Baby born with membrane around him at the time of birth. Which of the following conditions is depicted?

Lamellar ichthyosis (collodion membrane at birth)

X-linked ichthyosis (steroid sulfatase deficiency)

Generalized hyperkeratosis (thickened skin)

Ichthyosis vulgaris (dry, scaly skin)

Genetics in Dermatology for NEET-PG: High-Yield Dermatology Lessons

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Inheritance Patterns - Mendel's Skin Show

Pattern	Risk (Aff. Parent)	Risk (Carrier Parents)	Notes
AD	50%	-	Vertical; M=F. E.g., NF1. 📌 "Dominant Dads & Moms pass to 50%".
AR	-	25%	Horizontal; M=F. Consanguinity ↑. E.g., Albinism. 25% risk.
XLD	50% (mother); 100% daughters (father)	-	No male-to-male. Aff. father $\rightarrow$ all daughters. E.g., IP.
XLR	-	50% sons (carrier mother)	Males >> F. No male-to-male. E.g., Fabry.
Mito	100% (mother)	-	Maternal. All offspring of aff. mother. E.g., Kearns-Sayre.

Mosaicism: $\geq 2$ cell lines/individual.
Penetrance: % carriers show phenotype. (e.g., Incomplete)
Expressivity: Variable phenotype, same genotype.
Anticipation: Earlier onset / ↑ severity in generations.
Pleiotropy: 1 gene, many effects.

⭐ AD: New mutations common; affected usually heterozygous. """

Keratin & Adhesion Defects - Faulty Scaffolding

Ichthyoses (Cornification Disorders):
- Vulgaris: FLG (filaggrin); fine scales, hyperlinear palms.
- X-linked: STS (steroid sulfatase); dark scales, "dirty neck".
- Lamellar: TGM1 (transglutaminase-1); collodion baby, ectropion.
- Epidermolytic Hyperkeratosis (EHK/Bullous CIE): KRT1/KRT10; birth blisters, then hyperkeratosis.

Epidermolysis Bullosa (EB) (Blistering Disorders): 📌 EB Layers Mnemonic: Simple Epidermis, Junctional Lamina Lucida, Dystrophic Dermis.

EB Type	Protein (Gene)	Level	Inheritance	Feature
Simplex	Keratin 5/14 (KRT5/14)	Intraepidermal	AD	Non-scarring blisters
Junctional	Laminin-332 (LAMA3/B3/C2)	Lamina Lucida	AR	Severe, high mortality
Dystrophic	Collagen VII (COL7A1)	Sublamina Densa	AD/AR	Scarring, milia, mitten deformity
Kindler	Kindlin-1 (FERMT1)	Multiple levels	AR	Blisters, poikiloderma, photosensitivity

Skin layers and protein locations in Epidermolysis Bullosa

⭐ In Dystrophic EB, recurrent blistering and scarring can lead to pseudosyndactyly (mitten deformity) and an ↑ risk of squamous cell carcinoma.

Neurocutaneous & Pigmentary Syndromes - Brain-Skin Signals

Syndrome	Gene(s)	Key Skin	Key Systemic/Eye
Neurofibromatosis 1	NF1	≥6 Café-au-lait, Axillary freckling, Neurofibromas (≥2 or 1 plexiform)	≥2 Lisch nodules, Optic glioma
Neurofibromatosis 2	NF2	Cutaneous schwannomas	Bilateral vestibular schwannomas (diagnostic), Meningiomas
Tuberous Sclerosis	TSC1/TSC2	≥3 Ash-leaf spots, Angiofibromas, Shagreen patch	Cortical dysplasias, SEGA, Renal AML

Pigmentary Disorders:
- Oculocutaneous Albinism (OCA): TYR (OCA1). ↓Melanin, nystagmus.
- Hermansky-Pudlak Syndrome: OCA + bleeding, lung fibrosis.
- Chediak-Higashi Syndrome: OCA + immunodeficiency, giant granules.
- Piebaldism: KIT gene. White forelock, stable depigmented patches.
- Waardenburg Syndrome: PAX3, MITF. White forelock, dystopia canthorum, deafness.

⭐ Bilateral vestibular schwannomas are diagnostic of Neurofibromatosis Type 2.

Genetic Testing & Counseling - Future Derm Maps

Indications: Suspected genodermatosis, positive family history, pre-conception/prenatal queries.
Testing Methods:
- Karyotyping, FISH, Chromosomal Microarray (CMA).
- Sanger sequencing (targeted genes).
- NGS: Whole Exome (WES) / Whole Genome (WGS) for diagnostic odysseys.
Genetic Counseling:
- Core: Non-directiveness, risk assessment, psychosocial support.
- Includes prenatal diagnosis options (e.g., CVS, amniocentesis).

⭐ Whole Exome Sequencing (WES) is a high-yield NGS technique for identifying causative mutations in undiagnosed genodermatoses.

High‑Yield Points - ⚡ Biggest Takeaways

Autosomal Dominant (AD): Common in NF1, Tuberous Sclerosis, Darier disease. Remember variable expressivity.

Autosomal Recessive (AR): Key for Xeroderma Pigmentosum, Albinism, most Epidermolysis Bullosa (EB) types.

X-linked Recessive: Includes Anhidrotic Ectodermal Dysplasia, Wiskott-Aldrich syndrome.

X-linked Dominant: Incontinentia Pigmenti is a classic example.

FLG (Filaggrin) gene: Mutations cause Ichthyosis Vulgaris and predispose to Atopic Dermatitis.

KRT (Keratin) genes: Mutations lead to Epidermolysis Bullosa Simplex.

Mosaicism explains some sporadic genodermatoses and varied presentations.

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Genetics in Dermatology