iRoot BP Plus治疗大鼠牙髓损伤的研究分析

doi:10.13591/j.cnki.kqyx.2025.09.004

摘要/Abstract

摘要：

目的研究iRoot BP Plus在大鼠牙髓损伤过程中对牙髓腔修复的影响,初步探讨该疗法在牙髓损伤修复过程中可能发挥的作用。方法选取健康的8周龄SD大鼠共60只作为研究对象,对其双侧上颌第一磨牙进行开髓处理以构建动物模型;之后给予直接盖髓手术,分为iRoot BP Plus组(BP组)和对照组。组织学处理后,通过microCT和苏木精-伊红(hematoxylin-eosin,HE)染色观察牙髓组织损伤修复情况,髓腔钙化情况。提取大鼠牙髓组织mRNA,运用荧光定量PCR技术检测炎症和矿化基因表达变化。结果 microCT结果显示直接盖髓术后1、4、7 d牙髓组织均有不同程度的髓腔钙化。BP组与对照组在术后1 d差异较小,但是在术后4和7 d,BP组在开髓孔处形成较规则的钙化桥,而对照组开髓孔下方形成大面积不规则钙化团块,牙髓组织占比减少,X线片显示其髓腔出现大面积钙化影像。HE染色结果显示在术后1 d,牙髓组织炎症反应重,开髓孔附近有大量炎症细胞浸润,术后4和7 d,BP组开髓孔附近开始形成矿化组织,髓腔保留较多的健康牙髓组织。牙髓组织基因水平表明BP组白细胞介素-1β(interleukin-1β,IL-1β)、肿瘤坏死因子-α(tumor necrosis factor-α,TNF-α)表达水平较对照组降低,矿化相关基因Ⅰ型胶原(collagen type1,COL1)、牙本质涎磷蛋白(dentin sialophosphoprotein,DSPP)基因表达水平较对照组升高,有统计学差异(P<0.05)。结论牙髓损伤后会诱发牙髓免疫防御反应,若炎症控制不佳则会刺激牙髓腔钙化,iRoot BP Plus可以较好地调控牙髓微环境,控制炎症发展,减少牙髓损伤后的髓腔不良钙化团块形成,保存更多的健康牙髓组织。

关键词: 牙髓炎症, 牙髓损伤修复, iRoot BP plus, microCT

Abstract:

Objective To investigate the effect of iRoot BP Plus on the repair of dental pulp cavity during pulp injury in rats, and to explore the possible role of iRoot BP Plus in the process of damage repair. Methods Bilateral maxillary first molars of 60 8-week-old SD rats were treated with direct pulp capping after pulp opening. They were divided into iRoot BP Plus group(BP group)and control group. After histological processing, the damage of dental pulp tissue and the calcification of pulp cavities were observed by microCT and HE staining. mRNA was extracted from rat dental pulp tissue, and the expression of inflammation and mineralization genes were detected by real-time quantitatitive PCR. Results The results of this study showed that the dental pulp tissue had different degrees of calcification at 1, 4 and 7 days after direct pulp capping. There was no significant difference between the BP group and the control group on the 1st day after the operation, but on the 4th and 7th day after the operation, a regular calcified bridge was formed at the pulp hole in the BP group, and more pulp tissue was retained in the pulp cavity. In the control group, a large area of irregular calcified tissue was formed below the pulp hole. HE staining results showed that the pulp tissue had a heavy inflammatory response, and a large number of inflammatory cells infiltrated near the pulp orifice on the first day after the operation. On the 4th and 7th days after the operation, mineralized tissue began to form near the pulp orifice in the BP group, and healthier pulp tissue was retained in the pulp cavity. The gene levels of IL-1β and TNF-α in the BP group were lower than those in the control group, and the gene expression levels of mineralization indexes COL1 and DSPP were higher than those in the control group. The difference was statistically significant(P<0.05). Conclusion Dental pulp injury can induce the immune defense response. If the inflammation is not well controlled, it will stimulate the calcification of dental pulp cavities. iRoot BP Plus can better regulate the dental pulp microenvironment, control the development of inflammation, reduce the formation of adverse calcified masses in the pulp cavity after pulp injury, and preserve more pulp tissue.

Key words: pulp inflammation, dental pulp repair, iRoot BP plus, microCT

中图分类号:

R783.1

陈杰, 邢允波, 叶茂. iRoot BP Plus治疗大鼠牙髓损伤的研究分析[J]. 口腔医学, 2025, 45(9): 663-666.

CHEN Jie, XING Yunbo, YE Mao. Analysis of iRoot BP Plus in the treatment of rat dental pulp injury[J]. Stomatology, 2025, 45(9): 663-666.

