Second-Hit, Postzygotic <i>PMVK</i> and <i>MVD</i> Mutations in Linear Porokeratosis

Atzmony, Lihi; Khan, H.; Lim, Young Hee; Paller, Amy S.; Levinsohn, Jonathan L.; Holland, Kristen E.; Mirza, Fatima N.; Yin, Emily S.; Ko, Christine J.; Leventhal, Jonathan S.; Choate, Keith

doi:10.1001/jamadermatol.2019.0016

Cited by 61 publications

(68 citation statements)

References 31 publications

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“…We thus confirmed the recent report of Atzmony et al (2019) showing second hit genetic changes in the skin lesions of patients with LP with monoallelic germline mutations in MVD or MVK. Next, we explored whether second hit genetic changes were evident in the skin lesions of patients with DSAP.…”

Section: Resultssupporting

confidence: 91%

“…Congenital heterozygous mutations in genes encoding enzymes of the mevalonate pathway, including MVD and MVK, are responsible for familial and sporadic DSAP and LP Zhang et al, 2015). The coexistence of DSAP and LP in single patients or families suggests that acquired second hit genetic changes in those with monoallelic, pathogenic mutations underlie the development of porokeratosis (Commens and Shumack, 1987;Happle, 1991); such second hit changes were recently identified in the MVD or MVK genes of three patients with LP (Atzmony et al, 2019).…”

Section: Introductionmentioning

confidence: 99%

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Clonal Expansion of Second-Hit Cells with Somatic Recombinations or C>T Transitions Form Porokeratosis in MVD or MVK Mutant Heterozygotes

Kubo

Sasaki

Suzuki

et al. 2019

Journal of Investigative Dermatology

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Patients with disseminated superficial actinic porokeratosis (DSAP) and linear porokeratosis (LP) exhibit monoallelic germline mutations in genes encoding mevalonate pathway enzymes, such as MVD or MVK. Here, we showed that each skin lesion of DSAP exhibited an individual second hit genetic change in the wild-type allele of the corresponding gene specifically in the epidermis, indicating that a postnatal second hit triggering biallelic deficiency of the gene is required for porokeratosis to develop. Most skin lesions exhibited one of two principal second hits, either somatic homologous recombinations rendering the monoallelic mutation biallelic or C>T transition mutations in the wild-type allele. The second hits differed among DSAP lesions but were identical in those of congenital LP, suggesting that DSAP is attributable to sporadic postnatal second hits and congenital LP to a single second hit in the embryonic period. In the characteristic annular skin lesions of DSAP, the central epidermis featured mostly second hit keratinocytes, and that of the annular ring featured a mixture of such cells and naïve keratinocytes, implying that each lesion reflects the clonal expansion of single second hit keratinocytes. DSAP is therefore a benign intraepidermal neoplasia, which can be included in the genetic tumor disorders explicable by Knudson's two-hit hypothesis.

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Section: Resultssupporting

confidence: 91%

Section: Introductionmentioning

confidence: 99%

Clonal Expansion of Second-Hit Cells with Somatic Recombinations or C>T Transitions Form Porokeratosis in MVD or MVK Mutant Heterozygotes

Kubo

Sasaki

Suzuki

et al. 2019

Journal of Investigative Dermatology

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“…Genetic inheritance patterns for enzyme deficiency are typically recessive and the result of "loss-of-function" mutations. Second-hit genetic mosaicism is a rare cause of enzymatic loss of function, and Kubo et al (2019) confirm recent findings that second-hit postzygotic mutations or homologous recombination in mevalonate pathway genes cause the mosaic presentation of porokeratosis-LP (Atzmony et al, 2019). They further show that the autosomal dominant disorder DSAP, which typically presents with lesions later in life also results from second-hit mutations of the remaining wild-type allele.…”

supporting

confidence: 80%

Second-Hit Somatic Mutations in Mevalonate Pathway Genes Underlie Porokeratosis

Atzmony

Choate

2019

Journal of Investigative Dermatology

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Familial and sporadic porokeratosis are associated with germline heterozygous mutations in mevalonate pathway genes. Kubo et al. show that each skin lesion of disseminated superficial actinic porokeratosis originates from a postnatal keratinocyte clone with a different second-hit genetic event in the wild-type allele of the corresponding gene. They also confirm that linear porokeratosis derives from a single prenatal clone of keratinocytes with a second-hit genetic event.

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“…This study also highlights the difficulties in genetic analysis of mosaic disorders. In contrast to the inherited EHK‐associated dermatoses, wherein germline mutation results in the genetic change being readily detectable in DNA extracted from the blood via Sanger sequencing, genetic changes underlying mosaic disorders are detected only in the lesional tissue itself . Even when lesional tissue is utilized, admixture from neighboring cell types, as well as wild‐type cells of the same lineage, can lead to a low mutant allele fraction that cannot be readily detected via traditional capillary‐based sequencing technologies .…”

Section: Discussionmentioning

confidence: 99%

Mutations in KRT10 in epidermolytic acanthoma

et al. 2020

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Background: Epidermolytic acanthoma (EA) is a rare acquired lesion demonstrating a characteristic histopathological pattern of epidermal degeneration referred to as epidermolytic hyperkeratosis (EHK). On histopathological analysis, EA appears nearly identical to inherited EHK-associated dermatoses such as epidermolytic ichthyosis and ichthyosis bullosa of Siemens. While it has been speculated that EA is caused by mutations in KRT10, KRT1, or KRT2 found in these inherited dermatoses, none have yet been identified. Herein, we aim to identify the contributions of keratin mutations to EA.Methods: Using genomic DNA extracted from paraffin-embedded samples from departmental archives, we evaluated a discovery cohort using whole-exome sequencing (WES) and assessed remaining samples using Sanger sequencing screening and restriction fragment length polymorphism (RFLP) analysis. Results: DNA from 16/20 cases in our sample was of sufficient quality for polymerase chain reaction amplification. WES of genomic DNA from lesional tissue revealed KRT10 c.466C > T, p.Arg156Cys mutations in 2/3 samples submitted for examination. RFLP analysis of these samples as well as eight additional samples confirmed the mutations identified via WES and identified four additional cases with Arg156 mutations. In sum, 6/11 screened cases showed hotspot mutation in KRT10. Conclusions: Hotspot mutations in the Arg156 position of KRT10, known to cause epidermolytic ichthyosis, also underlie EA. K E Y W O R D S epidermolytic acanthoma, keratin 10, KRT10, mutations, whole-exome sequencing

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Second-Hit, Postzygotic PMVK and MVD Mutations in Linear Porokeratosis

Cited by 61 publications

References 31 publications

Clonal Expansion of Second-Hit Cells with Somatic Recombinations or C>T Transitions Form Porokeratosis in MVD or MVK Mutant Heterozygotes

Clonal Expansion of Second-Hit Cells with Somatic Recombinations or C>T Transitions Form Porokeratosis in MVD or MVK Mutant Heterozygotes

Second-Hit Somatic Mutations in Mevalonate Pathway Genes Underlie Porokeratosis

Mutations in KRT10 in epidermolytic acanthoma

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