Examining the association of MMP-1 gene −1607 (2G/1G) and −519 (A/G) polymorphisms with the risk of osteomyelitis

Kong, Qingzhu; Yu, Jingyin; Yan, Shi; Yin, Wenwu; Zhao, Jingxin; Feng, Zhen; Wei, Junqiang; Wang, Yu; Guo, Long; Yang, Jianing

doi:10.1097/md.0000000000004969

Cited by 4 publications

(4 citation statements)

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“…Seven studies have reported the associations between SNPs and three types of osteomyelitis (posttraumatic, hematogenous, and vascular insufficiency-related bacterial osteomyelitis; Asensi et al, 2003;Montes et al, 2006;Valle-Garay et al, 2013;Jiang et al, 2016;Hou et al, 2018;Perez-Is et al, 2019;Zhao et al, 2020). The other three studies have reported the relationship of SNP with unspecified types of bacterial osteomyelitis (Ocana et al, 2007;Tsezou et al, 2008;Kong et al, 2017). This systematic review involved 1,248 patients with bacterial osteomyelitis, including 719 patients with posttraumatic bacterial osteomyelitis, 190 patients with hematogenous bacterial osteomyelitis, 98 patients with vascular insufficiency-related bacterial osteomyelitis, and 241 patients with unspecified types of bacterial osteomyelitis.…”

Section: Characteristics Of the Included Studiesmentioning

confidence: 99%

“…Serum C-reactive protein (p = 0.017) and IL-6 (p = 0.006) levels were significantly higher in patients with posttraumatic osteomyelitis accompanied with the GG genotype, instead of the CG genotype. Kong et al (2017) have concluded that the G allele of rs1144393 in the MMP1 gene was regarded as a genetic risk factor and carriers of the GG genotype have an increased risk of osteomyelitis.…”

Section: Protein Receptor and Enzymementioning

confidence: 99%

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Genetic Determinants for Bacterial Osteomyelitis: A Focused Systematic Review of Published Literature

Xie

et al. 2021

Front. Genet.

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Background: Osteomyelitis is an inflammatory process characterized by progressive bone destruction. Moreover, chronic bacterial osteomyelitis is regarded as a difficult-to-treat clinical entity due to its long-standing course and frequent infection recurrence. However, the role of genetic factors in the occurrence and development of bacterial osteomyelitis is poorly understood.Methods: We performed a systematic review to assess the frequency of individual alleles and genotypes of single-nucleotide polymorphisms (SNPs) among patients with bacterial osteomyelitis and healthy people to identify whether the SNPs are associated with the risk of developing bacterial osteomyelitis. Then, gene ontology and Kyoto Encyclopedia of Gene and Genomes analyses were performed to identify the potential biological effects of these genes on the pathogenesis of bacterial osteomyelitis.Result: Fourteen eligible studies containing 25 genes were analyzed. In this review, we discovered that the SNPs in IL1B, IL6, IL4, IL10, IL12B, IL1A, IFNG, TNF, PTGS2, CTSG, vitamin D receptor (VDR), MMP1, PLAT, and BAX increased the risk of bacterial osteomyelitis, whereas those in IL1RN and TLR2 could protect against osteomyelitis. The bioinformatic analysis indicated that these osteomyelitis-related genes were mainly enriched in inflammatory reaction pathways, suggesting that inflammation plays a vital role in the development of bacterial osteomyelitis. Furthermore, functional notation for 25 SNPs in 17 significant genes was performed using the RegulomeDB and NCBI databases. Four SNPs (rs1143627, rs16944, rs2430561, and rs2070874) had smaller scores from regulome analysis, implying significant biological function.Conclusion: We systematically summarized several SNPs linked to bacterial osteomyelitis and discovered that these gene polymorphisms could be a genetic factor for bacterial osteomyelitis. Moreover, further large-scale cohort studies are needed to enhance our comprehensive understanding of the development of osteomyelitis to provide earlier individualized preventions and interventions for patients with osteomyelitis in clinical practice.

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Section: Characteristics Of the Included Studiesmentioning

confidence: 99%

Section: Protein Receptor and Enzymementioning

confidence: 99%

Genetic Determinants for Bacterial Osteomyelitis: A Focused Systematic Review of Published Literature

Xie

et al. 2021

Front. Genet.

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“…Recently, growing evidence has shown that single nucleotide polymorphism (SNP) also plays an important role in OM development. Several SNP sites have been found to be associated with the risk of OM development, such as rs16944, rs2234663, rs1143627, rs4251961, and rs1800796 (interleukin, IL genes) ( Alves De Souza et al, 2017 ; Jiang et al, 2020b ), rs45567233 (cathepsin G, CTSG gene) ( Pérez-Is et al, 2019 ), rs1799750, and rs1144393 (matrix metalloproteinase-1, MMP-1 gene) ( Kong et al, 2017 ), implying SNPs participate in OM pathogenesis.…”

Section: Introductionmentioning

confidence: 99%

Vitamin D Receptor Genetic Polymorphisms Associate With a Decreased Susceptibility to Extremity Osteomyelitis Partly by Inhibiting Macrophage Apoptosis Through Inhibition of Excessive ROS Production via VDR-Bmi1 Signaling

Zhao

Wan

et al. 2022

Front. Physiol.

