Periapical lesions are among the most frequently occurring pathological lesions (1) in the alveolar tissues surrounding the apex of the tooth root, the periodontal membrane, and the alveolar bone (2). They are predominantly precipitated by pulpal inflammation and/or necrosis, with consequent inflammatory mediators diffusing through the apical foramen into the surrounding tissues (3). Although the classification of the World Health Organization does not specifically feature the periapical lesions (4), Nair has classified periapical radiolucency into apical abscess (acute or chronic), acute apical periodontitis (primary or secondary), periapical cyst (true or pocket), and chronic apical periodontitis (granuloma) (5).

Periapical abscess is a localized collection of pus that occurs at the end of a root apex (6). Detectable levels of IL-8 are found in approximately 95% of periapical exudates, suggesting a pivotal role of IL-8 in acute phases of apical disease (7). Endodontic microorganisms are able to induce the production of IL-8 by pulp fibroblasts and osteoblasts (8). It has been found that leukotriene B4 (LTB4) is formed when arachidonic acid is oxidized via the lipoxygenase pathway, causing adhesion of polymorphonuclear leukocytes (PMNs) to the endothelial walls that attract macrophages to the affected area, leading to severe damage to the host tissues (9).

Radicular cyst is the most common odontogenic cyst (10) associated with bacterial (11), fungal, archaeal, and viral infections (12). A high level of bacterial endotoxin was detected in radicular cysts and was found to induce a proliferative effect on the epithelial cells (13). While the role of IL-12 (14) in the pathogenesis of radicular cyst is controversial, a confirmative role of IL-17 (15) on the immune response and bone resorption has been noted.

Periapical granuloma is a chronic inflammation located at the apex of a non-vital tooth. It comprises granulation and scar tissues permeated by diverse inflammatory cells including lymphocytes, plasma cells, macrophages, and mast cells (16). IL-17 (17), IL-10 (18), and IL-6 (19) are important cytokines found in apical periodontitis. The granulomatous tissue may frequently harbor microbes including bacteria (11), fungi, archaea, and viruses (12). The type of immune response in the periapical lesions is thought to be determined by the apically resident bacterial phylotypes (20).

There is a close relationship between the pathology of the periapical abscess, the resultant granuloma, and the eventual cystic lesion. The abscess theory describes the conversion of an acute inflammatory abscess to an inflammatory periapical cyst by enclosing and delimiting the area with proliferating epithelia (21). On the other hand, a periapical cyst may evolve from periapical granuloma as a consequence of untreated chronic periapical periodontitis (22). Furthermore, a dormant periapical abscess may develop into a periapical granuloma (1). Understanding this pathophysiological transformation as well as the metabolic behavior of the causative bacteria and their effect on the host responses can now be accomplished using new generation molecular methods. Furthermore, the metabolic background underlying these conditions or their roles in lesion progression have never been studied.

Distinct subpopulations of inflammatory cells have been described in periapical lesions. T cells are abundant in periapical lesions, but the activation and function of these cells are not well understood. T-helper cells are known to be mediators of bone resorption, while a larger population of activated T cells was found in granulomas compared with cysts (23). The cellular component of the periapical abscess is predominantly neutrophils and macrophages (24), although a scanty population of dendritic cells has been observed in periapical granulomas and cysts (25).

Metabolomics refer to all metabolites present in a given biological system, fluid, cell, or tissue (26). Metabolic profiling is highly informative since metabolites act as the end products of any biochemical metabolic pathway (27). Such pathways in immune cellular functions may be seen as surrogate markers of inflammation (28) consequential to host–microbe interactions (29). However, metabolite profiling in relation to dentoalveolar lesions has never been attempted before. In this study, the unique metabolites related to periapical lesions in comparison with healthy pulp tissue were mapped along with enriched pathways and then linked to previously published data involving the related active genes. The combined data generate a significant association between the metabolic pattern, enriched pathways, and the existence, maintenance, and progression of dentoalveolar lesions. Such data obtained based on metabolomics and immunological behavior can be used to decipher the transitional pathogenesis between periapical lesions.

