Lipid abnormalities in atopic skin are driven by type 2 cytokines

Berdyshev, Evgeny; Goleva, Elena; Bronova, Irina; Dyjack, Nathan; Rios, Cydney; Jung, John; Taylor, Patricia A.; Jeong, Mi Young; Hall, Clifton F.; Richers, Brittany; Norquest, Kathryn A.; Zheng, Tao; Seibold, Max A.; Leung, Donald Y.M.

doi:10.1172/jci.insight.98006

Cited by 190 publications

(232 citation statements)

References 40 publications

Supporting

Mentioning

212

Contrasting

Unclassified

Order By: Relevance

“…ELOVL3‐ablated mice showed skin dysfunction and no obvious fatty acid with more than 20 carbons . Both ELOVL3 and ELOVL6 are downregulated in the stratum corneum of atopic dermatitis patients, which had significant effects on the proportion of skin lipids, especially long‐chain fatty acids . Human skin sebum is unique in its fatty acid profile, with the highest monounsaturated being sapienic acid (16:1n‐10) produced by action of FADS2 on 16:0 .…”

Section: Discussionmentioning

confidence: 99%

Identification of genes mediating branched chain fatty acid elongation

Wang

Park

et al. 2019

FEBS Letters

View full text Add to dashboard Cite

Saturated branched chain fatty acids (BCFA) terminating with either a prop‐2‐yl (iso) or sec‐butan‐2‐yl (anteiso) group are common bioactive food components consumed from beef, fish, and dairy products. Little is known about the endogenous metabolism of BCFA and the enzymes mediating their interconversions. By using transient transfection studies, we report for the first time the substrate specificity of the elongase of very long chain fatty acids (ELOVL)1‐7 toward anteiso‐15:0 and iso‐18:0, and assessed competition between BCFA and normal saturated fatty acids (n‐SFA). ELOVL6 mediates elongation of anteiso‐15:0→anteiso‐17:0, while ELOVL3 is active toward iso‐18:0→iso‐20:0. Competition studies reveal n‐16:0 competes with anteiso‐15:0 for ELOVL6, while n‐18:0 competes with iso‐18:0 for ELOVL3. These competitions for elongation may have implications in specialized tissues where both BCFA and n‐SFA are present at comparable levels.

show abstract

Section: Discussionmentioning

confidence: 99%

Identification of genes mediating branched chain fatty acid elongation

Wang

Park

et al. 2019

FEBS Letters

View full text Add to dashboard Cite

show abstract

“…PC and PE are lipids known to enhance barrier function, provide direct and indirect protection against S. aureus, and modulate skin immunity (17,(31)(32)(33)(34). Furthermore, while the bioactivities of PC and PE with these specific acyl chains have not been assessed, recent studies have demonstrated that abnormalities in skin lipid content and metabolism are strongly associated with AD (35,36). Taken together with our clinical findings, these data suggest that repairing the strain-level dysbiosis in R. mucosa in patients with AD could R. mucosa growth is impacted by environmental exposures.…”

Section: R Mucosa Was Associated With Clinical Improvement and Safetmentioning

confidence: 99%

First-in-human topical microbiome transplantation with Roseomonas mucosa for atopic dermatitis

et al. 2018

View full text Add to dashboard Cite

“…2). Th2 cytokines further compromise the barrier by downregulating the synthesis of: (i) epidermal structural proteins [19], (ii) tight-junction proteins [20], (iii) ceramides [21], (iv) fatty acid elongases [22], and (v) a key antimicrobial peptide, LL-37 [23]. Hence, the initial outside-to-inside cytokine cascade in AD quickly morphs into an “outside-to-inside back to outside” vicious circle [24].…”

Section: Barrier-based Pathogenesis Of Admentioning

confidence: 99%

Moisturizers versus Current and Next-Generation Barrier Repair Therapy for the Management of Atopic Dermatitis

Elias¹,

Wakefield²,

Man³

2018

Skin Pharmacol Physiol

View full text Add to dashboard Cite

We compare here the principal characteristics of over-the-counter moisturizers with physiologic lipid-based barrier repair therapy. Moisturizers are standard ancillary therapy for anti-inflammatory skin disorders, like atopic dermatitis (AD), and can attenuate the emergence of AD, the initial step in the “atopic march.” But not all moisturizers are beneficial; some can make skin function worse, and can even induce inflammation, possibly accounting for the frequent occurrence of “sensitive skin” in women. In contrast, physiologic lipid-based barrier repair therapy, if comprised of the 3 key stratum corneum lipids, in sufficient quantities and at an appropriate molar ratio, can correct the barrier abnormality and reduce inflammation in AD, and perhaps in other inflammatory dermatoses.

show abstract

Lipid abnormalities in atopic skin are driven by type 2 cytokines

Cited by 190 publications

References 40 publications

Identification of genes mediating branched chain fatty acid elongation

Identification of genes mediating branched chain fatty acid elongation

First-in-human topical microbiome transplantation with Roseomonas mucosa for atopic dermatitis

Moisturizers versus Current and Next-Generation Barrier Repair Therapy for the Management of Atopic Dermatitis

Contact Info

Product

Resources

About