TY - JOUR
T1 - Population-specific facial traits and diagnosis accuracy of genetic and rare diseases in an admixed Colombian population
AU - Echeverry-Quiceno, Luis M.
AU - Candelo, Estephania
AU - Gómez, Eidith
AU - Solís, Paula
AU - Ramírez, Diana
AU - Ortiz, Diana
AU - González, Alejandro
AU - Sevillano, Xavier
AU - Cuéllar, Juan Carlos
AU - Pachajoa, Harry
AU - Martínez-Abadías, Neus
N1 - Funding Information:
We are grateful for the voluntary collaboration of all participants, including children and their families. We are thankful to Colegio Ecológico Scout and Universidad Icesi for granting us permission to organize the photographic sessions in Colombia; and Dr. Nelläker for help with accessing the European database. We thank Max Rubert for technical photographic assistance. We also thank the reviewers and editor for their insightful comments, which have greatly improved the quality of our manuscript. We acknowledge support from Proyecto COL0012168-1097 Interfacultades-ICESI, Grup de Recerca Consolidat (2021 SGR 00706), and Biological Anthropological Master UB-UAB.
Funding Information:
We are grateful for the voluntary collaboration of all participants, including children and their families. We are thankful to Colegio Ecológico Scout and Universidad Icesi for granting us permission to organize the photographic sessions in Colombia; and Dr. Nelläker for help with accessing the European database. We thank Max Rubert for technical photographic assistance. We also thank the reviewers and editor for their insightful comments, which have greatly improved the quality of our manuscript. We acknowledge support from Proyecto COL0012168-1097 Interfacultades-ICESI, Grup de Recerca Consolidat (2021 SGR 00706), and Biological Anthropological Master UB-UAB.
Publisher Copyright:
© 2023, The Author(s).
PY - 2023/4/27
Y1 - 2023/4/27
N2 - 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.
AB - 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.
KW - Admixture
KW - Ancestry
KW - Brain
KW - Cohort
KW - Disorders
KW - Down-syndrome
KW - Morquio
KW - Noonan syndrome
KW - Phenotypes
KW - Survival
UR - http://www.scopus.com/inward/record.url?scp=85158015556&partnerID=8YFLogxK
U2 - 10.1038/s41598-023-33374-x
DO - 10.1038/s41598-023-33374-x
M3 - Article
AN - SCOPUS:85158015556
SN - 2045-2322
VL - 13
JO - Scientific Reports
JF - Scientific Reports
IS - 1
M1 - 6869
ER -