Gene Variants in NKX2-1 Do Not Represent a Major Etiological Factor of Primary Congenital Hypothyroidism in Mexican Population

Abstract: Congenital hypothyroidism (CH), attributable to thyroid dysgenesis (TD), has an unusually high prevalence in Mexican population but the causes are unknown. NKX2-1, as a candidate gene, was subjected to automated Sanger sequencing in 122 unrelated Mexican patients with CH/TD. Although this study includes the largest number of TD-related CH patients in whom NKX2-1 has been analyzed, no pathogenic variants were detected; only three benign polymorphic changes were identified. These results suggest that NKX2-1 is n… Show more

“…We failed to identify any CNV-type change. Our results add to previous findings that 1% of CH-TD Mexican patients could be attributed to PAX8 missense defects [18], and there was no discernible participation of small-nucleotide NKX2-1 pathogenic changes [19]. Collectively, these data obtained in ≥100 Mexican patients suggest that germline small-nucleotide defects in the main TD-related genes, PAX8 [18], NKX2-1 [19], FOXE1, NKX2-5, and TSHR (this work), could explain ~ 2.5% of isolated CH-TD cases in Mexico, without any identified etiologic role for CNVs in PAX8, NKX2-1, FOXE1, or TSHR (NKX2-5 was not included in the employed MLPA kit).…”

“…Our results add to previous findings that 1% of CH-TD Mexican patients could be attributed to PAX8 missense defects [18], and there was no discernible participation of small-nucleotide NKX2-1 pathogenic changes [19]. Collectively, these data obtained in ≥100 Mexican patients suggest that germline small-nucleotide defects in the main TD-related genes, PAX8 [18], NKX2-1 [19], FOXE1, NKX2-5, and TSHR (this work), could explain ~ 2.5% of isolated CH-TD cases in Mexico, without any identified etiologic role for CNVs in PAX8, NKX2-1, FOXE1, or TSHR (NKX2-5 was not included in the employed MLPA kit). Although this explains only a small proportion of cases, it is higher than that documented in 90 Brazilian CH-TD patients, where PAX8, NKX2-5, TSHR, and HES1 (MIM*139605) did not reveal any pathogenic or VUS change [31,32], and seems quite similar to the rate obtained in Japanese CH patients (2.0%, N=2/102), at least 50% of whom carried a confirmed TD phenotype [16].…”

“…One familial case of neurofibromatosis type 1 (MIM#162200) was identified in a patient (HC-222) and her mother. A normal Sanger sequencing result for the NKX2-1 gene was previously reported for 122 of the 128 patients included herein [19].…”

“…In contrast to the information available in the literature for Caucasian and Asian CH patients [3,6,7,13,16], relatively little is known about the participation of genetic factors in the etiology of CH-TD in Latin-American populations. To date, limited publications are available for Brazilian [31,32] and Mexican [18,19] populations. Given the predominance of TD (~93%) in the etiology of primary permanent CH in Mexicans [17], the aim of this work was to examine whether germline small-nucleotide (NKX2-5, FOXE1, and TSHR) and CNV-type (FOXE1, PAX8, NKX2-1, PAX8, and TSHR) changes in TD-related genes play an etiological role in some Mexican CH patients lacking clinical suspicion of a syndromic form and with a confirmed TD imaging-based diagnosis.…”

“…CNV-type changes in TD-related genes have not been explored in Latin American CH populations [18,19,31,32]. In a small sample of Polish CH-TD patients directly subjected to MLPA, whole-exon heterozygous deletions in PAX8, TSHR, and FOXE1 genes surprisingly comprised 11% (N=5/45) of the underlying TD pathogenic genotypes [15].…”

Further Evidence that Defects in mMain Thyroid Dysgenesis-Related Genes are an Uncommon Etiology for Primary Congenital Hypothyroidism in Mexican Patients: Report of Rare Variants in FOXE1, NKX2-5 and TSHR

“…We failed to identify any CNV-type change. Our results add to previous findings that 1% of CH-TD Mexican patients could be attributed to PAX8 missense defects [18], and there was no discernible participation of small-nucleotide NKX2-1 pathogenic changes [19]. Collectively, these data obtained in ≥100 Mexican patients suggest that germline small-nucleotide defects in the main TD-related genes, PAX8 [18], NKX2-1 [19], FOXE1, NKX2-5, and TSHR (this work), could explain ~ 2.5% of isolated CH-TD cases in Mexico, without any identified etiologic role for CNVs in PAX8, NKX2-1, FOXE1, or TSHR (NKX2-5 was not included in the employed MLPA kit).…”

“…Our results add to previous findings that 1% of CH-TD Mexican patients could be attributed to PAX8 missense defects [18], and there was no discernible participation of small-nucleotide NKX2-1 pathogenic changes [19]. Collectively, these data obtained in ≥100 Mexican patients suggest that germline small-nucleotide defects in the main TD-related genes, PAX8 [18], NKX2-1 [19], FOXE1, NKX2-5, and TSHR (this work), could explain ~ 2.5% of isolated CH-TD cases in Mexico, without any identified etiologic role for CNVs in PAX8, NKX2-1, FOXE1, or TSHR (NKX2-5 was not included in the employed MLPA kit). Although this explains only a small proportion of cases, it is higher than that documented in 90 Brazilian CH-TD patients, where PAX8, NKX2-5, TSHR, and HES1 (MIM*139605) did not reveal any pathogenic or VUS change [31,32], and seems quite similar to the rate obtained in Japanese CH patients (2.0%, N=2/102), at least 50% of whom carried a confirmed TD phenotype [16].…”

“…One familial case of neurofibromatosis type 1 (MIM#162200) was identified in a patient (HC-222) and her mother. A normal Sanger sequencing result for the NKX2-1 gene was previously reported for 122 of the 128 patients included herein [19].…”

“…In contrast to the information available in the literature for Caucasian and Asian CH patients [3,6,7,13,16], relatively little is known about the participation of genetic factors in the etiology of CH-TD in Latin-American populations. To date, limited publications are available for Brazilian [31,32] and Mexican [18,19] populations. Given the predominance of TD (~93%) in the etiology of primary permanent CH in Mexicans [17], the aim of this work was to examine whether germline small-nucleotide (NKX2-5, FOXE1, and TSHR) and CNV-type (FOXE1, PAX8, NKX2-1, PAX8, and TSHR) changes in TD-related genes play an etiological role in some Mexican CH patients lacking clinical suspicion of a syndromic form and with a confirmed TD imaging-based diagnosis.…”

“…CNV-type changes in TD-related genes have not been explored in Latin American CH populations [18,19,31,32]. In a small sample of Polish CH-TD patients directly subjected to MLPA, whole-exon heterozygous deletions in PAX8, TSHR, and FOXE1 genes surprisingly comprised 11% (N=5/45) of the underlying TD pathogenic genotypes [15].…”

Further Evidence that Defects in mMain Thyroid Dysgenesis-Related Genes are an Uncommon Etiology for Primary Congenital Hypothyroidism in Mexican Patients: Report of Rare Variants in FOXE1, NKX2-5 and TSHR

Further Evidence That Defects in Main Thyroid Dysgenesis-Related Genes Are an Uncommon Etiology for Primary Congenital Hypothyroidism in Mexican Patients: Report of Rare Variants in FOXE1, NKX2-5 and TSHR