Relationship between gene expression associated with cellular senescence in cells from discarded wound dressings and wound healing: A retrospective cohort study

IF 2.4 3区 医学 Q2 DERMATOLOGY Journal of tissue viability Pub Date : 2024-11-01 Epub Date: 2024-07-22 DOI:10.1016/j.jtv.2024.07.014
Chihiro Takizawa , Qi Qin , Daijiro Haba , Sanae Sasaki , Akiko Kawasaki , Tomomi Miyake , Jun Oba , Aya Kitamura , Mari Abe , Sanai Tomida , Gojiro Nakagami
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Abstract

Aim

Senescent cells, inducing a senescence-associated secretory phenotype (SASP), lead to chronic inflammation in hard-to-heal wound tissue. However, eliminating senescent cells may impede normal wound healing due to their important role in the wound healing mechanism. Accordingly, we focused on wound exudates in hard-to-heal wounds, which contain many inflammation biomarkers consistent with SASP. Therefore, we hypothesized that senescent cells might be present in the exudates and induce chronic inflammation. This study investigated the relationship between gene expression associated with cellular senescence in exudates from pressure injuries and wound healing status.

Methods

This retrospective cohort study involved patients treated by a pressure injury team. We collected viable cells from wound dressings and analyzed gene expression. Pearson's correlation coefficient was calculated between cellular senescence and SASP expression. The relationship between the gene expression of cellular senescence and the wound area reduction rate by the following week was examined using a mixed-effects model.

Results

CDKN1A—related to cellular senescence—was expressed in 96.3 % of 54 samples, and CDKN1A expression and SASPs positively correlated (PLAU: r = 0.68 and TNF: r = 0.34). Low CDKN1A expression was statistically associated with a large wound area reduction rate (β = 0.83, p < 0.01).

Conclusions

Gene expression of both cellular senescence and SASP factor in wound dressings suggests the presence of cellular senescence. Senescent cells in wound dressings could be associated with delayed wound healing in the following week.
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废弃伤口敷料细胞中与细胞衰老相关的基因表达与伤口愈合之间的关系:回顾性队列研究
衰老细胞,诱导衰老相关的分泌表型(SASP),导致难以愈合的伤口组织的慢性炎症。然而,由于衰老细胞在伤口愈合机制中的重要作用,清除衰老细胞可能会阻碍正常的伤口愈合。因此,我们将重点放在难以愈合伤口的伤口渗出物上,这些伤口渗出物含有许多与SASP一致的炎症生物标志物。因此,我们假设衰老细胞可能存在于渗出液中并诱导慢性炎症。本研究探讨了压伤渗出液中与细胞衰老相关的基因表达与伤口愈合状态的关系。方法本研究采用回顾性队列研究,纳入了在压力损伤组治疗的患者。我们从伤口敷料中收集活细胞并分析基因表达。计算细胞衰老与SASP表达之间的Pearson相关系数。采用混合效应模型研究细胞衰老基因表达与周后创面缩小率的关系。结果与细胞衰老相关的scdkn1a在54份样本中的表达率为96.3%,且CDKN1A表达与SASPs呈正相关(PLAU: r = 0.68, TNF: r = 0.34)。CDKN1A低表达与大创面减少率有统计学意义(β = 0.83, p <;0.01)。结论创面敷料中细胞衰老和SASP因子的基因表达均提示细胞衰老的存在。伤口敷料中的衰老细胞可能与随后一周的伤口愈合延迟有关。
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来源期刊
Journal of tissue viability
Journal of tissue viability DERMATOLOGY-NURSING
CiteScore
3.80
自引率
16.00%
发文量
110
审稿时长
>12 weeks
期刊介绍: The Journal of Tissue Viability is the official publication of the Tissue Viability Society and is a quarterly journal concerned with all aspects of the occurrence and treatment of wounds, ulcers and pressure sores including patient care, pain, nutrition, wound healing, research, prevention, mobility, social problems and management. The Journal particularly encourages papers covering skin and skin wounds but will consider articles that discuss injury in any tissue. Articles that stress the multi-professional nature of tissue viability are especially welcome. We seek to encourage new authors as well as well-established contributors to the field - one aim of the journal is to enable all participants in tissue viability to share information with colleagues.
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