Expression and regulation of human beta-defensin in Campylobacter jejuni infection

doi:10.3969/j.issn.1673-8640.2016.08.006

Abstract

Abstract:

Objective To investigate the infection status of Campylobacter jejuni isolated from diarrhea syndrome and pathogenic monitoring study in Shanghai from 2012 to 2013. To study the immune regulation of human beta-defensin （hBD） in gastrointestinal infection caused by Campylobacter jejuni. Methods Campylobacter jejuni were isolated from diarrhea syndrome and pathogenic monitoring study in Shanghai from 2012 to 2013. Minimal inhibitory concentrations（MIC） to 7 antibiotics [gentamycin（GEN）,tetracycline（TET）,azithromycin（AZI）,erythromycin（ERY）,clindamycin（CLI）,ciprofloxacin（CIP） and nalidixic acid（NAL）] were determined by agar dilution method. Sodium dodecyl sulfate-pulsed-field gel electrophoresis （SDS-PFGE） was carried out for analyzing molecular epidemic trend. Human intestinal epithelial cell line Caco-2 was infected with Campylobacter jejuni. The transcription levels of hBD-1,hBD-2,hBD-3,TLR2 and TLR4 genes were determined by fluorescence quantitation polymerase chain reaction （PCR）,and the expressions of hBD-1,hBD-2,hBD-3,TLR2 and TLR4 were determined by western blotting. Results The isolation rate of Campylobacter jejuni isolated from diarrhea syndrome and pathogenic monitoring study in Shanghai from 2012 to 2013 was 1.6%. The drug resistance rates to TET and NAL were high （95.7% and 97.8%）. There were 9 PFGE patterns. After Campylobacter jejuni infected human intestinal epithelial cell line Caco-2,the transcription levels of hBD-1,hBD-2 and hBD-3 genes reached the highest at 6 h,and the expressions of hBD-1,hBD-2 and hBD-3 reached the highest at 24 h. The transcription level of TLR2 at 24 h was higher than those at 0,6 and 10 h. However,the transcription level of TLR4 reached the highest at 6 h. The expressions of TLR2 and TLR4 were the same as their transcription levels. Conclusions hBD plays a role in defense of Campylobacter jejuni infection.

Key words: Human beta-defensin, Campylobacter jejuni, Immune defense

CLC Number:

R446.5

WU Qiong, CHEN Hongyou, TU Lihong, SONG Yuanjun, ZHANG Wenxia, CHEN Min. Expression and regulation of human beta-defensin in Campylobacter jejuni infection[J]. Laboratory Medicine, 2016, 31(8): 662-666.

