研究者業績

瓦井 裕也

カワライ ユウヤ  (Yuya Kawarai)

基本情報

所属
千葉大学 医学部附属病院整形外科 助教
学位
医学博士(2018年3月 千葉大学)

研究者番号
20902589
ORCID ID
 https://orcid.org/0000-0002-3321-9389
J-GLOBAL ID
202101003937993679
researchmap会員ID
R000016736

主要な論文

 50
  • Yuya Kawarai, Junichi Nakamura, Shigeo Hagiwara, Miyako Suzuki-Narita, Kazuhide Inage, Seiji Ohtori
    Journal of orthopaedic surgery and research 19(1) 357-357 2024年6月16日  査読有り筆頭著者責任著者
    BACKGROUND: This study aimed to validate alterations in the gene expression of DNA methylation-related enzymes and global methylation in the peripheral blood mononuclear cell (PBMC) and synovial tissues of animal hip osteoarthritis (OA) models. METHODS: Animals were assigned to the control (no treatment), sham (25 µL of sterile saline), and OA (25 µL of sterile saline and 2 mg of monoiodoacetate) groups. Microcomputed tomography scan, histopathological assessment and pain threshold measurement were performed after induction. The mRNA expression of the DNA methylation machinery genes and global DNA methylation in the PBMC and hip synovial tissue were evaluated. RESULTS: The OA group presented with hip joint OA histopathologically and radiologically and decreased pain threshold. The mRNA expression of DNA methyltransferase (Dnmt 3a), ten-eleven translocation (Tet) 1 and Tet 3 in the synovial tissue of the OA group was significantly upregulated. Global DNA methylation in the synovial tissue of the OA group was significantly higher than that of the control and sham groups. CONCLUSIONS: The intra-articular administration of monoiodoacetate induced hip joint OA and decreased pain threshold. The DNA methylation machinery in the synovial tissues of hip OA was altered.
  • Seunghwan Lee, Yuya Kawarai, Jean Ouellet, Lisbet Haglund, Moshe Szyf, Laura S. Stone
    JOURNAL OF PAIN 23(5) 38-39 2022年5月  
  • Yuya Kawarai, Seon Ho Jang, Seunghwan Lee, Magali Millecamps, HyungMo Kang, Stephanie Gregoire, Miyako Suzuki-Narita, Seiji Ohtori, Laura S Stone
    The Spine Journal 21(11) 1938-1949 2021年6月  筆頭著者
    BACKGROUND CONTEXT: Chronic low back pain (LBP) is a multifactorial disorder with complex underlying mechanisms, including associations with intervertebral disc (IVD) degeneration in some individuals. It has been demonstrated that epigenetic processes are involved in the pathology of IVD degeneration. Epigenetics refers to several mechanisms, including DNA methylation, that have the ability to change gene expression without inducing any change in the underlying DNA sequence. DNA methylation can alter the entire state of a tissue for an extended period of time and thus could potentially be harnessed for long-term pain relief. Lifestyle factors, such as physical activity, have a strong influence on epigenetic regulation. Exercise is a commonly prescribed treatment for chronic LBP, and sex-specific epigenetic adaptations in response to endurance exercise have been reported. However, whether exercise interventions that attenuate LBP are associated with epigenetic alterations in degenerating IVDs has not been evaluated. PURPOSE: We hypothesize that the therapeutic efficacy of physical activity is mediated, at least in part, at the epigenetic level. The purpose of this study was to use the SPARC-null mouse model of LBP associated with IVD degeneration to clarify (1) if IVD degeneration is associated with altered expression of epigenetic regulatory genes in the IVDs, (2) if epigenetic regulatory machinery is sensitive to therapeutic environmental intervention, and (3) if there are sex-specific differences in (1) and/or (2). STUDY DESIGN: Eight-month-old male and female SPARC-null and age-matched control (WT) mice (n=108) were assigned to exercise (n=56) or sedentary (n=52) groups. Deletion of SPARC is associated with progressive IVD degeneration and behavioral signs of LBP. The exercise group received a circular plastic home cage running wheel on which they could run freely. The sedentary group received an identical wheel secured in place to prevent rotation. After 6 months, the results obtained in each group were compared. METHODS: After 6 months