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Gremlin 2抑制人类皮肤中干细胞/祖细胞的分化。

Gremlin 2 suppresses differentiation of stem/progenitor cells in the human skin.

作者信息

Kawagishi-Hotta Mika, Hasegawa Seiji, Inoue Yu, Hasebe Yuichi, Arima Masaru, Iwata Yohei, Sugiura Kazumitsu, Akamatsu Hirohiko

机构信息

Research Laboratories, Nippon Menard Cosmetic Co., LTD., Japan.

Nagoya University-MENARD Collaborative Research Chair, Nagoya University Graduate School of Medicine, Japan.

出版信息

Regen Ther. 2021 Jul 12;18:191-201. doi: 10.1016/j.reth.2021.06.007. eCollection 2021 Dec.

Abstract

INTRODUCTION

The skin is comprised of various kinds of cells and has three layers, the epidermis, dermis and subcutaneous adipose tissue. Stem cells in each tissue duplicate themselves and differentiate to supply new cells that function in the tissue, and thereby maintain the tissue homeostasis. In contrast, senescent cells accumulate with age and secrete senescence-associated secretory phenotype (SASP) factors that impair surrounding cells and tissues, which lowers the capacity to maintain homeostasis in each tissue. Previously, we found Gremlin 2 (GREM2) as a novel SASP factor in the skin and reported that GREM2 suppressed the differentiation of adipose-derived stromal/stem cells. In the present study, we investigated the effects of GREM2 on stem cells in the epidermis and dermis.

METHODS

To examine whether GREM2 expression and the differentiation levels in the epidermis and dermis are correlated, the expressions of GREM2, stem cell markers, an epidermal differentiation marker Keratin 10 (KRT10) and a dermal differentiation marker type 3 procollagen were examined in the skin samples (n = 14) randomly chosen from the elderly where GREM2 expression level is high and the individual differences of its expression are prominent. Next, to test whether GREM2 affects the differentiation of skin stem cells, cells from two established lines (an epidermal and a dermal stem/progenitor cell model) were cultured and induced to differentiate, and recombinant GREM2 protein was added.

RESULTS

In the human skin, the expression levels of GREM2 varied among individuals both in the epidermis and dermis. The expression level of GREM2 was not correlated with the number of stem cells, but negatively correlated with those of both an epidermal and a dermal differentiation markers. The expression levels of epidermal differentiation markers were significantly suppressed by the addition of GREM2 in the three-dimensional (3D) epidermis generated with an epidermal stem/progenitor cell model. In addition, by differentiation induction, the expressions of dermal differentiation markers were induced in cells from a dermal stem/progenitor cell model, and the addition of GREM2 significantly suppressed the expressions of the dermal differentiation markers.

CONCLUSIONS

GREM2 expression level did not affect the numbers of stem cells in the epidermis and dermis but affects the differentiation and maturation levels of the tissues, and GREM2 suppressed the differentiation of stem/progenitor cells . These findings suggest that GREM2 may contribute to the age-related reduction in the capacity to maintain skin homeostasis by suppressing the differentiation of epidermal and dermal stem/progenitor cells.

摘要

引言

皮肤由多种细胞组成,有三层结构,即表皮、真皮和皮下脂肪组织。每个组织中的干细胞自我复制并分化,以提供在该组织中发挥功能的新细胞,从而维持组织的稳态。相反,衰老细胞会随着年龄的增长而积累,并分泌衰老相关分泌表型(SASP)因子,这些因子会损害周围的细胞和组织,进而降低每个组织维持稳态的能力。此前,我们发现Gremlin 2(GREM2)是皮肤中一种新的SASP因子,并报道GREM2可抑制脂肪来源的基质/干细胞的分化。在本研究中,我们研究了GREM2对表皮和真皮中干细胞的影响。

方法

为了研究GREM2表达与表皮和真皮中分化水平是否相关,在从老年人中随机选取的皮肤样本(n = 14)中检测了GREM2、干细胞标志物、表皮分化标志物角蛋白10(KRT10)和真皮分化标志物Ⅲ型前胶原的表达,这些样本中GREM2表达水平较高且个体差异显著。接下来,为了测试GREM2是否影响皮肤干细胞的分化,培养了两个已建立细胞系(一个表皮和一个真皮干细胞/祖细胞模型)的细胞并诱导其分化,并添加了重组GREM2蛋白。

结果

在人类皮肤中,GREM2在表皮和真皮中的表达水平因个体而异。GREM2的表达水平与干细胞数量无关,但与表皮和真皮分化标志物的表达呈负相关。在由表皮干细胞/祖细胞模型生成的三维(3D)表皮中添加GREM2后,表皮分化标志物的表达水平受到显著抑制。此外,通过诱导分化,在真皮干细胞/祖细胞模型的细胞中诱导了真皮分化标志物的表达,而添加GREM2显著抑制了真皮分化标志物的表达。

结论

GREM2表达水平不影响表皮和真皮中干细胞的数量,但影响组织的分化和成熟水平,并且GREM2抑制干细胞/祖细胞的分化。这些发现表明,GREM2可能通过抑制表皮和真皮干细胞/祖细胞的分化,导致与年龄相关的皮肤稳态维持能力下降。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/56e2/8280529/72fd2b9ecad3/gr1.jpg

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