Figures/Tables 7

References 13

[1]	ALTEKRUSE SF,STERN NJ,FIELDS PI,et al.Campylobacter jejuni-an emerging foodborne pathogen[J]. Emerg Infect Dis,1999,5(1):28-35.
[2]	GIBREEL A,TAYLOR DE.Macrolide resistance in Campylobacter jejuni and Campylobacter coli[J]. J Antimicrob Chemother,2006,58(2):243-255.
[3]	谢永强,周珍文,虢艳,等. 广州地区儿童空肠弯曲菌感染的病原学研究[J]. 中国当代儿科杂志,2009,11(6):422-424.
[4]	张晓利. 动物性食品源空肠弯曲杆菌的分离鉴定及其二重PCR检测方法的建立[D]. 成都:四川农业大学,2009.
[5]	KONKEL ME,KLENA JD,RIVERA-AMILL V,et al.Secretion of virulence proteins from Campylobacter jejuni is dependent on a functional flagellar export apparatus[J]. J Bacteriol,2004,186(11):3296-3303.
[6]	LOCHT H,KROGFELT KA.Comparison of rheumatological and gastrointestinal symptoms after infection with Campylobacter jejuni/coli and enterotoxigenic Escherichia coli[J]. Ann Rheum Dis,2002,61(5):448-452.
[7]	DOMMETT R,ZILBAUER M,GEORGE JT,et al.Innate immune defence in the human gastrointestinal tract[J]. Mol Immunol,2005,42(8): 903-912.
[8]	DIAMOND G,ZASLOFF M,ECK H,et al.Tracheal antimicrobial peptide,a cysteine-rich peptide from mammalian tracheal mucosa:peptide isolation and cloning of a cDNA[J]. Proc Natl Acad Sci USA,1991,88(9):3952-3956.
[9]	TENOVER FC,ARBEIT RD,GOERING RV,et al.Interpreting chromosomal DNA restriction patterns produced by pulsed-field gel electrophoresis:criteria for bacterial strain typing[J]. J Clin Microbiol,1995,33(9):2233-2239.
[10]	SAMUEL MC,VUGIA DJ,SHALLOW S,et al.Epidemiology of sporadic Campylobacter infection in the United States and declining trend in incidence,FoodNet 1996-1999[J]. Clin Infect Dis,2004,38(Suppl 3): S165-S174.
[11]	SWARTZ MN.Human diseases caused by foodborne pathogens of animal origin[J]. Clin Infect Dis,2002,34(Suppl 3):S111-S122.
[12]	KOUNO T,FUJITANI N,MIZUGUCHI M,et al.A novel beta-defensin structure:a potential strategy of big defensin for overcoming resistance by Gram-positive bacteria[J]. Biochemistry,2008,47(40):10611-10619.
[13]	张磊,印树葳,张婷,等. 抗菌肽人β防御素3对肺炎克雷伯菌临床菌株的抑制作用研究[J]. 检验医学,2014,29(11):1184-1187.

引物名称	引物序列
qRT-hBD-1-S	ACCTTCTGCTGTTTACTCTCTGCT
qRT-hBD-1-AS	GACATTGCCCTCCACTGCT
qRT-hBD-2-S	GGTGGTATAGGCGATCCTGTT
qRT-hBD-2-AS	AGGGCAAAAGACTGGATGACA
qRT-hBD-3-S	TGAAGCCTAGCAGCTATGAGGATC
qRT-hBD-3-AS	CCGCCTCTGACTCTGCAATAA
qRT-TLR4-F	CTGCAATGGATCAAGGACCA
qRT-TLR4-R	TTATCTGAAGGTGTTGCACATTCC
qRT-TLR2-F	ATCCTCCAATCAGGCTTCTCT
qRT-TLR2-R	GGACAGGTCAAGGCTTTTTACA

引物名称	引物序列
qRT-hBD-1-S	ACCTTCTGCTGTTTACTCTCTGCT
qRT-hBD-1-AS	GACATTGCCCTCCACTGCT
qRT-hBD-2-S	GGTGGTATAGGCGATCCTGTT
qRT-hBD-2-AS	AGGGCAAAAGACTGGATGACA
qRT-hBD-3-S	TGAAGCCTAGCAGCTATGAGGATC
qRT-hBD-3-AS	CCGCCTCTGACTCTGCAATAA
qRT-TLR4-F	CTGCAATGGATCAAGGACCA
qRT-TLR4-R	TTATCTGAAGGTGTTGCACATTCC
qRT-TLR2-F	ATCCTCCAATCAGGCTTCTCT
qRT-TLR2-R	GGACAGGTCAAGGCTTTTTACA

抗菌药物	MIC
抗菌药物	区间	MIC₅₀	MIC₉₀
AZI	0.03~>64	0.03	0.25
CIP	0.06~>64	32	32
ERY	0.12~>64	0.5	2
GEN	<0.12~>32	<0.12	0.25
TET	0.12~>64	>64	>64
NAL	<4~>64	>64	>64
CLI	0.12~>16	0.5	2

抗菌药物	MIC
抗菌药物	区间	MIC₅₀	MIC₉₀
AZI	0.03~>64	0.03	0.25
CIP	0.06~>64	32	32
ERY	0.12~>64	0.5	2
GEN	<0.12~>32	<0.12	0.25
TET	0.12~>64	>64	>64
NAL	<4~>64	>64	>64
CLI	0.12~>16	0.5	2

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