Departament de Biologia Evolutiva, Ecologia i Ciències Ambientals (BEECA), Facultat de Biologia, Universitat de Barcelona (UB), Av. Diagonal, 643. Planta 2, 08028, Barcelona, Spain.
Centro de Investigaciones en Anomalías Congénitas y Enfermedades Raras (CIACER), Universidad ICESI, Cali, Colombia.
Sci Rep. 2023 Apr 27;13(1):6869. doi: 10.1038/s41598-023-33374-x.
Up to 40% of rare disorders (RD) present facial dysmorphologies, and visual assessment is commonly used for clinical diagnosis. Quantitative approaches are more objective, but mostly rely on European descent populations, disregarding diverse population ancestry. Here, we assessed the facial phenotypes of Down (DS), Morquio (MS), Noonan (NS) and Neurofibromatosis type 1 (NF1) syndromes in a Latino-American population, recording the coordinates of 18 landmarks in 2D images from 79 controls and 51 patients. We quantified facial differences using Euclidean Distance Matrix Analysis, and assessed the diagnostic accuracy of Face2Gene, an automatic deep-learning algorithm. Individuals diagnosed with DS and MS presented severe phenotypes, with 58.2% and 65.4% of significantly different facial traits. The phenotype was milder in NS (47.7%) and non-significant in NF1 (11.4%). Each syndrome presented a characteristic dysmorphology pattern, supporting the diagnostic potential of facial biomarkers. However, population-specific traits were detected in the Colombian population. Diagnostic accuracy was 100% in DS, moderate in NS (66.7%) but lower in comparison to a European population (100%), and below 10% in MS and NF1. Moreover, admixed individuals showed lower facial gestalt similarities. Our results underscore that incorporating populations with Amerindian, African and European ancestry is crucial to improve diagnostic methods of rare disorders.
多达 40%的罕见疾病(RD)表现出面部畸形,临床诊断通常采用视觉评估。定量方法更客观,但大多依赖欧洲血统人群,忽略了不同人群的祖先。在这里,我们评估了拉丁裔人群中的唐氏综合征(DS)、黏多糖贮积症(MS)、努南综合征(NS)和神经纤维瘤病 1 型(NF1)综合征的面部表型,记录了 79 名对照和 51 名患者的 2D 图像中 18 个标志点的坐标。我们使用欧几里得距离矩阵分析量化了面部差异,并评估了自动深度学习算法 Face2Gene 的诊断准确性。诊断为 DS 和 MS 的个体表现出严重的表型,有 58.2%和 65.4%的面部特征存在显著差异。NS 的表型较轻(47.7%),NF1 则无明显差异(11.4%)。每种综合征都表现出独特的畸形模式,支持面部生物标志物的诊断潜力。然而,在哥伦比亚人群中检测到了特定的群体特征。DS 的诊断准确率为 100%,NS 的准确率为 66.7%,但与欧洲人群相比(100%)较低,MS 和 NF1 的准确率则低于 10%。此外,混血个体的面部整体相似度较低。我们的研究结果强调,纳入具有美洲印第安人、非洲和欧洲血统的人群对于改进罕见疾病的诊断方法至关重要。