然而，在环磷酰胺表现最好的临床试验中，它是与另一种药物（化疗药物或免疫检查点抑制剂）联合给药的。在I-III期临床试验中，与传统疫苗或其他药物相比，环磷酰胺通常有更低的中位总生存率和中位进展生存率（表1）。此外，环磷酰胺与更高级别的3-4级不良事件的发生率相关，在许多试验中，注射部位反应率为100%（表1）。环磷酰胺在癌症患者中启动多方面免疫反应的能力使其成为癌症研究中的主要内容，与其他疗法结合使用时取得了成功。不幸的是，这种药物在疗效和毒性之间似乎有一条微妙的界线，需要进行更多的研究以确定有效且安全剂量。其他与免疫疗法一起探索的化疗药物包括氟尿嘧啶和多柔比星。各种正在进行的临床试验正在探索联合治疗，包括表1中列出的例子，如GVAX + Ipilimumab（胰腺癌）、gp100疫苗IFA + Fludarabine（黑色素瘤）、PANVAC + Docetaxel + GM-CSF（乳腺癌）、Vigil疫苗（GM-CSF）+ Carboplatinum ± Taxol（卵巢癌）。 6、结论这篇综述总结了目前临床试验中用于癌症免疫治疗的佐剂使用情况。尽管传统的癌症治疗方法（例如，化疗、放疗）一直是并将继续是有利的；然而，这些药物的有效性和毒性仍然存在问题。大多数来自临床试验的佐剂（例如，GM-CSF、IFA和IL-2）数据是安全数据。然而，一些临床试验也报告了这些药物的有效性数据。GM-CSF的添加已经提高了多种实体瘤的总生存率和无进展生存率。IFA提高了黑色素瘤患者的总生存率和无进展生存率。IL-2与IFA的组合已被证明可以提高黑色素瘤患者的总生存率和无进展生存率。随着临床试验的结束和进入后期阶段，未来几年将有更多的癌症疫苗有效性数据可用。此外，更多的疫苗正在临床前试验中开发和测试。佐剂具有许多不同的机制，可以用于治疗肿瘤逃避的不同方法，特别是CD8+ T细胞逃避或耗竭。目前的临床试验数据支持，结合具有不同机制和不同免疫学靶点的佐剂可以增加肿瘤抗原特异性免疫、总生存率和无进展生存率。药物-佐剂组合的无限可能性使得找到特定癌症类型的最好治疗方法几乎是不可能的。然而，在过去十年中，一些成功的癌症疫苗疗法已经出现，包括用于转移性前列腺癌的sipuleucel-T（Provenge™）、用于膀胱癌的BCG Theracys™（TICE）和用于黑色素瘤的Talimogene Laherparepvec（T-vec™），为这一研究领域的未来带来了希望。开发能够引发持续免疫反应的带有佐剂的癌症疫苗仍然是一个障碍，因为这些药物的持久性在临床试验中仍然有限。此外，对动态肿瘤微环境带来的挑战、TAAs和TSAs的突变、佐剂在引发所需水平的免疫刺激方面的局限性以及免疫相关不良效应的管理存在理解上的差距。临床前研究正在稳步进展以解决这些知识差距。同样，一些临床试验正在进行中，以寻找有效的癌症疫苗佐剂；一些已经进展到II期和III期。在未来十年中，我们期待一些临床研究能够产生具体的结果，并增加FDA批准的带有佐剂的癌症疫苗列表。总之，使用佐剂或佐剂组合与已建立的癌症治疗方法一起治疗患有高疾病负担的患者具有巨大的前景。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。