The lesion samples used in this study included periapical abscesses, radicular cysts, and periapical granulomas. Both radicular cysts and periapical granulomas were discriminated following histopathological examination (Figure 1). The metabolic profiling of both healthy pulp tissue (used as a control) and lesion samples was performed using GC-MS analysis. A flowchart summarizes the methodological procedures in Figure S1. The identified metabolites were compared, classified, and correlated with the clinical characteristics of the investigated lesion types. Over a hundred metabolites were identified, some of them were shared between lesions and the healthy control, others were shared between the lesions only, and others were unique to a lesion type (Figure 2A, Table 3, and Table S5). Heatmap analysis showed that the identified metabolites clustered into two separate groups: a group representing the healthy control and radicular cyst and the other group representing the periapical abscess and granuloma (Figure 2B and Tables S3, S4). Unique metabolites to a lesion type in comparison with healthy pulp tissue were mapped as shown in Table 3 and Table S5. Metabolite occurrence was classified as below.

Cellular metabolites provide a true image of the interactions between a genome of a specific cell and its environment and, thus, yield an unbiased perspective of the cellular state either in health and disease (102). The metabolomic profiling of periapical lesions and healthy pulp tissue reported here reveals for the first time a metabolite environment that clearly separates the periapical granuloma and abscess from the radicular cyst and healthy control. Indeed, our study sheds light on the role of the unique metabolites in the initiation, maintenance, and progression of each subtype of oral lesion, although the role of the shared metabolites such as nonadecane, disulfide, di-tert-dodecyl, and 2-methylhexacosane in the remodeling of periapical lesions needs further investigation. In our study, the calculated area under the peak value (instead of area percentage) was used, because this is more accurate and, following normalization, allows for better data visualization/representation. In addition, fold changes provide a general overview for the relative analyte abundance, helpful for comparison with future studies.

In the healthy control group, unique metabolites in cluster C include glycolic acid, itaconic acid, and 2-butenedioic acid, all of which are carboxylic acids used to prepare dental pellets (103) for conservative replacement. In cluster D, physiologic signal transduction in healthy pulp tissues is mediated by the neurotransmitter metabolites, like L-aspartic acid and L-glutamic acid (104), in addition to 10-undecynoic acid that maintains the healthy condition due to its antibacterial and antibiofilm activities (105). Unique metabolites in cluster E, like pentadecanoic acid, enhance NK cell activity (106), while 3-dodecanol has antifungal activity (107). Oleic acid in cluster F, which is the most prominent metabolite in healthy pulp tissue, has anti-inflammatory (108), antibacterial (109), and antifungal activities (110) beyond promoting dendritic cell activation (111) to maintain physiologic pulpal conditions. Cluster G palmitic and stearic acids are known to increase NK cell activity (106) and dendritic cell sensitization (111) and induce apoptotic cellular response (112).

In the periapical abscess, cluster H metabolites are mostly known to be correlated to M2 polarization and IL-10 expression; for example, arsenous acid (113) and cholesterol can induce anti-inflammatory M2 polarization (114). These metabolites are present in periapical abscess in lower concentration than in periapical granuloma, indicating that M2 polarization is more inducible in periapical granuloma than in periapical abscess. In cluster I, we found n-butanol, reported to promote NK cell proliferation (115), while butyrate stimulated NK cell cytotoxicity (116) and increased the expression of MMP-9 (117). In the same cluster, alkane metabolites (such as octadecane) stimulate dendritic cells to release IL-6 and IL-10 (118, 119), while isovalerate downregulates the pro-inflammatory polarization of macrophages (120). All metabolites in cluster J are with omega configurations corresponding to fatty acids, dicarboxylic acids, and acetylene. The omega-6 fatty acid, linoelaidic acid, is a pro-inflammatory metabolite (121); dicarboxylic acid calcium oxalate activates human monocytes and enhances the production of IL-8 and IL-10 (122). Finally, the acetylene 17-octadecynoic acid is known to be related to 16-20-HETE, positively correlated with the expression of CYP4F3 (43), VEGF (46), and IL-8 (49).

In the radicular cyst, the alkane and alkene metabolites identified in cluster K are generally known to have a role in inducing cellular membrane flexibility required for optimal cell division and growth (123) and, hence, necessary for radicular cyst expansion. Nonane alkanes and their derivatives in cluster L are considered to be highly hydrophobic lipid molecules (124)and expected to be released during lipophagy. In cluster M, palmitic and stearic acids are significantly correlated with the induction of apoptosis (112), which was identified as the major enrichment pathway in the development of radicular cyst.