of exercise, LBP-related behavioral indices were determined, and global DNA methylation (5-methylcytosine) and epigenetic regulatory gene mRNA expression in IVDs were assessed. This project was supported by the Canadian Institutes for Health Research. The authors have no conflicts of interest. RESULTS: Lumbar IVDs from WT sedentary and SPARC-null sedentary mice had similar levels of global DNA methylation (%5-mC) and comparable mRNA expression of epigenetic regulatory genes (Dnmt1,3a,b, Mecp2, Mbd2a,b, Tet1-3) in both sexes. Exercise attenuated LBP-related behaviors, decreased global DNA methylation in both WT (p<.05) and SPARC-null mice (p<.01) and reduced mRNA expression of Mecp2 in SPARC-null mice (p<.05). Sex-specific effects of exercise on expression of mRNA were also observed. CONCLUSIONS: Exercise alleviates LBP in a mouse model. This may be mediated, in part, by changes in the epigenetic regulatory machinery in degenerating IVDs. Epigenetic alterations due to a lifestyle change could have a long-lasting therapeutic impact by changing tissue homeostasis in IVDs. CLINICAL SIGNIFICANCE: This study confirmed the therapeutic benefits of exercise on LBP and suggests that exercise results in sex-specific alterations in epigenetic regulation in IVDs. Elucidating the effects of exercise on epigenetic regulation may enable the discovery of novel gene targets or new strategies to improve the treatment of chronic LBP.
  • Yuya Kawarai, Sumihisa Orita, Junichi Nakamura, Shuichi Miyamoto, Miyako Suzuki, Kazuhide Inage, Shigeo Hagiwara, Takane Suzuki, Takayuki Nakajima, Tsutomu Akazawa, Seiji Ohtori
    Journal of orthopaedic research : official publication of the Orthopaedic Research Society 38(2) 422-430 2020年2月  筆頭著者責任著者
    We investigated the efficacy of duloxetine on hyperalgesia, histopathological and radiographic findings, pain-related sensory innervation of dorsal-root ganglia (DRG), and spinal changes in a rat model of induced hip osteoarthritis (OA). The right hip joints of male Sprague-Dawley rats (n = 6 rats/group) in the Sham group were injected with 25 μl of sterile saline and 25 μl of sterile saline with 2 mg of monosodium iodoacetate (MIA) were injected to the MIA + Vehicle and MIA + Duloxetine groups. We injected duloxetine 20 mg/kg intraperitoneally in the MIA + Duloxetine group 28 days after injection, whereas rats in the MIA + Vehicle group were injected with 0.5 ml of 20% dimethyl sulfoxide. We assessed hyperalgesia, histopathological changes, immunoreactive (-ir) neurons for calcitonin gene-related peptide and activating transcription factor 3 in DRG, and immunoreactive neurons for ionized-calcium-binding adaptor molecule 1 (Iba1) in the dorsal horn of the spinal cord. MIA administration into the hip joint let to mechanical hyperalgesia of the ipsilateral hind paw (p < 0.05). A single injection of duloxetine significantly attenuated it in induced hip OA (p < 0.05) and suppressed the number of Iba1-ir microglia of the ipsilateral dorsal horn (p < 0.05). These results suggest that a single injection of duloxetine suppressed mechanical hyperalgesia and may influence the expression of Iba1 in the microglia of the ipsilateral dorsal horn in the MIA-induced hip OA. This finding implies the inhibitory effects of duloxetine against neuropathic pain, which may lead to a change of microglial activities. © 2019 Orthopaedic Research Society. Published by Wiley Periodicals, Inc. J Orthop Res 38:422-430, 2020.
  • Yuya Kawarai, Sumihisa Orita, Junichi Nakamura, Shuichi Miyamoto, Miyako Suzuki, Kazuhide Inage, Shigeo Hagiwara, Takane Suzuki, Takayuki Nakajima, Tsutomu Akazawa, Seiji Ohtori
    Journal of orthopaedic research : official publication of the Orthopaedic Research Society 36(11) 2978-2986 2018年11月  筆頭著者責任著者
