Uncovering the contribution of rare genetic variants in orofacial clefts Open Access

Abstract

Orofacial clefts (OFCs) are common craniofacial congenital anomalies that occur when the palate and/or the lip fail to form properly during development. Approximately 70% of OFCs are considered non-syndromic, occurring as isolated events without additional structural or cognitive anomalies. They are heterogeneous etiologies involving environmental and genetic risk factors that include Mendelian and non-Mendelian causes. However, much of the focus has been on common variants and genome-wide association studies, which only account for ~25% of the heritable risk for OFCs. The unaccounted heritability may be attributed to other sources of variation, including rare variants that are examined using sequencing approaches (e.g., whole-exome sequencing (WES) and whole-genome sequencing (WGS)). We hypothesize that rare variants contribute to the OFC risk through different genetic mechanisms. We first investigated rare variants using WES in 31 multiplex families, each with multiple affected individuals that were consistent with Mendelian inheritance. Nineteen of these families were deeply phenotyped to assess subclinical phenotypes, which are subtle phenotypes hypothesized to exist within the same etiological spectrum as OFCs. We identified likely causal variants in 25% of multiplex families. Several variants were in genes that are mutated in Mendelian syndromes that include OFCs as a feature. Although some variants were found in individuals with subclinical phenotypes, we cumulatively failed to find clear evidence supporting the subclinical phenotype hypothesis. To explore all possible types of inheritance, we next analyzed 50 consanguineous families from Colombia and Turkey. The identified variants of interest included dominant-acting heterozygous variants as well as recessive homozygous variants. Finally, we estimated the diagnostic yield of 841 cases and 294 controls with WGS using 418 genes previously implicated in OFCs. We found 9.04% of cases had a pathogenic variant and nine genes alone accounted for 4.64% of the yield. Taken together, these findings provide evidence of the role of rare variants in OFCs and underscore the etiologic heterogeneity of OFCs. Further elucidation of the genetic architectures of all OFC types will aid in improving recurrence risk estimations and developing tailored management plans for individuals with OFCs.

Table of Contents

CHAPTER I. INTRODUCTION 1

What are OFCs? 1

Overview of Craniofacial Development 2

Broadening the Phenotypic Spectrum of OFCs 3

Syndromic and Non-Syndromic Forms of OFCs 6

What causes OFCs? 7

Environment in OFCs 7

Genetics and Environment Contributions in OFCs 9

Epigenetics Contributions in OFCs 9

Genetic Contributions in OFCs 10

Syndromic Gene Mapping 12

Genetics in Non-Syndromic OFCs 12

Overlap in Genetics Between Syndromic and Non-Syndromic OFCs 17

A Phenotypic Spectrum from Syndromic to Non-Syndromic OFCs 19

Conclusion 21

Tables 23

Figures 25

References 27

CHAPTER II. RARE VARIANTS FOUND IN MULTIPLEX FAMILIES WITH OROFACIAL CLEFTS: DOES EXPANDING THE PHENOTYPE MAKE A DIFFERENCE? 45

Introduction 46

Methods 48

Results 52

Discussion 57

Figures 60

Supplementary Tables 62

References 67

CHAPTER III. IDENTIFYING RARE RECESSIVE MUTATIONS IN CONSANGUINEOUS FAMILIES WITH OROFACIAL CLEFTS 72

Introduction 73

Methods 74

Results 76

Discussion 80

Tables 84

Figures 85

References 86

CHAPTER IV. RARE VARIANTS FOUND IN CLINICAL GENE PANELS ILLUMINATE THE GENETIC AND ALLELIC ARCHITECTURE OF OROFACIAL CLEFTING 90

Introduction 91

Methods 92

Results 99

Discussion 104

Figures 108

Supplementary Tables 111

Supplementary Figures 133

References 141

CHAPTER V. DISCUSSION 145

Summary 145

Diagnostic Yield Comparisons Across Studies 146

Genetic Heterogeneity of OFCs 148

Genetic Architecture of Cleft Subtypes and Subclinical Phenotypes 149

Future Directions 151

Conclusion 152

References 154

About this Dissertation

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School	Laney Graduate School
Department	Biological and Biomedical Sciences
Subfield / Discipline	Genetics and Molecular Biology
Degree	Ph.D.
Submission	Dissertation
Language	English
Research Field	Biology, Genetics Biology, Bioinformatics
Keyword	rare variants orofacial clefts human genetics genetic sequencing
Committee Chair / Thesis Advisor	Leslie, Elizabeth, Emory University
Committee Members	Epstein, Michael, Emory University Cutler, David, Emory University Conneely, Karen, Emory University Gambello, Michael, Emory University

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