CD3+CD56+ natural killer T cell infiltration is increased in cervical cancer and negatively correlated with tumour progression

This study investigated the phenotype and function of natural killer T (NKT) cells infiltrating cervical cancer tissues, in an attempt to understand the regulation of NKT cells by cervical cancer cells. Forty-two patients with cervical cancer were included. Flow cytometry was used to analyze the per...

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Main Authors: Yunxia Tu, Mei Pan, Shuhong Song, Jinren Hua, Rongfang Liu, Longyu Li
Format: Article
Language:English
Published: Taylor & Francis Group 2019-01-01
Series:Biotechnology & Biotechnological Equipment
Subjects:
Online Access:http://dx.doi.org/10.1080/13102818.2019.1669489
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spelling doaj-02ef25a550d44c0fabbb0db975cb4cd02020-11-25T02:28:48ZengTaylor & Francis GroupBiotechnology & Biotechnological Equipment1310-28181314-35302019-01-013311380139110.1080/13102818.2019.16694891669489CD3+CD56+ natural killer T cell infiltration is increased in cervical cancer and negatively correlated with tumour progressionYunxia Tu0Mei Pan1Shuhong Song2Jinren Hua3Rongfang Liu4Longyu Li5Nanchang UniversityMaternal and Child Health Hospital of Jiangxi ProvinceJishui People's HospitalMaternal and Child Health Hospital of Jiangxi ProvinceMaternal and Child Health Hospital of Jiangxi ProvinceNanchang UniversityThis study investigated the phenotype and function of natural killer T (NKT) cells infiltrating cervical cancer tissues, in an attempt to understand the regulation of NKT cells by cervical cancer cells. Forty-two patients with cervical cancer were included. Flow cytometry was used to analyze the percentage of NKT cells in tumour tissues and its correlation with clinical staging and lymphatic metastasis. The expression of surface receptor and effector molecules on infiltrating NKT cells was determined. The changes of the phenotype, subtype and cytotoxicity of NKT cells were investigated. The regulation of NKT cells by cervical cancer cells was investigated by co-culture with HeLa or SiHa cells. The effect of TGF-β1 on NKT activity regulated by cervical cancer cells was studied. The results showed that the infiltration of NKT cells in cervical cancer tissues was significantly higher than that in tumour-adjacent tissues, and the degree of infiltration was negatively correlated with the progression of the disease. The activity and killing effect of infiltrating NKT were inhibited in cervical cancer tissues, leading to increase of CD4+NKT cells and decrease of CD8−CD4−NKT cells. The activity of NKT cells was down-regulated by co-culture with cervical cancer cells, but subtypes of NKT cells were not altered. Cervical cancer cells inhibited the function of NKT cells by secreting TGF-β1. The study demonstrates that the infiltration of NKT cells in cervical cancer tissues is increased significantly and negatively correlated with tumour progression.http://dx.doi.org/10.1080/13102818.2019.1669489cd3+cd56+ nktinfiltrationcervical cancertgf-β1
collection DOAJ
language English
format Article
sources DOAJ
author Yunxia Tu
Mei Pan
Shuhong Song
Jinren Hua
Rongfang Liu
Longyu Li
spellingShingle Yunxia Tu
Mei Pan
Shuhong Song
Jinren Hua
Rongfang Liu
Longyu Li
CD3+CD56+ natural killer T cell infiltration is increased in cervical cancer and negatively correlated with tumour progression
Biotechnology & Biotechnological Equipment
cd3+cd56+ nkt
infiltration
cervical cancer
tgf-β1
author_facet Yunxia Tu
Mei Pan
Shuhong Song
Jinren Hua
Rongfang Liu
Longyu Li
author_sort Yunxia Tu
title CD3+CD56+ natural killer T cell infiltration is increased in cervical cancer and negatively correlated with tumour progression
title_short CD3+CD56+ natural killer T cell infiltration is increased in cervical cancer and negatively correlated with tumour progression
title_full CD3+CD56+ natural killer T cell infiltration is increased in cervical cancer and negatively correlated with tumour progression
title_fullStr CD3+CD56+ natural killer T cell infiltration is increased in cervical cancer and negatively correlated with tumour progression
title_full_unstemmed CD3+CD56+ natural killer T cell infiltration is increased in cervical cancer and negatively correlated with tumour progression
title_sort cd3+cd56+ natural killer t cell infiltration is increased in cervical cancer and negatively correlated with tumour progression
publisher Taylor & Francis Group
series Biotechnology & Biotechnological Equipment
issn 1310-2818
1314-3530
publishDate 2019-01-01
description This study investigated the phenotype and function of natural killer T (NKT) cells infiltrating cervical cancer tissues, in an attempt to understand the regulation of NKT cells by cervical cancer cells. Forty-two patients with cervical cancer were included. Flow cytometry was used to analyze the percentage of NKT cells in tumour tissues and its correlation with clinical staging and lymphatic metastasis. The expression of surface receptor and effector molecules on infiltrating NKT cells was determined. The changes of the phenotype, subtype and cytotoxicity of NKT cells were investigated. The regulation of NKT cells by cervical cancer cells was investigated by co-culture with HeLa or SiHa cells. The effect of TGF-β1 on NKT activity regulated by cervical cancer cells was studied. The results showed that the infiltration of NKT cells in cervical cancer tissues was significantly higher than that in tumour-adjacent tissues, and the degree of infiltration was negatively correlated with the progression of the disease. The activity and killing effect of infiltrating NKT were inhibited in cervical cancer tissues, leading to increase of CD4+NKT cells and decrease of CD8−CD4−NKT cells. The activity of NKT cells was down-regulated by co-culture with cervical cancer cells, but subtypes of NKT cells were not altered. Cervical cancer cells inhibited the function of NKT cells by secreting TGF-β1. The study demonstrates that the infiltration of NKT cells in cervical cancer tissues is increased significantly and negatively correlated with tumour progression.
topic cd3+cd56+ nkt
infiltration
cervical cancer
tgf-β1
url http://dx.doi.org/10.1080/13102818.2019.1669489
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