Age‐specific hormonal decline is accompanied by transcriptional changes in human sebocytes <i>in vitro</i>

Makrantonaki, Evgenia; Adjaye, James; Herwig, Ralf; Brink, Thore C.; Groth, Detlef; Hultschig, Claus; Lehrach, Hans; Zouboulis, Christos C.

doi:10.1111/j.1474-9726.2006.00223.x

Cited by 103 publications

(86 citation statements)

References 74 publications

(78 reference statements)

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“…Though not proven, these results might imply that a disturbed hormone status might induce the regulation of these genes and the generation of neurodegenerative diseases (Makrantonaki et al, 2006).…”

Section: Skin and Cns -mentioning

confidence: 99%

Skin and brain age together: The role of hormones in the ageing process

Makrantonaki

Schönknecht

Hossini

et al. 2010

Experimental Gerontology

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The importance of the endocrine environment in the initiation of the ageing process has been elucidated in several in vivo an in vitro studies. Changes in endocrine pathways accompany healthy ageing, these include the growth hormone /insulin like growth factor-I axis (somatopause) and that of sexual hormones, namely estradiol (menopause), testosterone (andropause), and dehydroepiandrosterone and its sulphate (adrenopause). The clinical significance of these changes is variable and results in morphological and functional alterations of all organ systems including the skin and the central nervous system. Moreover, the pathogenesis of age-associated diseases such as epithelial skin cancer and neurodegenerative diseases has been partly attributed to the lack of hormones. Several studies have been conducted in an attempt to reverse the ageing process and clinical signs by substitution of the serum hormone levels in older individuals, however the benefits of hormone replacement therapy, if any, are still controversial. On the other hand, recent data suggest that skin is a window to the human organism and represents an adequate model for ageing research, also implying the use of skin samples for evaluating the ageing status of the central nervous system.

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Section: Skin and Cns -mentioning

confidence: 99%

Skin and brain age together: The role of hormones in the ageing process

Makrantonaki

Schönknecht

Hossini

et al. 2010

Experimental Gerontology

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“…46 Recent data suggest that incubation of human sebaceous gland cells with a hormone mixture consisting of growth factors and sex steroids at age-specific levels may alter the biological activity of the cells by regulating their transcriptome and thus illustrate the importance of the hormone environment for cell function. 58 Human SZ95 sebocytes treated with hormone levels that can be found in 60 year-old women produce less lipids than sebocytes treated with a hormone mixture representing that found in serum of 20 year-old women. 58 Gene expression profiling via cDNA microarray between SZ95 sebocytes under the 20 and 60 year-old hormone mixture detected differentially expressed genes, which are involved in biological processes such as DNA repair and stability, mitochondrial function, oxidative stress, cell cycle and apoptosis, ubiquitin-induced proteolysis and transcriptional regulation.…”

Section: Effects Of Hormones On Sebaceous Gland Cellsmentioning

confidence: 99%

“…58 Human SZ95 sebocytes treated with hormone levels that can be found in 60 year-old women produce less lipids than sebocytes treated with a hormone mixture representing that found in serum of 20 year-old women. 58 Gene expression profiling via cDNA microarray between SZ95 sebocytes under the 20 and 60 year-old hormone mixture detected differentially expressed genes, which are involved in biological processes such as DNA repair and stability, mitochondrial function, oxidative stress, cell cycle and apoptosis, ubiquitin-induced proteolysis and transcriptional regulation. The most significantly altered signalling pathway was that of transforming growth factor-β (TGFβ).…”

Section: Effects Of Hormones On Sebaceous Gland Cellsmentioning

confidence: 99%

An update on the role of the sebaceous gland in the pathogenesis of acne

Makrantonaki

Gancevičienė²,

Zouboulis³

2011

Dermato-Endocrinology

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206

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“…Several mitochondrial modifications occur within differentiated somatic cells during aging [29]. Indeed, transcriptome analysis of human skin aging has identified specific alterations in pathways related to mitochondria and oxidative stress [30]. mtDNA undergoes a high rate of mutation, due to elevated ROS levels and the lack of histones and efficient repairing mechanisms.…”

Section: Introductionmentioning

confidence: 99%

The Senescence-Related Mitochondrial/Oxidative Stress Pathway is Repressed in Human Induced Pluripotent Stem Cells

et al. 2010

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The ability of stem cells to propagate indefinitely is believed to occur via the fine modulation of pathways commonly involved in cellular senescence, including the telomerase, the p53, and the mitochondrial/oxidative stress pathways. Induced pluripotent stem cells (iPSCs) are a novel stem cell population obtained from somatic cells through forced expression of a set of genes normally expressed in embryonic stem cells (ESCs). These reprogrammed cells acquire self-renewal properties and appear almost undistinguishable from ESCs in terms of morphology, gene expression, and differentiation potential. Accordingly, iPSCs exhibit alterations of the senescence-related telomerase and p53 signaling pathways. However, although treatments with antioxidants have been recently shown to enhance cellular reprogramming, detailed information regarding the state of the mitochondrial/oxidative stress pathway in iPSCs is still lacking. Mitochondria undergo specific changes during organismal development and aging. Thus, addressing whether somatic mitochondria within iPSCs acquire ESC-like features or retain the phenotype of the parental cell is an unanswered but relevant question. Herein, we demonstrate that somatic mitochondria within human iPSCs revert to an immature ESC-like state with respect to organelle morphology and distribution, expression of nuclear factors involved in mitochondrial biogenesis, content of mitochondrial DNA, intracellular ATP level, oxidative damage, and lactate generation. Upon differentiation, mitochondria within iPSCs and ESCs exhibited analogous maturation and anaerobic-to-aerobic metabolic modifications. Overall, the data highlight that human iPSCs and ESCs, although not identical, share similar mitochondrial properties and suggest that cellular reprogramming can modulate the mitochondrial/oxidative stress pathway, thus inducing a rejuvenated state capable of escaping cellular senescence.

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Age‐specific hormonal decline is accompanied by transcriptional changes in human sebocytes in vitro

Cited by 103 publications

References 74 publications

Skin and brain age together: The role of hormones in the ageing process

Skin and brain age together: The role of hormones in the ageing process

An update on the role of the sebaceous gland in the pathogenesis of acne

The Senescence-Related Mitochondrial/Oxidative Stress Pathway is Repressed in Human Induced Pluripotent Stem Cells

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