Lethal COG6‐CDG in neonatal patient with arachnodactyly, joint contractures, and skin manifestations: Founder mutation in the Southeastern European population?

Abstract: Herein, we report a lethal case of the ultra-rare COG6congenital disorder of glycosylation (CDG) presenting with skin manifestations (scaling and erosions) and joint contractures in a neonate of Albanian origin. The patient was homozygous for a COG6 pathogenic variant, previously reported in another three individuals of Greek, Bulgarian and Turkish descent. The presence of a founder mutation in the geographical area is possible. The index case emphasizes the need to consider CDGs in neonatal patients with skin… Show more

“… Note : Features of the two COG6‐CDG patients in our cohort (P1 and P2) and the previously published cases (R1:1, Cirnigliaro et al 6 ; R2:1, Ververi et al 7 ; R3:1, Zhao et al 8 ; R4:1, Lugli et al 10 ; R5:1, Lugli et al 9 ; R6:1, R6:2, Komlosi et al 11 ; R7:1, R7:2, Mandel et al 12 ; R8:1, Li et al 13 ; R9:1, Althonaian et al 14 ; R10:1, Wu et al 15 ; R11:1‐R11:7, Alsubhi et al 16 ; R12:1; Pérez‐Cerdá et al 17 ; R13:1‐R13:7, Rymen et al 18 ; R14:1, Shaheen et al 19 ; R15:1, Huybrechts et al 20 ; R16:1, Lubbehusen et al 21 In Shaheen et al, 19 11 more patients are mentioned but not individually clinically described). …”

“… Note : Features of the two COG6‐CDG patients in our cohort (P1 and P2) and the previously published cases (R1:1, Cirnigliaro et al 6 ; R2:1, Ververi et al 7 ; R3:1, Zhao et al 8 ; R4:1, Lugli et al 10 ; R5:1, Lugli et al 9 ; R6:1, R6:2, Komlosi et al 11 ; R7:1, R7:2, Mandel et al 12 ; R8:1, Li et al 13 ; R9:1, Althonaian et al 14 ; R10:1, Wu et al 15 ; R11:1‐R11:7, Alsubhi et al 16 ; R12:1; Pérez‐Cerdá et al 17 ; R13:1‐R13:7, Rymen et al 18 ; R14:1, Shaheen et al 19 ; R15:1, Huybrechts et al 20 ; R16:1, Lubbehusen et al 21 In Shaheen et al, 19 11 more patients are mentioned but not individually clinically described). Abbreviations: ALT, alanine aminotransferase; aPTT, activated partial thromboplastin time; ASD, atrial septal defect; AST, aspartate aminotransferase; AV, aortic valve; BRP, birth‐related problems; CK, creatine kinase; DD, developmental delay; ep, epicanthal; F, female; FTT, failure to thrive; FXI, factor 11; HLH, hemophagocytic lymphohistiocytosis; ID, intellectual disability; IN, inverted nipples; LSE, low‐set ears; M, male; P, percentile; PDA, persistent ductus arteriosus; PFO, persistent foramen ovale; PT, prothrombin time; PVL, periventricular leukomalacia; SD, standard deviation; trc, thrombocytes; US, ultrasound; VSD, ventricular septal defect; WM, white matter; ‐, not present; +, present, N/R, not reported.…”

“…The mutations divide in seven missense, eight nonsense, and five splice variants (Figure 2 ). Homozygosity for p.Arg141* causes a particularly severe phenotype where the four published cases died within 40 days of age, 7 , 11 , 18 whereas Gly390Phefs*6 has a much milder clinical presentation (also known as Shaheen syndrome 19 ). Homozygous variants, suggesting consanguinity, were found in 32/43 patients.…”

“… 5 There are 16 publications totaling 41 patients with COG6‐CDG, of which 30 have clinical descriptions and 16 derive from two families (12 + 4). 6 , 7 , 8 , 9 , 10 , 11 , 12 , 13 , 14 , 15 , 16 , 17 , 18 , 19 , 20 , 21 Of the 41, only 9 presented with compound heterozygous variants, whereas the others were homozygous. The phenotype of COG6‐CDG varies between subjects, but is severe in a significant proportion with growth retardation, microcephaly, DD or ID, hypohidrosis, arthrogryposis, and 17/41 fatalities during the first 15 months of life.…”