疫苗免疫疗法临床研究

100 项与四价人乳头瘤病毒疫苗（酿酒酵母）相关的药物交易

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外链

KEGG	Wiki	ATC	Drug Bank
-	四价人乳头瘤病毒疫苗（酿酒酵母）	J07BM01	-

研发状态

批准上市

10 条最早获批的记录,

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适应症	国家/地区	公司	日期
肛门癌前病变	日本	Merck Sharp & Dohme Corp.	2020-12-25
HPV相关癌症	欧盟	Merck Sharp & Dohme BV	2015-06-10
HPV相关癌症	冰岛	Merck Sharp & Dohme BV	2015-06-10
HPV相关癌症	列支敦士登	Merck Sharp & Dohme BV	2015-06-10
HPV相关癌症	挪威	Merck Sharp & Dohme BV	2015-06-10
原位腺癌	日本	Merck Sharp & Dohme Corp.	2011-07-01
宫颈癌	日本	Merck Sharp & Dohme Corp.	2011-07-01
外阴肿瘤	日本	Merck Sharp & Dohme Corp.	2011-07-01
肛门肿瘤	欧盟	Merck Sharp & Dohme Ireland Ltd.	2006-09-19
肛门肿瘤	冰岛	Merck Sharp & Dohme Ireland Ltd.	2006-09-19
肛门肿瘤	列支敦士登	Merck Sharp & Dohme Ireland Ltd.	2006-09-19
肛门肿瘤	挪威	Merck Sharp & Dohme Ireland Ltd.	2006-09-19
尖锐湿疣	欧盟	Merck Sharp & Dohme Ireland Ltd.	2006-09-19
尖锐湿疣	冰岛	Merck Sharp & Dohme Ireland Ltd.	2006-09-19
尖锐湿疣	列支敦士登	Merck Sharp & Dohme Ireland Ltd.	2006-09-19
尖锐湿疣	挪威	Merck Sharp & Dohme Ireland Ltd.	2006-09-19
人瘤病毒相关性宫颈癌	欧盟	Merck Sharp & Dohme Ireland Ltd.	2006-09-19
人瘤病毒相关性宫颈癌	冰岛	Merck Sharp & Dohme Ireland Ltd.	2006-09-19
人瘤病毒相关性宫颈癌	列支敦士登	Merck Sharp & Dohme Ireland Ltd.	2006-09-19
人瘤病毒相关性宫颈癌	挪威	Merck Sharp & Dohme Ireland Ltd.	2006-09-19

未上市

10 条进展最快的记录,

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适应症	最高研发状态	国家/地区	公司	日期
子宫颈发育不良	申请上市	中国	Merck Sharp & Dohme Corp.	2023-07-11
宫颈原位腺癌	临床3期	中国	Merck & Co., Inc.	2018-08-31
人瘤病毒相关性宫颈原位腺癌	临床3期	中国	Merck Sharp & Dohme Corp.	2018-08-31
人乳头瘤病毒相关的宫颈上皮内瘤样病变	临床3期	中国	Merck Sharp & Dohme Corp.	2018-08-31
白喉	临床3期	-	Merck Sharp & Dohme Corp.	2006-05-01
腺上皮肿瘤	临床3期	-	Merck Sharp & Dohme Corp.	2006-05-01
脊髓灰质炎	临床3期	-	Merck Sharp & Dohme Corp.	2006-05-01
破伤风	临床3期	-	Merck Sharp & Dohme Corp.	2006-05-01
百日咳	临床3期	-	Merck Sharp & Dohme Corp.	2006-05-01
肿瘤	临床3期	-	Merck Sharp & Dohme Corp.	2004-06-16

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临床结果

适应症

分期

评价

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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


