根据 HLA 遗传风险类别分析儿科患者的乳糜泻:一项回顾性观察研究。
Celiac disease in pediatric patients according to HLA genetic risk classes: a retrospective observational study.
机构信息
Department of Pediatrics, University of Campania Luigi Vanvitelli, Naples, Italy.
Department of Public Health, University of Naples Federico II, Naples, Italy.
出版信息
Ital J Pediatr. 2021 May 5;47(1):107. doi: 10.1186/s13052-021-01052-1.
BACKGROUND
Celiac disease (CD) is an autoimmune enteropathy in which HLA-DQ haplotypes define susceptibility. Our aim was to evaluate if belonging to a certain HLA-DQ class risk could be associated to the clinical, serological and histological presentation of CD.
METHODS
We performed a retrospective observational monocentric study including all 300 patients diagnosed with CD, who underwent HLA typing. Clinical, serological and histological data was collected from clinical records and their association with HLA-DQ class risk was verified through statistical tests.
RESULTS
In our sample mean age at onset was 6.7 ± 4.2 years, with a prevalence of females (n = 183; 61%), typical symptoms (n = 242; 80.6%) and anti-tTG IgA ≥ 100 U/mL (n = 194; 64.7%). Family history was present only in 19% (n = 57) of patients, and it was not significantly associated with any of the clinical and demographical data analyzed or the belonging to a certain HLA-DQ class risk. We found in the male population more frequently a coexistence of CD and atopic syndrome (males: n = 47; 40.2%; females: n = 50; 27.3%; p = 0.020). Early age of onset, instead, was associated with typical symptoms (m = 6.4 ± 4; p = 0.045) and elevated liver enzymes (m = 5 ± 3.8; p < 0.001), while later age of onset was associated with presence of other autoimmune diseases (m = 8.2 ± 4; p = 0.01). We observed statistically significant influences of HLA class risk on antibodies and liver enzymes levels: G1, G4 and G2 classes showed more frequently anti-tTG IgA ≥ 100 U/mL (n = 44; 80%, n = 16; 69.6%, n = 48; 67.6% respectively; p-value = 0.037), and in patients from G2 class we found enhanced liver enzymes (n = 28; 39.4%; p-value = 0.005). HLA class risk was still significantly associated with anti-tTG ≥ 100 (p = 0.044) and with hypertransaminasemia (p = 0.010) after a multiple logistic regression adjusted for the effect of gender, age at onset and family history.
CONCLUSIONS
We failed to prove an association between HLA-DQ genotypes and the clinical features in our CD pediatric patients. Although, our results suggest an effect of the DQB1-02 allele not only on the level of antibodies to tTG, but possibly also on liver involvement.
背景
乳糜泻(CD)是一种自身免疫性肠病,其中 HLA-DQ 单倍型定义了易感性。我们的目的是评估是否属于特定的 HLA-DQ 类风险可能与 CD 的临床、血清学和组织学表现相关。
方法
我们进行了一项回顾性观察性单中心研究,包括所有 300 名接受 HLA 分型诊断为 CD 的患者。从临床记录中收集临床、血清学和组织学数据,并通过统计检验验证其与 HLA-DQ 类风险的关联。
结果
在我们的样本中,发病年龄的平均值为 6.7±4.2 岁,女性患病率较高(n=183;61%),典型症状(n=242;80.6%)和抗 tTG IgA≥100 U/mL(n=194;64.7%)。家族史仅存在于 19%(n=57)的患者中,但与分析的任何临床和人口统计学数据或特定 HLA-DQ 类风险无关。我们在男性人群中发现更频繁地存在 CD 和特应性综合征共存(男性:n=47;40.2%;女性:n=50;27.3%;p=0.020)。相反,发病年龄较早与典型症状(m=6.4±4;p=0.045)和升高的肝酶(m=5±3.8;p<0.001)相关,而发病年龄较晚与其他自身免疫性疾病的存在相关(m=8.2±4;p=0.01)。我们观察到 HLA 类风险对抗体和肝酶水平有统计学显著影响:G1、G4 和 G2 类更频繁地出现抗 tTG IgA≥100 U/mL(n=44;80%,n=16;69.6%,n=48;67.6%分别;p 值=0.037),并且在 G2 类患者中我们发现肝酶升高(n=28;39.4%;p 值=0.005)。在调整性别、发病年龄和家族史影响的多变量逻辑回归后,HLA 类风险仍然与抗 tTG≥100(p=0.044)和高转氨酶血症(p=0.010)显著相关。
结论
我们未能证明 HLA-DQ 基因型与我们 CD 儿科患者的临床特征之间存在关联。尽管如此,我们的结果表明 DQB1-02 等位基因不仅对 tTG 抗体的水平有影响,而且可能对肝脏受累也有影响。
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