Enhancing fetal alcohol spectrum disorders diagnosis with a classifier based on the intracerebellar gradient of volumetric undersizing

Author:

Fraize Justine12ORCID,Fischer Clara3,Elmaleh‐Bergès Monique24ORCID,Kerdreux Eliot12ORCID,Beggiato Anita5ORCID,Ntorkou Alexandra4ORCID,Duchesnay Edouard3ORCID,Bekha Dhaif12,Boespflug‐Tanguy Odile6ORCID,Delorme Richard5ORCID,Hertz‐Pannier Lucie12ORCID,Germanaud David127ORCID

Affiliation:

1. CEA Paris‐Saclay, Joliot Institute, NeuroSpin, UNIACT, Centre d'études de Saclay Gif‐sur‐Yvette France

2. Université Paris Cité, Inserm, U1141 NeuroDiderot, inDEV Paris France

3. CEA Paris‐Saclay, Joliot Institute, NeuroSpin, BAOBAB, Centre d'études de Saclay Gif‐sur‐Yvette France

4. Department of Pediatric Radiology, Centre of Excellence InovAND, AP‐HP Robert‐Debré Hospital Paris France

5. Department of Child and Adolescent Psychiatry, Centre of Excellence InovAND, AP‐HP, Robert‐Debré Hospital Paris France

6. Université Paris Cité, U1141 NeuroDiderot, NeuroDEV Paris France

7. Department of Genetics, Centre of Excellence InovAND AP‐HP, Robert‐Debré Hospital Paris France

Abstract

AbstractIn fetal alcohol spectrum disorders (FASD), brain growth deficiency is a hallmark of subjects both with fetal alcohol syndrome (FAS) and with non‐syndromic FASD (NS‐FASD, i.e., those without specific diagnostic features). However, although the cerebellum was suggested to be more severely undersized than the rest of the brain, it has not yet been given a specific place in the FASD diagnostic criteria where neuroanatomical features still count for little if anything in diagnostic specificity. We applied a combination of cerebellar segmentation tools on a 1.5 T 3DT1 brain MRI dataset from a monocentric population of 89 FASD (52 FAS, 37 NS‐FASD) and 126 typically developing controls (6–20 years old), providing 8 volumes: cerebellum, vermis and 3 lobes (anterior, posterior, inferior), plus total brain volume. After adjustment of confounders, the allometric scaling relationship between these cerebellar volumes (Vi) and the total brain or cerebellum volume (Vt) was fitted (Vi = bVta), and the effect of group (FAS, control) on allometric scaling was evaluated. We then estimated for each cerebellar volume in the FAS population the deviation from the typical scaling (vDTS) learned in the controls. Lastly, we trained and tested two classifiers to discriminate FAS from controls, one based on the total cerebellum vDTS only, the other based on all the cerebellar vDTS, comparing their performance both in the FAS and the NS‐FASD group. Allometric scaling was significantly different between FAS and control group for all the cerebellar volumes (p < .001). We confirmed the excess of total cerebellum volume deficit (vDTS = −10.6%) and revealed an antero‐inferior‐posterior gradient of volumetric undersizing in the hemispheres (−12.4%, 1.1%, 2.0%, respectively) and the vermis (−16.7%, −9.2%, −8.6%, repectively). The classifier based on the intracerebellar gradient of vDTS performed more efficiently than the one based on total cerebellum vDTS only (AUC = 92% vs. 82%, p = .001). Setting a high probability threshold for >95% specificity of the classifiers, the gradient‐based classifier identified 35% of the NS‐FASD to have a FAS cerebellar phenotype, compared to 11% with the cerebellum‐only classifier (pFISHER = 0.027). In a large series of FASD, this study details the volumetric undersizing within the cerebellum at the lobar and vermian level using allometric scaling, revealing an anterior‐inferior‐posterior gradient of vulnerability to prenatal alcohol exposure. It also strongly suggests that this intracerebellar gradient of volumetric undersizing may be a reliable neuroanatomical signature of FAS that could be used to improve the specificity of the diagnosis of NS‐FASD.

Funder

Agence Nationale de la Recherche

Publisher

Wiley

Subject

Neurology (clinical),Neurology,Radiology, Nuclear Medicine and imaging,Radiological and Ultrasound Technology,Anatomy

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