Pubmed	N/A	-	-	4-valent human papillomavirus vaccine	願簾願築範範築蓋範淵(齋襯糧壓範範選壓構膚) = 範憲衊醖鏇築築範選鹹繭憲夢醖繭鬱積選鏇遞 (選蓋鹽餘範醖鏇憲廠鬱, 18.89 ~ 23.44)	-	2022-11-30
HIPvac factorial RCT (Pubmed \| Health Technol Assess)	N/A	尖锐湿疣	503	Imiquimod cream	築壓窪鑰築艱壓艱憲醖(艱蓋遞襯簾鹽廠憲鹽觸): adjusted odds ratio = 0.81 (95% CI, 0.54 ~ 1.23) 更多	-	2020-09-01
				Podophyllotoxin cream
NCT01928225 (CTgov)	临床2期	宫颈鳞状上皮内病变 \| HIV感染 \| 鳞状上皮内病变	180	Human Papillomavirus vaccine (Human Papillomavirus Vaccine)	築鹹夢憲廠積夢願窪觸(餘衊鹹鏇顧窪築網觸製) = 淵獵齋衊簾壓構顧觸繭淵觸醖網廠憲夢齋餘簾 (築觸夢憲衊觸鏇積製築, 鏇衊鹽簾憲窪壓壓簾鹹 ~ 夢餘範獵製鏇範襯糧鏇) 更多	-	2020-06-24
				Human Papillomavirus vaccine (Saline Placebo)	築鹹夢憲廠積夢願窪觸(餘衊鹹鏇顧窪築網觸製) = 壓齋網製糧糧蓋襯簾鬱淵觸醖網廠憲夢齋餘簾 (築觸夢憲衊觸鏇積製築, 鏇壓鑰構網獵淵醖窪膚 ~ 鏇鑰蓋築鹽簾廠構淵選) 更多
NCT02993757 (CTgov)	临床3期	乳头状瘤病毒感染 \| 严重登革热	528	CYD Dengue Vaccine+Human Papillomavirus Quadrivalent [Types 6, 11, 16, (CYD Dengue Vaccine + Gardasil (Concomitant Administration))	構淵簾積遞選鹽窪鏇蓋(鏇製餘選齋願鏇築膚鏇) = 願築繭鹹齋憲廠製鬱衊觸醖選鏇廠網顧鏇襯範 (範鏇簾鬱網願膚築壓積, 簾窪鏇選衊簾襯鹽醖糧 ~ 鹽蓋蓋繭襯蓋醖蓋餘網) 更多	-	2020-06-11
				CYD Dengue Vaccine+Human Papillomavirus Quadrivalent [Types 6, 11, 16, (CYD Dengue Vaccine + Gardasil (Sequential Administration))	構淵簾積遞選鹽窪鏇蓋(鏇製餘選齋願鏇築膚鏇) = 壓壓選積鏇夢窪鑰顧衊觸醖選鏇廠網顧鏇襯範 (範鏇簾鬱網願膚築壓積, 願選獵遞製繭鹹選衊齋 ~ 願蓋憲夢網簾鏇鏇選膚) 更多
NCT02199691 (CTgov)	临床2期	流行性脑脊髓膜炎	1,715	Meningococcal Polysaccharide (Serogroups A, C, Y,+W135) Tetanus Toxoid Conjugate Vaccine (Group 1: MenACYW Conjugate Vaccine)	範觸遞憲廠遞襯鏇選顧(衊觸齋製鹹窪鹽鏇遞夢) = 鑰製繭獵窪膚憲壓鏇鹽獵蓋繭鹽餘夢衊鏇鬱積 (簾糧醖觸蓋襯構選範顧, 糧築膚齋廠鹹遞糧築廠 ~ 鹽鏇衊壓憲淵選鏇鏇觸) 更多	-	2020-06-09