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Background: Previous studies had reported that vitamin D receptor (VDR) gene polymorphisms were related to the development of several inflammatory disorders. However, potential links between such variations and the risk of developing a bone infection and underlying mechanisms remain unclear. This study aimed to analyze potential associations between VDR genetic variations and susceptibility to extremity osteomyelitis (OM) in a Chinese Han population and investigate potential mechanisms.Methods: Between January 2016 and August 2020, altogether 398 OM patients and 368 healthy controls were genotyped for six VDR gene polymorphisms, including ApaI (rs7975232), BsmI (rs1544410), FokI (rs2228570), TaqI (rs731236), GATA (rs4516035), and Cdx-2 (rs11568820) by the SNaPshot genotyping method. Then, male C57BL/6 mice were randomly divided into vitamin D–standard, –excess, –deficient, and –rescued groups. One week after making the model surgery, OM occurrence and severity were assessed using the bacterial count and histopathological staining. In vitro, phagocytosis, apoptosis, and bactericidal ability of macrophages were evaluated by overexpression or knockdown of VDR protein.Results: Significant associations were found among rs7975232, rs1544410, and OM development by the recessive model (AA vs. AC + CC, p = 0.037, OR = 0.594), homozygous model (AA vs. CC, p = 0.033, OR = 0.575), and heterozygous model (CT vs. CC, p = 0.049, OR = 0.610), respectively. Patients with the AA genotype of rs7975232 had a relatively higher mean level of vitamin D than those with AC and CC genotypes (22.5 vs. 20.7 vs. 19.0 ng/ml). Similarly, patients with CT genotype of rs1544410 had a relatively higher mean vitamin D level than those with CC genotype (20.94 vs. 19.89 ng/ml). Outcomes of in vivo experiments showed that the femoral bacterial load of vitamin D–deficient mice was highest among different vitamin D dose groups, with the most severe histopathological features of infection, and vitamin D supplementation partly reversed the changes. While in vitro experiment results revealed that active vitamin D promoted phagocytosis and sterilization of macrophages and inhibited apoptosis during infection. Reactive oxygen species (ROS) inhibitor inhibited apoptosis of macrophages induced by bacterial infection. Active vitamin D inhibited excessive ROS production in macrophages via the VDR-Bmi1 signaling pathway.Conclusion: In this Chinese cohort, ApaI and BsmI are associated with a decreased risk of OM development by influencing serological vitamin D level, the latter of which reduced macrophage apoptosis with inhibition of excessive ROS production via the VDR-Bmi1 signaling pathway.

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“…[ 8 ] CRP and ESR are currently used in all patients suspected of having VO; however, they lack the accuracy to differentiate between patients with and without VO. [ 4 ] Anti-glucosaminidase IgG, [ 9 ] iron-regulated surface determinant protein B, [ 10 ] CCL11/eotaxin, [ 11 ] interleukin-6, [ 11 ] S100 calcium binding protein A11, E-selectin, and matrix metalloproteinase-1 [ 12 ] have been reported as potential biomarkers [ 13 ] ; yet, they have not been used for the clinical diagnosis of VO. A review of the literature, employing a data mining approach using Open Targets Platform ( https://www.targetvalidation.org/ ), [ 14 ] presented a list of VO-associated antigens showing elevated autoantibody responses [ 14 ] ; the results are shown in Supplemental Digital Content (Appendix 2, which lists open target database).…”

Section: Introductionmentioning

confidence: 99%

Potential novel proteomic biomarkers for diagnosis of vertebral osteomyelitis identified using an immunomics protein array technique

Chen¹,

Chang²,

Wang³

et al. 2020

Medicine

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Rationale: Although vertebral osteomyelitis (VO) is commonly associated with high morbidity and high recurrence rate, effective diagnostic and prognostic biomarkers of VO are still lacking. Patients concerns: Case 1: a 60-year-old male had had upper back pain for 3 days. Case 2: a 71-year-old female presented upper back pain for 2 days. Diagnoses: Based on physical examination and findings of magnetic resonance imaging and findings by matrix-assisted laser desorption ionization-time of flight mass spectrometry, they were diagnosed with Staphylococcus aureus VO. Interventions: Using Sengenics Immunome TM Protein Array by analyzing autoantibodies in both VO patients, potential biomarkers of VO were explored. Outcomes: Four subjects with more than 1600 antigens screened while the results showed that 14-3-3 protein gamma, pterin-4-alpha-carbinolamine dehydratase, fructose-bisphosphate aldolase A , and keratin type II cytoskeletal 8 were highly differentially expressed among VO and controls. Relevant auto-antibody profiles were discovered after intra-group and inter-group comparison, and based on functional rationality, an adapter protein 14-3-3 protein gamma, and pterin-4-alpha-carbinolamine dehydratase that involved in tetrahydrobiopterin biosynthesis, might serve as valuable diagnostic biomarkers. Lessons: This pilot study on 4 subjects with more than 1600 antigens screened on the Sengenics Immunome protein array provided a general outlook on autoantibody biomarker profiles of VO subjects. Future large-scale trials with longer follow-up times are warranted.

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Examining the association of MMP-1 gene −1607 (2G/1G) and −519 (A/G) polymorphisms with the risk of osteomyelitis

Cited by 4 publications

References 35 publications

Genetic Determinants for Bacterial Osteomyelitis: A Focused Systematic Review of Published Literature

Genetic Determinants for Bacterial Osteomyelitis: A Focused Systematic Review of Published Literature

Vitamin D Receptor Genetic Polymorphisms Associate With a Decreased Susceptibility to Extremity Osteomyelitis Partly by Inhibiting Macrophage Apoptosis Through Inhibition of Excessive ROS Production via VDR-Bmi1 Signaling

Potential novel proteomic biomarkers for diagnosis of vertebral osteomyelitis identified using an immunomics protein array technique

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