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参考文献 24

[1]	周学东, 黄定明, 刘建国, 等. 牙髓损伤的活髓保存治疗[J]. 华西口腔医学杂志, 2017, 35(4): 339-347.
[2]	Goldberg M, Farges JC, Lacerda-Pinheiro S, et al. Inflammatory and immunological aspects of dental pulp repair[J]. Pharmacol Res, 2008, 58(2): 137-147. doi: 10.1016/j.phrs.2008.05.013 pmid: 18602009
[3]	Ricucci D, Siqueira JF, Li YY, et al. Vital pulp therapy: Histopathology and histobacteriology-based guidelines to treat teeth with deep caries and pulp exposure[J]. J Dent, 2019, 86: 41-52. doi: S0300-5712(19)30105-8 pmid: 31121241
[4]	卢艳红, 王静, 吴晓光. iRoot BP Plus在年轻恒牙活髓切断术中的临床效果及美观性观察[J]. 中国美容医学, 2022, 31(10): 141-144.
[5]	Cooper PR, Takahashi Y, Graham LW, et al. Inflammation-regeneration interplay in the dentine-pulp complex[J]. J Dent, 2010, 38(9): 687-697. doi: 10.1016/j.jdent.2010.05.016 pmid: 20580768
[6]	Cooper PR, Holder MJ, Smith AJ. Inflammation and regeneration in the dentin-pulp complex: A double-edged sword[J]. J Endod, 2014, 40(4 Suppl): S46-S51.
[7]	Zaky SH, Shehabeldin M, Ray H, et al. The role of inflammation modulation in dental pulp regeneration[J]. Eur Cell Mater, 2021, 41: 184-193. doi: 10.22203/eCM.v041a13 pmid: 33583014
[8]	Öncel Torun Z, Torun D, Demirkaya K, et al. Effects of iRoot BP and white mineral trioxide aggregate on cell viability and the expression of genes associated with mineralization[J]. Int Endod J, 2015, 48(10): 986-993. doi: 10.1111/iej.12393 pmid: 25286824
[9]	Wang XY, Xiao YZ, Song WC, et al. Clinical application of calcium silicate-based bioceramics in endodontics[J]. J Transl Med, 2023, 21(1): 853. doi: 10.1186/s12967-023-04550-4 pmid: 38007432
[10]	周杨, 李谨, 朱庆萍, 等. 硅酸钙生物材料诱导牙源性干细胞成牙/成骨分化机制的研究进展[J]. 口腔医学, 2020, 40(2):169-175.
[11]	Choi BD, Jeong SJ, Wang GL, et al. Temporal induction of secretory leukocyte protease inhibitor(SLPI)in odontoblasts by lipopolysaccharide and wound infection[J]. J Endod, 2009, 35(7): 997-1002.
[12]	Chen J, Xu HX, Xia K, et al. Resolvin E1 accelerates pulp repair by regulating inflammation and stimulating dentin regeneration in dental pulp stem cells[J]. Stem Cell Res Ther, 2021, 12(1): 75. doi: 10.1186/s13287-021-02141-y pmid: 33482900
[13]	Goldberg M, Njeh A, Uzunoglu E. Is pulp inflammation a prerequisite for pulp healing and regeneration?[J]. Mediators Inflamm, 2015, 2015: 347649.
[14]	Manaspon C, Jongwannasiri C, Chumprasert S, et al. Human dental pulp stem cell responses to different dental pulp capping materials[J]. BMC Oral Health, 2021, 21(1): 209. doi: 10.1186/s12903-021-01544-w pmid: 33902558
[15]	Ricucci D, Rôças IN, Alves FRF, et al. Outcome of direct pulp capping using calcium hydroxide: A long-term retrospective study[J]. J Endod, 2023, 49(1): 45-54. doi: 10.1016/j.joen.2022.11.005 pmid: 36375647
[16]	Schuurs AH, Gruythuysen RJ, Wesselink PR. Pulp capping with adhesive resin-based compositevs. calcium hydroxide: A review[J]. Endod Dent Traumatol, 2000, 16(6): 240-250. pmid: 11202889
[17]	Wang Y, Li J, Song W, et al. Mineral trioxide aggregate upregulates odonto/osteogenic capacity of bone marrow stromal cells from craniofacial bones JNK and ERK MAPK signalling pathways[J]. Cell Prolif, 2014, 47(3): 241-248.
[18]	Brizuela C, Ormeño A, Cabrera C, et al. Direct pulp capping with calcium hydroxide, mineral trioxide aggregate, and biodentine in permanent young teeth with caries: A randomized clinical trial[J]. J Endod, 2017, 43(11): 1776-1780. doi: S0099-2399(17)30818-X pmid: 28917577
[19]	Cushley S, Duncan HF, Lappin MJ, et al. Efficacy of direct pulp capping for management of cariously exposed pulps in permanent teeth: A systematic review and meta-analysis[J]. Int Endod J, 2021, 54(4): 556-571. doi: 10.1111/iej.13449 pmid: 33222178
[20]	Rao Q, Kuang J, Mao CX, et al. Comparison of iRoot BP plus and calcium hydroxide as pulpotomy materials in permanent incisors with complicated crown fractures: A retrospective study[J]. J Endod, 2020, 46(3): 352-357. doi: S0099-2399(19)30981-1 pmid: 32035640
[21]	梁颂, 周庆楠, 宿颖, 等. iRoot BP Plus应用于乳牙牙髓切断术后的组织学改变[J]. 北京口腔医学, 2024, 32(3): 190-195.
[22]	张小芳, 刘朝进, 李祖进, 等. iRoot BP Plus用于外伤露髓年轻恒牙活髓切断术对牙齿变色率及根管钙化的影响[J]. 口腔材料器械杂志, 2022, 31(4):301-304.
[23]	Liu SY, Wang SN, Dong YM. Evaluation of a bioceramic as a pulp capping agentand in vivo[J]. J Endod, 2015, 41(5): 652-657.
[24]	陆嘉敏, 闫明, 李泽汉, 等. iRoot BP Plus对骨髓间充质干细胞成牙/成骨分化及自噬的影响[J]. 口腔医学, 2019, 39(10):873-879.

基因名称	引物序列(5'→3')
IL-1β	F:AAGACAAGCCTGTGTTGCTGAAGG R:TCCCAGAAGAAAATGAGGTCGGTC
TNF-α	F:CTTCTCATTCCTGCTCGTGG R:GCTACGGGCTTGTCACTCG
COL1	F:GCCTCCCAGAACATCACCTA R:GCAGGGACTTCTTGAGGTTG
DSPP	F:GGGAAGCTCAGTGGAAGTAAAG R:CTGCTGTGTCCCATGTTGTAT
GAPDH	F:CAACTCCCTCAAGATTGTCAGCAA R:GGCATGGACTGTGGTCATGA