A Case-Control Study to Evaluate Broad-Spectrum Antibiotic use and High Birth Weight as Potential Risk Factors for Early-Onset Colorectal Cancer
一项病例对照研究,评估广谱抗生素的使用和高出生体重作为早发性结直肠癌的潜在危险因素
基本信息
- 批准号:10304590
- 负责人:
- 金额:$ 37.99万
- 依托单位:
- 依托单位国家:美国
- 项目类别:
- 财政年份:2021
- 资助国家:美国
- 起止时间:2021-09-15 至 2024-08-31
- 项目状态:已结题
- 来源:
- 关键词:20 year oldAccountingAddressAdultAgeAge-YearsAnatomyAnimalsAntibioticsAnxietyBiologicalBiometryBirthBirth WeightCaliforniaCancer ControlCancer EtiologyCarcinogensCase SeriesCase-Control StudiesCessation of lifeCharacteristicsChemicalsChildColorectal CancerComputerized Medical RecordCountryDataDeveloped CountriesDevelopmentDiabetes MellitusDiagnosisDietDiseaseEnvironmental ExposureEpidemicEpidemiologistEpidemiologyExposure toFibrinogenFoodFoundationsFrightGastroenterologyHereditary Neoplastic SyndromesHigh birth weight infantHormonesHumanIncidenceIncomeIndividualInterruptionKnowledgeLate-Onset DisorderLife StyleLightLinkLiteratureMalignant NeoplasmsMolecularNested Case-Control StudyObesityPathologicPathway interactionsPharmacoepidemiologyPhysical activityPlayPositioning AttributePreventionPrevention strategyPrivate SectorPublic HealthPublic SectorQuality of lifeResearch DesignRiskRisk FactorsRoleSample SizeSamplingSomatomedinsStudy SubjectSubgroupSymptomsSystemTestingUnited StatesWaterWeight Gainage groupcancer diagnosiscancer riskcancer sitecarcinogenesiscolorectal cancer riskdensityearly life exposureearly onsetearly onset colorectal cancerearly screeningearly-onset colorectal carcinogenesisethnic diversityexperiencegut dysbiosisgut microbiomeimprovedin uteroinsightmRNA Differential Displaysnovelpopulation basedprenatalpublic health interventionracial and ethnicrisk predictionrisk prediction modelscreeningsedentary lifestylestem cellstrendyoung adult
项目摘要
Project Abstract
The incidence of colorectal cancer in young adults under age 50 (referred to as early onset colorectal cancer
[eoCRC]) has been rising by a striking 2% per year in the United States since the 1990s. Even more notably, a
significant increase in eoCRC is experienced by every 5-year age group from as young as age 20 years. The
accompanying human toll should not be understated considering the mirroring rise of deaths due to eoCRC,
and the loss in quality of life given that most eoCRC are diagnosed at advanced stages. Despite urgent needs
to interrupt this trajectory, factors responsible for the rise of eoCRC are unknown, rendering the development
of effective cancer control strategies difficult. This study seeks to shed light on eoCRC risk factors that may
contribute to the rising incidence of this disease, directly addressing Provocative Question1 from RFA-CA-20-
004: “What are the underlying causes of the unexplained rising incidence in early-onset cancers?” Evidence
suggests that eoCRC may be a distinct disease subset with differential key risk factors from late-onset CRC.
To date, studies that investigated eoCRC etiology remain sparse, and they mostly focused on the role of
established risk factors for late-onset CRC, such as obesity, diet and physical activities. There has been a
general lack of studies that evaluate the role of alternative risk factors such as those that involve gut dysbiosis
and early life exposures in eoCRC etiology. To fill this critical gap, we will test novel hypotheses on the roles of
broad-spectrum antibiotic use and high birth weight in eoCRC etiology. Use of broad-spectrum antibiotics
results in intense and long-lasting gut dysbiosis, which is strongly implicated in CRC carcinogenesis. Further,
animal studies and recent epidemiologic evidence supports the role of broad-spectrum antibiotics as CRC
carcinogens. High birth weight, likely reflecting altered in-utero programming of key hormone pathways such as
the insulin-like growth factor system and higher number of stem cells at risk for carcinogenesis, has been
linked to risk of other young-onset cancers and late-onset CRC. Further, both broad-spectrum antibiotic use
and high birth weight have been on the rise for decades preceding the rise of eoCRC. We will use a
population-based, nested case-control study design, including ~1,100 eoCRC cases diagnosed between 2009-
2021 at Kaiser Permanente Southern California (KPSC) to carry out the following Specific Aims: (SA1) Test
the hypothesis that greater exposure to broad-spectrum antibiotics increases risk of eoCRC; and (SA2)
Test the hypothesis that high birth weight increases risk of eoCRC. KPSC's unique strengths include
large sample size, comprehensive electronic medical records, long-term membership retention, and great
racial/ethnic diversity. At the completion of these aims, we expect to (1) offer new insights into the
carcinogenesis of eoCRC; (2) facilitate the development of eoCRC risk prediction models; (3) inform targeted
early screening strategies; and (3) inform novel prevention strategies to amend this devastating epidemic.