				Meningococcal (Groups A, C, Y+W135) Oligosaccharide Diphtheria CRM197 Conjugate Vaccine (Group 2: MENVEO® Vaccine)	範觸遞憲廠遞襯鏇選顧(衊觸齋製鹹窪鹽鏇遞夢) = 鏇鏇顧觸淵餘襯餘獵蓋獵蓋繭鹽餘夢衊鏇鬱積 (簾糧醖觸蓋襯構選範顧, 鏇艱壓衊艱願夢選艱蓋 ~ 膚觸衊遞鬱廠製願顧選) 更多
NCT03493542 (V501-213, CTgov)	临床3期	人瘤病毒相关性宫颈原位腺癌 \| 人乳头瘤病毒相关的宫颈上皮内瘤样病变 \| 人瘤病毒相关性宫颈癌	766	V501 (Chinese Girls Aged 9 to 19 Years)	範構夢簾廠鏇齋齋醖壓(網遞齋醖獵醖艱積襯鹽) = 艱觸廠襯淵積觸顧壓衊鏇衊膚廠憲蓋願鹹壓憲 (壓窪鹽選衊衊憲夢夢觸, 遞網壓觸積鹽憲獵夢憲 ~ 觸齋餘廠艱獵獵構築鏇) 更多	-	2020-05-04
				V501 (Chinese Young Women Aged 20 to 26 Years)	範構夢簾廠鏇齋齋醖壓(網遞齋醖獵醖艱積襯鹽) = 獵簾築鏇顧鹹鑰壓窪選鏇衊膚廠憲蓋願鹹壓憲 (壓窪鹽選衊衊憲夢夢觸, 積醖遞觸夢齋膚鏇餘鑰 ~ 願淵鏇艱積窪餘壓簾餘) 更多
NCT02576054 (V501-200, Pubmed \| Jpn J Infect Dis) 人工标引	临床3期	乳头状瘤病毒感染	99	Quadrivalent HPV Vaccine	築獵餘壓構範範繭願製(遞選鏇繭鏇願觸蓋衊獵) = 顧網艱鬱糧鹹鑰憲窪選鏇憲衊鏇築築遞齋餘範 (齋顧範壓淵鏇衊製糧築, 94.4 ~ 100.0) 更多	积极	2019-09-19
NCT01092195 (CTgov)	临床1期	-	64	Gardasil (Transplant With Immunosuppression)	簾齋糧膚獵簾網願築廠(顧糧鑰憲獵壓鑰窪襯齋) = 醖製繭淵顧糧製範襯夢齋淵衊顧衊糧繭齋選繭 (憲繭窪鑰淵鬱願選糧衊, 築製壓糧襯齋衊艱淵齋 ~ 艱觸製獵鏇鬱糧蓋鹽構) 更多	-	2019-07-01
				Gardasil (Transplant With no Immunosuppression)	簾齋糧膚獵簾網願築廠(顧糧鑰憲獵壓鑰窪襯齋) = 淵構積衊遞遞顧蓋憲膚齋淵衊顧衊糧繭齋選繭 (憲繭窪鑰淵鬱願選糧衊, 夢簾齋鏇觸簾網獵膚窪 ~ 顧築網淵築選網鑰壓選) 更多
NCT01741012 (GARDASIL, CTgov)	临床1期	系统性红斑狼疮	37	Gardasil	鏇網獵選襯憲窪簾製觸(範鬱繭顧顧壓醖蓋構網) = 積構蓋壓醖夢淵願蓋憲築糧蓋膚鬱鑰夢鏇製繭 (鏇鬱鹽獵鏇選艱鏇糧壓, 鑰襯選願艱淵製簾範築 ~ 憲餘簾蓋衊築艱範獵膚) 更多	-	2018-11-05
NCT01862874 (V501-122, CTgov)	临床3期	尖锐湿疣	1,124	V501 (V501)	廠鹽遞築鹽鏇網壓廠願(網餘鬱網廠夢遞製鹽醖) = 壓膚積憲襯壓鹹鏇鑰憲鹹鏇壓艱艱觸遞鏇廠醖 (製蓋積顧鏇範醖簾襯憲, 鬱鏇選網膚積壓壓齋選 ~ 廠範襯網觸醖築廠衊夢) 更多	-	2018-08-31
				Placebo (Placebo)	廠鹽遞築鹽鏇網壓廠願(網餘鬱網廠夢遞製鹽醖) = 餘獵壓構鬱醖餘艱積網鹹鏇壓艱艱觸遞鏇廠醖 (製蓋積顧鏇範醖簾襯憲, 範積鏇構構積鏇範獵膚 ~ 簾齋鏇憲鑰餘淵願廠膚) 更多