“…The COG complex contains eight subunits, of which deficiencies in seven (all but COG3) have been described to cause a CDG 5 . There are 16 publications totaling 41 patients with COG6‐CDG, of which 30 have clinical descriptions and 16 derive from two families (12 + 4) 6–21 . Of the 41, only 9 presented with compound heterozygous variants, whereas the others were homozygous.…”

The SwedishCOG6‐CDGexperience and a comprehensive literature review

“… Note : Features of the two COG6‐CDG patients in our cohort (P1 and P2) and the previously published cases (R1:1, Cirnigliaro et al 6 ; R2:1, Ververi et al 7 ; R3:1, Zhao et al 8 ; R4:1, Lugli et al 10 ; R5:1, Lugli et al 9 ; R6:1, R6:2, Komlosi et al 11 ; R7:1, R7:2, Mandel et al 12 ; R8:1, Li et al 13 ; R9:1, Althonaian et al 14 ; R10:1, Wu et al 15 ; R11:1‐R11:7, Alsubhi et al 16 ; R12:1; Pérez‐Cerdá et al 17 ; R13:1‐R13:7, Rymen et al 18 ; R14:1, Shaheen et al 19 ; R15:1, Huybrechts et al 20 ; R16:1, Lubbehusen et al 21 In Shaheen et al, 19 11 more patients are mentioned but not individually clinically described). …”

“… Note : Features of the two COG6‐CDG patients in our cohort (P1 and P2) and the previously published cases (R1:1, Cirnigliaro et al 6 ; R2:1, Ververi et al 7 ; R3:1, Zhao et al 8 ; R4:1, Lugli et al 10 ; R5:1, Lugli et al 9 ; R6:1, R6:2, Komlosi et al 11 ; R7:1, R7:2, Mandel et al 12 ; R8:1, Li et al 13 ; R9:1, Althonaian et al 14 ; R10:1, Wu et al 15 ; R11:1‐R11:7, Alsubhi et al 16 ; R12:1; Pérez‐Cerdá et al 17 ; R13:1‐R13:7, Rymen et al 18 ; R14:1, Shaheen et al 19 ; R15:1, Huybrechts et al 20 ; R16:1, Lubbehusen et al 21 In Shaheen et al, 19 11 more patients are mentioned but not individually clinically described). Abbreviations: ALT, alanine aminotransferase; aPTT, activated partial thromboplastin time; ASD, atrial septal defect; AST, aspartate aminotransferase; AV, aortic valve; BRP, birth‐related problems; CK, creatine kinase; DD, developmental delay; ep, epicanthal; F, female; FTT, failure to thrive; FXI, factor 11; HLH, hemophagocytic lymphohistiocytosis; ID, intellectual disability; IN, inverted nipples; LSE, low‐set ears; M, male; P, percentile; PDA, persistent ductus arteriosus; PFO, persistent foramen ovale; PT, prothrombin time; PVL, periventricular leukomalacia; SD, standard deviation; trc, thrombocytes; US, ultrasound; VSD, ventricular septal defect; WM, white matter; ‐, not present; +, present, N/R, not reported.…”

“…The mutations divide in seven missense, eight nonsense, and five splice variants (Figure 2 ). Homozygosity for p.Arg141* causes a particularly severe phenotype where the four published cases died within 40 days of age, 7 , 11 , 18 whereas Gly390Phefs*6 has a much milder clinical presentation (also known as Shaheen syndrome 19 ). Homozygous variants, suggesting consanguinity, were found in 32/43 patients.…”

“… 5 There are 16 publications totaling 41 patients with COG6‐CDG, of which 30 have clinical descriptions and 16 derive from two families (12 + 4). 6 , 7 , 8 , 9 , 10 , 11 , 12 , 13 , 14 , 15 , 16 , 17 , 18 , 19 , 20 , 21 Of the 41, only 9 presented with compound heterozygous variants, whereas the others were homozygous. The phenotype of COG6‐CDG varies between subjects, but is severe in a significant proportion with growth retardation, microcephaly, DD or ID, hypohidrosis, arthrogryposis, and 17/41 fatalities during the first 15 months of life.…”

“…The COG complex contains eight subunits, of which deficiencies in seven (all but COG3) have been described to cause a CDG 5 . There are 16 publications totaling 41 patients with COG6‐CDG, of which 30 have clinical descriptions and 16 derive from two families (12 + 4) 6–21 . Of the 41, only 9 presented with compound heterozygous variants, whereas the others were homozygous.…”

The SwedishCOG6‐CDGexperience and a comprehensive literature review