项目摘要
50岁以下青壮年结直肠癌(简称早发性结直肠癌)发病率
[eoCRC])自 20 世纪 90 年代以来在美国每年以惊人的 2% 的速度增长。
从 20 岁开始,每个 5 岁年龄组的 eoCRC 都会显着增加。
考虑到 eoCRC 导致的死亡人数相应上升,不应低估随之而来的人员伤亡,
尽管需求迫切,但大多数 eoCRC 仍处于晚期诊断,导致生活质量下降。
为了打断这一轨迹,导致 eoCRC 兴起的因素尚不清楚,因此发展
这项研究旨在揭示可能的 eoCRC 危险因素。
导致这种疾病发病率上升,直接解决 RFA-CA-20 中的挑衅性问题 1-
004:“早发癌症发病率不明原因上升的根本原因是什么?”
表明 eoCRC 可能是一个独特的疾病子集,其关键危险因素与晚发性 CRC 不同。
迄今为止,调查 eoCRC 病因学的研究仍然很少,而且主要集中在
确定了迟发性结直肠癌的危险因素,例如肥胖、饮食和体力活动。
普遍缺乏评估其他危险因素(例如涉及肠道菌群失调的因素)作用的研究
为了填补这一关键空白,我们将测试关于 eoCRC 病因学的新假设。
eoCRC 病因中广谱抗生素的使用和高出生体重。
导致强烈且持久的肠道菌群失调,这与结直肠癌的致癌作用密切相关。
动物研究和最近的流行病学证据支持广谱抗生素在结直肠癌中的作用
高出生体重,可能反映了关键激素途径的子宫内编程改变,例如
胰岛素样生长因子系统和更多数量的干细胞有致癌风险,
此外,广谱抗生素的使用与其他年轻发病癌症和晚发结直肠癌的风险有关。
在 eoCRC 兴起之前的几十年里,高出生体重的情况一直在上升。
基于人群的巢式病例对照研究设计,包括 2009 年至 2009 年期间诊断的约 1,100 例 eoCRC 病例
2021 年在南加州凯撒医疗机构 (KPSC) 实施以下具体目标:(SA1) 测试
假设更多地接触广谱抗生素会增加 eoCRC 的风险;以及 (SA2)
检验高出生体重会增加 eoCRC 风险的假设,KPSC 的独特优势包括:
样本量大、电子病历全面、会员长期保留、
完成这些目标后,我们期望 (1) 提供关于种族/民族多样性的新见解。
eoCRC 的致癌作用;(2) 促进 eoCRC 风险预测模型的开发;(3) 为目标提供信息;
早期筛查策略;(3) 提供新的预防策略来改变这种毁灭性的流行病。
项目成果
期刊论文数量(0)
专著数量(0)
科研奖励数量(0)
会议论文数量(0)
专利数量(0)
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Chun R. Chao其他文献
An unmasking phenomenon in an observational post-licensure safety study of adolescent girls and young women.
对青春期女孩和年轻女性进行的观察性许可后安全研究中揭示的现象。
- DOI:
- 发表时间:
2012 - 期刊:
- 影响因子:5.5
- 作者:
Steven J. Jacobsen;L. Sy;B. Ackerson;Chun R. Chao;J. M. Slezak;T. Cheetham;H. Takhar;C. Velicer;John R Hansen;Nicola P. Klein - 通讯作者:
Nicola P. Klein
Chun R. Chao的其他文献
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{{ truncateString('Chun R. Chao', 18)}}的其他基金
Effectiveness and Mechanisms of Multilevel Implementation Strategies to Improve Provider Recommendation and Advance HPV Vaccination: a Cluster Randomized Trial
改善提供者推荐和推进 HPV 疫苗接种的多层次实施策略的有效性和机制:整群随机试验
- 批准号:
10296607 - 财政年份:2021
- 资助金额:
$ 37.99万 - 项目类别:
Effectiveness and Mechanisms of Multilevel Implementation Strategies to Improve Provider Recommendation and Advance HPV Vaccination: a Cluster Randomized Trial
改善提供者推荐和推进 HPV 疫苗接种的多层次实施策略的有效性和机制:整群随机试验
- 批准号:
10450821 - 财政年份:2021
- 资助金额:
$ 37.99万 - 项目类别:
Effectiveness and Mechanisms of Multilevel Implementation Strategies to Improve Provider Recommendation and Advance HPV Vaccination: a Cluster Randomized Trial
改善提供者推荐和推进 HPV 疫苗接种的多层次实施策略的有效性和机制:整群随机试验
- 批准号:
10650395 - 财政年份:2021
- 资助金额:
$ 37.99万 - 项目类别:
A Case-Control Study to Evaluate Broad-Spectrum Antibiotic use and High Birth Weight as Potential Risk Factors for Early-Onset Colorectal Cancer
一项病例对照研究,评估广谱抗生素的使用和高出生体重作为早发性结直肠癌的潜在危险因素
- 批准号:
10687185 - 财政年份:2021
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$ 37.99万 - 项目类别:
Follow-up care and preventive service use among survivors of adolescent and young adult cancer.
青少年和青年癌症幸存者的后续护理和预防服务使用。
- 批准号:
9178444 - 财政年份:2016
- 资助金额:
$ 37.99万 - 项目类别:
Prognostic Markers for HIV-Postive Diffuse Large B-Cell Lymphoma
HIV 阳性弥漫性大 B 细胞淋巴瘤的预后标志物
- 批准号:
7691293 - 财政年份:2008
- 资助金额:
$ 37.99万 - 项目类别:
Prognostic Markers for HIV-Postive Diffuse Large B-Cell Lymphoma
HIV 阳性弥漫性大 B 细胞淋巴瘤的预后标志物
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8120890 - 财政年份:2008
- 资助金额:
$ 37.99万 - 项目类别:
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