In the periapical granuloma, cluster N contains arsenous acid (113), cholesterol (114), octanoic acid (125), L-serine (126), ethanolamine (127), and butanoic acid derivatives (128) that reduce pro-inflammatory M1 or induce anti-inflammatory M2 polarization. Cluster O metabolites included phosphoric acid, which favors chronic inflammation (129), while butylated hydroxytoluene induces M2 macrophage polarization (130). Cluster P predominated in periapical granuloma and clearly differentiated this from other lesions. Despite similar concentrations of ethylene glycol in the periapical abscess and granuloma, the important contributor (L-(+)-lactic acid) was absent in periapical abscess. Interestingly, both L-(+)-lactic acid and ethylene glycol appear to be involved in granuloma formation, a complication associated with skin fillers in plastic surgery (131, 132). This phenomenon is thought to be due to failure in effective phagocytosis leading eventually to granuloma formation (133). Furthermore, ethylene glycol is known to cross-link hyaluronic acid, important for tissue formation/volume (134), while L-lactate polarizes macrophage toward M2 and reduces NK cell cytotoxicity (135–137). Poly-ethylene glycol is also known to favor regenerative M2 macrophage responses (138).

In the healthy pulp tissue, oleic, palmitic, and stearic acids were found to play a crucial role in maintaining a healthy pulpo-dentinal complex (139, 140) with intrinsic antimicrobial activity (141–143). The top enriched metabolic pathways identified in healthy controls are listed in Table 4. The highest MCODE in healthy controls reveals that ionotropic receptors N-methyl-D-aspartate (NMDA) (144) and kainate receptors (96) are critical contributors to the maintenance of a healthy pulp (96). Gαq subunit of G protein-coupled receptors (145) appears to activate phospholipase Cβ leading to a significant efflux of Ca²⁺ from the endoplasmic reticulum into the cytosol (146). It has been reported that a high expression of glutamate receptor ionotropic kainate 1 (GRIK1) in healthy pulp tissues correlates with profound tooth sensitivity (147). GRIK2 increases the permeability of Ca²⁺ inside the cell (148), and Ca²⁺ overload results in ischemic cell death (149), which is a phenomenon related to dying tooth pulp during surgical extraction of a healthy tooth. Although GRIN genes are encoding NMDA receptor, GRIA encoded the α-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid (AMPA) receptor, which is another related group of glutamate ionotropic receptor (150). We further identified free fatty acid receptors (FFAR), especially FFAR1 and FFAR3 in healthy pulp tissue, previously reported to bind to palmitic, stearic, and oleic acids (151). These receptors are known to play a key role in maintaining a systemic health condition (140). Activation of group I glutamate metabotropic receptors (GRM), including GRM1 and GRM5, generally induces normal neuronal plasticity (152) (Figure S2A).

Although normal healthy pulp was considered to be a sterile space devoid of flora, relatively recent next-generation sequencing data have clearly shown the intriguing presence of bacteria in this tissue space (153) likely to play an important role in maintaining healthy homeostasis. TLR4 on normal odontoblasts (154) binds to LPS, which in turn induces differentiation of human dental pulp stem cells to pulpal odontoblasts (155). In healthy pulp tissue, the predominant immune cells were T-helper cells followed by NK cells, dendritic cells, and CD8 T cells as previously suggested (156–159). Kawashima et al. also reported the presence of NKT cells (160) in healthy pulp tissue, revealing the importance of these in the maintenance of normal pulp homeostasis.

