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DNA 修复缺陷型着色性干皮病患者发生内脏肿瘤风险增加:四项国际队列研究分析。

Increased risk of internal tumors in DNA repair-deficient xeroderma pigmentosum patients: analysis of four international cohorts.

机构信息

INSERM U981, Gustave Roussy Institute, Université Paris-Saclay, Villejuif, France.

Laboratory of Genome Integrity and Cancers, CNRS UMR9019, Gustave Roussy Institute, Université Paris-Saclay, 114 rue Edouard Vaillant, 94805, Villejuif, France.

出版信息

Orphanet J Rare Dis. 2022 Mar 4;17(1):104. doi: 10.1186/s13023-022-02203-1.

Abstract

BACKGROUND

Xeroderma pigmentosum (XP) is a rare, autosomal, recessive DNA repair-deficiency disorder with a frequency of 1-3 per million livebirths in Europe and USA but with higher frequencies in isolated islands or in countries with a high level of consanguinity. XP is characterized by high incidence of skin cancers on sun-exposed sites. Recent improvement in life expectancy of XP patients suggests an increased risk of frequently aggressive and lethal internal tumors. Our purpose was to quantify relative risks of internal tumor development for XP patients by tumor type, XP-subtype, patients' ages and ethnicity through comparison with the US general population.

METHODS

We analyzed four independent international well-characterized XP cohorts (from USA, UK, France and Brazil) with a total of 434 patients, where 11.3% developed internal tumors and compared them to the American general population. We also compiled, through PubMed/Medline, a dataset of 89 internal tumors in XP patients published between 1958 and 2020.

RESULTS

In the combined 4-XP cohort, relative risk of internal tumors was 34 (95% confidence interval (CI) 25-47) times higher than in the general population (p-value = 1.0E-47) and tumor arose 50 years earlier. The XP-C group was at the highest risk for the 0-20 years old-patients (OR = 665; 95% CI 368-1200; p-value = 4.3E-30). The highest risks were observed for tumors of central nervous system (OR = 331; 95% CI 171-641; p-value = 2.4E-20), hematological malignancies (OR = 120; 95% CI 77-186; p-value = 3.7E-36), thyroid (OR = 74; 95% CI 31-179; p-value = 1.2E-8) and gynecological tumors (OR = 91; 95% CI 42-193; p-value = 3.5E-12). The type of mutation on the XPC gene is associated with different classes of internal tumors. The majority of French XP-C patients (80%) are originated from North Africa and carried the XPC delTG founder mutation specific from the South Mediterranean area. The OR is extremely high for young (0-20 years) patients with more than 1300-fold increase for the French XPs carrying the founder mutation.

CONCLUSION

Because the age of XP population is increasing due to better sun-protection and knowledge of the disease, these results are of particular importance for the physicians to help in early prevention and detection of internal tumors in their XP patients. Few preventive blood analyses or simple medical imaging may help to better detect early cancer appearance in this population.

摘要

背景

着色性干皮病(XP)是一种罕见的常染色体隐性 DNA 修复缺陷疾病,在欧洲和美国的活产儿中发病率为每百万 1-3 例,但在孤立岛屿或高近亲结婚率的国家中发病率更高。XP 的特征是在暴露于阳光的部位发生高频率的皮肤癌。XP 患者的预期寿命最近有所提高,这表明他们经常发生侵袭性和致命性的内部肿瘤的风险增加。我们的目的是通过肿瘤类型、XP 亚型、患者年龄和种族,与美国普通人群进行比较,量化 XP 患者发生内部肿瘤的相对风险。

方法

我们分析了来自美国、英国、法国和巴西的四个独立的国际 XP 队列(共 434 名患者),其中 11.3%的患者发生了内部肿瘤,并将其与美国普通人群进行了比较。我们还通过 PubMed/Medline 汇编了 XP 患者在 1958 年至 2020 年期间发表的 89 例内部肿瘤的数据集。

结果

在联合的 4-XP 队列中,内部肿瘤的相对风险是普通人群的 34 倍(95%置信区间(CI)25-47)(p 值=1.0E-47),并且肿瘤出现的时间早了 50 年。XP-C 组的 0-20 岁患者的风险最高(OR=665;95%CI 368-1200;p 值=4.3E-30)。中枢神经系统肿瘤(OR=331;95%CI 171-641;p 值=2.4E-20)、血液系统恶性肿瘤(OR=120;95%CI 77-186;p 值=3.7E-36)、甲状腺肿瘤(OR=74;95%CI 31-179;p 值=1.2E-8)和妇科肿瘤(OR=91;95%CI 42-193;p 值=3.5E-12)的风险最高。XPC 基因的突变类型与不同类型的内部肿瘤有关。大多数法国 XP-C 患者(80%)来自北非,携带特定于南地中海地区的 XPC delTG 创始人突变。携带该创始人突变的法国 XP-C 患者的风险极高,尤其是 0-20 岁的年轻患者,风险增加超过 1300 倍。

结论

由于 XP 人群的年龄因更好的防晒和对疾病的认识而增加,因此这些结果对医生特别重要,可以帮助他们在早期预防和发现 XP 患者的内部肿瘤。一些预防性血液分析或简单的医学影像学检查可能有助于更好地发现该人群中早期癌症的出现。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b257/8896305/c9324cac8bbb/13023_2022_2203_Fig1_HTML.jpg

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