Biallelic GLTP mutations cause nonsyndromic epidermal differentiation disorder via disrupted epidermal glucosylceramide transport
Zeqiao Zhang, Shimiao Huang, Adam Jackson, Elizabeth A Jones, Siddharth Banka, Chao Yang, Sisi Zhao, Kunlun Lv, Sha Peng, Zhimiao Lin, Huijun Wang
Zeqiao Zhang, Shimiao Huang, Adam Jackson, Elizabeth A Jones, Siddharth Banka, Chao Yang, Sisi Zhao, Kunlun Lv, Sha Peng, Zhimiao Lin, Huijun Wang
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Research Article Dermatology Genetics Metabolism

Biallelic GLTP mutations cause nonsyndromic epidermal differentiation disorder via disrupted epidermal glucosylceramide transport

Abstract

Ceramides are essential skin lipids for maintaining the mammalian skin permeability barrier, which protects against external stimuli. The precursor of epidermal ceramides, glucosylceramides (GlcCer), is synthesized within granular keratinocytes while its precise cellular transport mechanisms remain poorly characterized. Here, we identified 3 pathogenic variants in the GLTP gene, which encodes glycolipid transfer protein, in 5 unrelated families with nonsyndromic epidermal differentiation disorder presenting with generalized skin scaling. The biallelic GLTP variants resulted in loss of competent GLTP expression. CRISPR/Cas9-generated Gltp-knockout mice exhibited lethal barrier defects, partially recapitulating the clinical features of our patients. We demonstrated that GLTP facilitated GlcCer transport in differentiated keratinocytes, with its deficiency causing impaired GlcCer trafficking and consequent aberrant retention in lysosomes, thereby disrupting lysosome function. The lysosomal dysfunction impaired autophagy flux, resulting in delayed keratinocyte terminal differentiation, which is expected to compromise the skin barrier integrity and ultimately lead to abnormal scaling. Pharmacological inhibition of GlcCer synthesis effectively rescued both autophagy and keratinocyte differentiation defects. Our findings establish GLTP as a novel underlying gene for nonsyndromic epidermal differentiation disorders and unravel its essential role in maintaining skin homeostasis during terminal differentiation by mediating epidermal GlcCer transport.

Authors

Zeqiao Zhang, Shimiao Huang, Adam Jackson, Elizabeth A Jones, Siddharth Banka, Chao Yang, Sisi Zhao, Kunlun Lv, Sha Peng, Zhimiao Lin, Huijun Wang

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Figure 1

Clinical manifestations and histopathological findings of patients with nEDD.

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Clinical manifestations and histopathological findings of patients with ...
(A) Pedigrees of the 5 nEDD families with individuals (solid symbols) carrying biallelic GLTP variants. Slashes, deceased individuals; double horizontal lines, consanguinity; arrows, probands. (B) P1 exhibits generalized, brownish-to-gray scales on the neck and trunk. P2 shows dry, thickened skin with fine scales on the legs. Large, plate-like, geometric scales are prominent on the legs of P3 and P4. Affected family members (P5, P6) demonstrate widespread ichthyosis featuring marked hyperkeratosis and hyperpigmentation in flexural areas. (C) H&E staining of skin biopsies from P1 and P2 shows hyperplasia with focal parakeratosis, thickened stratum granulosum layer with numerous intracellular vacuoles, and mild perivascular lymphocytic infiltration in the superficial dermis. Scale bars: 100 μm.