This study has reported for the first time the role of 20-HETE in the pathogenesis of periapical abscess. It has been found that 17-octadecynoic acid is a partial inhibitor of CYP4Fs (161). In our study, the inhibition of CYP4F3 in abscess was not correlated to 17-octadecynoic acid, the most abundant metabolite significantly identified in the periapical abscess, perhaps due to the significant upregulation of CYP4F3 (Figure 6A). This result was consistent with the highest PPI involved in periapical abscess including CYP1A2, CYP2C9, and CYP4F2 (Figure S2B). Additionally, the relation between 20-HETE and the significant upregulated genes is highlighted in Table 4 and Figure 8A. Some of the significantly upregulated genes were previously investigated in periapical abscess (7, 162–164), but here, we provide evidence suggesting how they impact metabolic pathways in disease. Our in silico immunological profiling of the periapical abscess showed a predominance of T-helper cells followed by dendritic cells. While Ferreira et al. have significantly reported the presence of T-helper cell-related IL-17A production in periapical abscess (163), Harmon et al. demonstrated the presence of mature dendritic in dental abscess compared with healthy dental tissues (165). All the periapical abscess samples in this study were obtained from patients with an Asian ethnicity. Our results reveal that 80% of the recorded mutations in active genes are related to the Asian population, particularly for MAPT and CYP1A2 genes (Table 2). In contrast, Salles et al. reported significant polymorphisms in IL-1B, IL-6, and IL-8 genes in periapical abscess (166). The metabolic environment of periapical abscess may stimulate the conversion of LTB4 to a less active form, 20-HETE (167), and the downregulation of IL-12A (Figure 8A). 20-HETE stimulates the release of IL-8 from endothelial cells by increasing the production of reactive oxygen species and activating the NF-κB pathway (49). Furthermore, both the increase in 20-HETE and the downregulation of IL-12A significantly upregulate the expression of MMP-9 and VEGF (47). This in turn is likely to increase the T-helper cell population, the differentiation of naive T cells into Th1 cells (168), and the stimulation of NK cells (169) and CD8 cytotoxic T lymphocytes (170) (Figure 8A).

The abundance of palmitic acid in radicular cyst-derived keratinocytes reveals a high metabolic activity in these cells (171). However, 1-nonadecene, the highest identified unique metabolite in the radicular cyst, has not been reported before and its significance needs to be further studied. While Takata et al. (171) detected the presence of high metabolic activity in radicular cyst, Güler et al. (172) confirmed the significant proliferative capacity in radicular cyst. Excessive cell proliferation in the epithelial lining that may mediate a nutritional deficiency leading to lipophagy (56, 57) is believed to be positively correlated to specific inflammatory mediators such as IL-17 (68) and IL-12A (173) (Table 4 and Figures 6F, J). The prominent PPI in radicular cyst was for protein kinase AMP-activated (PRKA) (Figure S2C), considered a master activator of autophagy (174). Interestingly, our results reveal the predominance of memory CD8 T cells, followed by pro-inflammatory M1 macrophages and naive CD8 T cells in the radicular cysts. Other studies found that the most abundant immune cells in radicular cysts were memory CD8 T cells (62), in addition to the high polarization toward pro-inflammatory M1 macrophages (175) and a scant presence of CD8 T cells (176). Despite the highest SNPs for POLB were reported in other African population, the Asian population has the highest SNP for PRKAG2, PRKAB2, and F2 (Table 2). An evidence of TP63 SNPs in radicular cyst was previously reported by Souza et al. (177). In the radicular cyst, beta-sitosterol and ethanimidic acid were the only unique metabolites found to provide the enriched metabolic pathways as described in Table 4. Nevertheless, 1-nonadecene was the highest unique metabolite in the cyst, whose biological and immunological significance has not been reported thus far. In our study, IL-12A was the most upregulated gene in radicular cyst compared with other periapical lesions (Figure 6J). IL-12 is important in CD8 T-cell clonal expansion in addition to the generation of memory CD8 T cells (65), which in turn stimulate lipophagy (Figure 8B). Lipophagy was reported in lipid-laden macrophages (foam macrophages) (59, 60) in odontogenic cyst (63) and in memory CD8 T cells (61). Additionally, IL-12A inhibits VEGF and MMP-9 reducing angiogenesis (66). Furthermore, upregulation of IL-17A may also support lipophagy while enhancing bone resorption via osteoclast differentiation (68) (Figure 8B).

