The expression of P16 and S100 associated with elastin degradation and fibrosis of the Ligamentum Flavum hypertrophy

The expression of P16 and S100 associated with elastin degradation and fibrosis of the Ligamentum Flavum hypertrophy

Abstract Background One of the characteristics of lumbar spinal stenosis (LSS) is elastin degradation and fibrosis in the ligamentum flavum (LF). However, the biochemical factors that cause these histologic changes is unclear. P16 and S100 participate in scar formation and collagen development in wo...

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Main Authors: Wei Hu, Shunli Kan, Guang Liu, Zegang Cao, Rusen Zhu
Format: Article
Language:English
Published: BMC 2019-10-01
Series:BMC Musculoskeletal Disorders
Subjects:
Ligamentum Flavum
Hypertrophy
Histology
Spinal stenosis
Elastin
Fibrosis
Online Access:http://link.springer.com/article/10.1186/s12891-019-2825-4
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spelling doaj-a86b09ce1a854188b2baaa5ccd42b4ff2020-11-25T03:59:58ZengBMCBMC Musculoskeletal Disorders1471-24742019-10-012011810.1186/s12891-019-2825-4The expression of P16 and S100 associated with elastin degradation and fibrosis of the Ligamentum Flavum hypertrophyWei Hu0Shunli Kan1Guang Liu2Zegang Cao3Rusen Zhu4Department of Spine Surgery, Tianjin Union Medical CenterDepartment of Spine Surgery, Tianjin Union Medical CenterDepartment of Pathology, Tianjin Union Medical CenterDepartment of Spine Surgery, Tianjin Union Medical CenterDepartment of Spine Surgery, Tianjin Union Medical CenterAbstract Background One of the characteristics of lumbar spinal stenosis (LSS) is elastin degradation and fibrosis in the ligamentum flavum (LF). However, the biochemical factors that cause these histologic changes is unclear. P16 and S100 participate in scar formation and collagen development in wound healing and fibrosis diseases. In this study, we investigate the association between P16 and S100 expression and the fibrosis of the hypertrophic LF in LSS. Methods The LF specimens were surgically obtained from 30 patients with single-segment LSS (SLSS), 30 patients with double-segment LSS (DLSS) and 30 patients with L4/5 lumbar disc herniation (LDH). The LF thickness was measured by axial T1-weighted MRI. The extent of LF elastin degradation and fibrosis were graded based on hematoxylin-eosin (HE) and Verhoff’s Van Gieson’s (VVG) stain, respectively. The localization of P16 and S100 was determined by immunohistochemistry. Results The Absolute and relative LF thickness were greater in the DLSS group compared with the SLSS and LDH groups (p <  0.05). The elastic tissue from the dorsal aspect to the dural aspect in SLSS and DLSS groups was significantly increased. The amount of collagen deposition and elastic tissue is significantly higher in the DLSS group compared with the SLSS and LDH groups (p <  0.05). The specimens in the DLSS group showed positive staining of P16, especially in the dorsal layer. Almost all samples in the SLSS group were partially positive for P16. The LDH group showed negative staining of P16 in both the dural and dorsal layers. All the three groups were stained with S100 in the dorsal layer of the LF. On the contrary, S100 staining was absent in the dural layer of the LF in the three groups. Conclusions Elastin degradation and fibrosis of the LF in the DLSS patients is more severe compared with the SLSS and LDH patients. Increased expression of P16 associated with LF fibrosis and thickness, suggested that the expression of P16 may related to LF hypertrophy in the patients who suffer with LSS. LF hypertrophy process may not be associated with high expression of S100.http://link.springer.com/article/10.1186/s12891-019-2825-4Ligamentum FlavumHypertrophyHistologySpinal stenosisElastinFibrosis
collection DOAJ
language English
format Article
sources DOAJ
author Wei Hu
Shunli Kan
Guang Liu
Zegang Cao
Rusen Zhu
spellingShingle Wei Hu
Shunli Kan
Guang Liu
Zegang Cao
Rusen Zhu
The expression of P16 and S100 associated with elastin degradation and fibrosis of the Ligamentum Flavum hypertrophy
BMC Musculoskeletal Disorders
Ligamentum Flavum
Hypertrophy
Histology
Spinal stenosis
Elastin
Fibrosis
author_facet Wei Hu
Shunli Kan
Guang Liu
Zegang Cao
Rusen Zhu
author_sort Wei Hu
title The expression of P16 and S100 associated with elastin degradation and fibrosis of the Ligamentum Flavum hypertrophy
title_short The expression of P16 and S100 associated with elastin degradation and fibrosis of the Ligamentum Flavum hypertrophy
title_full The expression of P16 and S100 associated with elastin degradation and fibrosis of the Ligamentum Flavum hypertrophy
title_fullStr The expression of P16 and S100 associated with elastin degradation and fibrosis of the Ligamentum Flavum hypertrophy
title_full_unstemmed The expression of P16 and S100 associated with elastin degradation and fibrosis of the Ligamentum Flavum hypertrophy
title_sort expression of p16 and s100 associated with elastin degradation and fibrosis of the ligamentum flavum hypertrophy
publisher BMC
series BMC Musculoskeletal Disorders
issn 1471-2474
publishDate 2019-10-01
description Abstract Background One of the characteristics of lumbar spinal stenosis (LSS) is elastin degradation and fibrosis in the ligamentum flavum (LF). However, the biochemical factors that cause these histologic changes is unclear. P16 and S100 participate in scar formation and collagen development in wound healing and fibrosis diseases. In this study, we investigate the association between P16 and S100 expression and the fibrosis of the hypertrophic LF in LSS. Methods The LF specimens were surgically obtained from 30 patients with single-segment LSS (SLSS), 30 patients with double-segment LSS (DLSS) and 30 patients with L4/5 lumbar disc herniation (LDH). The LF thickness was measured by axial T1-weighted MRI. The extent of LF elastin degradation and fibrosis were graded based on hematoxylin-eosin (HE) and Verhoff’s Van Gieson’s (VVG) stain, respectively. The localization of P16 and S100 was determined by immunohistochemistry. Results The Absolute and relative LF thickness were greater in the DLSS group compared with the SLSS and LDH groups (p <  0.05). The elastic tissue from the dorsal aspect to the dural aspect in SLSS and DLSS groups was significantly increased. The amount of collagen deposition and elastic tissue is significantly higher in the DLSS group compared with the SLSS and LDH groups (p <  0.05). The specimens in the DLSS group showed positive staining of P16, especially in the dorsal layer. Almost all samples in the SLSS group were partially positive for P16. The LDH group showed negative staining of P16 in both the dural and dorsal layers. All the three groups were stained with S100 in the dorsal layer of the LF. On the contrary, S100 staining was absent in the dural layer of the LF in the three groups. Conclusions Elastin degradation and fibrosis of the LF in the DLSS patients is more severe compared with the SLSS and LDH patients. Increased expression of P16 associated with LF fibrosis and thickness, suggested that the expression of P16 may related to LF hypertrophy in the patients who suffer with LSS. LF hypertrophy process may not be associated with high expression of S100.
topic Ligamentum Flavum
Hypertrophy
Histology
Spinal stenosis
Elastin
Fibrosis
url http://link.springer.com/article/10.1186/s12891-019-2825-4
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