In periapical granuloma, L-(+)-lactic acid was the highest unique metabolite. Previously, Lactobacilli were associated to periapical granuloma (11) and they are exclusively producing L(+)-lactic acid (178). PPI revealed the relation between ESR1, ESRRA, and NR0B1 to periapical granuloma. While granuloma formation is highly dependent on estrogen (179), NR0B1 is related to retinoic acid receptor (180), but data about its relation to periapical granuloma were not reported before. The most predominant immune cells found in periapical granuloma were T-helper cells and M2 macrophages. Previously, T-helper 17 was involved (181) in addition to inflammatory M2 macrophage (175). In our study, datasets of the identified active genes revealed that periapical granulomas have the highest correlation with SNPs for PPARD, TSHR, and SLC16A1 in the African population. In agreement with this, some of the samples included in our study were derived from individuals of Egyptian/North African ethnicity. Lawoyin (182) reported that periapical granuloma accounted for the second most common oral lesion after oral neoplasm in the African population, suggesting that undiscovered SNPs could be associated with the high incidence of periapical granuloma in this population. On the other hand, a significant correlation of SNPs in MMP-1 was reported in periapical granuloma (183). We identified L-(+)-lactic acid as a unique metabolite (Figure 8C). This polarizes CD⁴⁺ T cells toward the T-helper 17 phenotype through the stimulation of the transcription factor RORγ (184). Furthermore, lactic acid stimulates RXR-VDR target genes (185) and peroxisome proliferator-activated receptor alpha (PPAR-α) signaling pathway (186). RXR-VDR inhibits MMP-9 (81), while PPAR-α negatively regulates VEGF (187) and TLR4 (88). Additionally, lactic acid polarizes macrophages toward an anti-inflammatory M2 phenotype (188) and favors IL-10 responses (189) and IL-6 release from peripheral blood monocytes (PBMCs) (190) (Figure 8C).

This study is the first to investigate the metabolomic and immunological triggers involved in the development and progression of periapical lesions, yet there are few limitations. First, some of the identified metabolites such as 1-noandecene, 5-5-diethylpentadecane, octadecane, 4,4-dimethoxy-2-methyl-2-butanol, and 2,2-dimethyl-1-octanol, that have been searched in PubChem, did not return any related genes (due to no available literature), so these were excluded from further analysis. Second, when using the CIBERSORT tool, the signature matrix or reference list of immune cell genes, LM22 has a limited number of barcode genes. For this reason, we have included another signature genes list from a previous study (39) with a higher number of barcode genes than the LM22, but unfortunately with limited immune cell profiles. In addition, there are no published data about nonadecane, the shared metabolite in our investigated periapical lesions; thus, future investigations are required. Furthermore, future studies are required to validate our gene expression analyses via a proteomic approach and investigate the pathogenicity of the identified metabolites on different oral cell lines.

Periapical lesions of abscess, cyst, and granuloma differ metabolically and immunologically. In comparison with healthy pulp tissue, periapical abscess is predominant with lipid metabolism of 16-20-HETE and 17-octadecynoic acid pathways. Mediators of inflammation and factors involved in their synthesis, like CYP4F3, VEGF, MMP-9, and IL-8, were associated to more acute inflammatory manifestations. Our analysis suggested that radicular cyst correlates with active proliferative responses, characterized by glycogen and lipophagy processes. Immunological markers such as IL-12A may play a critical role in the maintenance of memory CD8 T cells, in radicular cysts. For periapical granuloma, L-(+)-lactic acid and ethylene glycol clustered together and related to granuloma formation. Nuclear receptor transcription factors RXR/VDR and RORγt (which shares sequence similarity with RXR) may be involved in periapical granuloma, supported by substantial expression of IL-17A.

The datasets presented in this study can be found in online repositories. The names of the repository/repositories and accession number(s) can be found in the article/Supplementary Material.

The studies involving human participants were reviewed and approved by Research Ethics Committee at the University of Sharjah (Reference number REC-18-12-17-02-S on 17/02/2019). The patients/participants provided their written informed consent to participate in this study.

AA, SS, and RH were responsible for the conception, design, and development of the methodology. AA, SS, and TV shared practical application of the methodology. AA and RH performed the bioinformatics analysis. AA, RH, SS, and LS were responsible for writing and editing the manuscript. RH, SS, and LS supervised the study. SS and RH funded the study. All authors contributed to the article and approved the submitted version.

This study was funded by the University of Sharjah (Grant No. 1901110132 to SS and Grant Nos. CoV19-0308, MED001, and 1901090254 to RH).

The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest.

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