    The aim of this study was to investigate the local production of proinflammatory cytokines, pain-related sensory innervation of dorsal-root ganglia (DRG), and spinal changes in a rat model of induced hip osteoarthritis (OA). Seventy-five Sprague-Dawley rats were used, including 25 controls and 50 injected into the right hip joints (sham group, injected with 25 µl of sterile saline: N = 25; and monosodium iodoacetate (MIA) group, injected with 25 µl of sterile saline with 2 mg of MIA: N = 25). We measured the local production of TNF-α, immunoreactive (-ir) neurons for calcitonin gene-related peptide (CGRP), and growth associated protein-43 (GAP-43) in DRG, and immunoreactive neurons for ionized-calcium-binding adaptor molecule-1 (Iba-1) in the dorsal horn of spinal cord, on post-induction days 7, 14, 28, 42, and 56 (N = 5 rats/group/time point). For post-induction days 7-42, the MIA group presented significantly elevated concentrations of TNF-α than the other groups (p < 0.01), and a higher expression of CGRP-ir in FG-labeled DRG neurons than the sham group (p < 0.01). MIA rats also presented significantly more FG-labeled GAP-43-ir DRG neurons than the sham group on post-induction days 28, 42, and 56 (p < 0.05), and a significantly higher number of Iba-1-ir microglia in the ipsilateral dorsal horn than the other groups, on post-induction days 28, 42, and 56. The results suggest that in rat models, pain-related pathologies due to MIA-induced hip OA, originate from inflammation caused by cytokines, which leads to progressive, chronic neuronal damage that may cause neuropathic pain. © 2018 Orthopaedic Research Society. Published by Wiley Periodicals, Inc. J Orthop Res 36:2978-2986, 2018.
  • Yuya Kawarai, Junichi Nakamura, Takane Suzuki, Shigeo Hagiwara, Michiaki Miura, Seiji Ohtori
    The Journal of arthroplasty 33(8) 2647-2651 2018年8月  筆頭著者責任著者
    BACKGROUND: The purpose of this cadaveric study was to clarify the proximal limit for the subvastus approach (SVA) in total knee arthroplasty to decrease potential vascular injury. METHODS: Seventy embalmed knees underwent a modified SVA using a 14-cm oblique medial incision. Anatomical features of the descending genicular artery (DGA) were investigated with regard to variation, distance of the vessels from surgical landmarks, and sex differences. RESULTS: The DGA was identified in 62 knees (89%), while it was absent in 8 knees (11%); in the latter, the articular, saphenous, and muscular branches arose separately from the femoral artery. The mean distances from the tibial tuberosity and medial joint line to the origin of the DGA were 15.5 ± 1.6 cm and 12.6 ± 1.6 cm, respectively. Both distances were significantly longer in males than in females (P < .01, respectively). A strong positive correlation was found between the distance from the tibial tuberosity to the origin of the DGA and the distance from the medial joint line to the origin of the DGA (Spearman's correlation coefficient, R2 = 0.72, P < .01). A weak positive correlation was found between the distance from the tibial tuberosity to the origin of the DGA and lower leg length (R2 = 0.13, P < .01). No vascular injuries were observed in this surgical exposure. CONCLUSION: The DGA showed several variations and was absent 11% of the time. An oblique medial incision within 14 cm from the tibial tuberosity followed by arthrotomy is considered a safe zone for the SVA.
  • Yuya Kawarai, Satoshi Iida, Junichi Nakamura, Yoshiyuki Shinada, Chiho Suzuki, Seiji Ohtori
    International orthopaedics 41(12) 2487-2493 2017年12月  筆頭著者責任著者
    PURPOSE: The purpose of this study was to clarify the difference in implant alignment between the direct anterior approach (DAA) and the anterolateral approach in the supine position (ALS). METHODS: A retrospective comparative study consisted of 215 consecutive primary total hip arthroplasties using tapered polished and straight cemented-stems via two different minimally invasive approaches (DAA group in 106 hips and ALS group in 109 hips). RESULTS: The cup radiographic anteversion angle was significantly lower in the ALS group than in the DAA group (12.9° versus 16.9°, p = 0.001). The frequency of the safe zone tended to be more favourable in the ALS group than in the DAA group (95% versus 87%, p = 0.052). Stem alignment in the sagittal plane was significantly better in the ALS group than in the DAA group (84% versus 71%, p = 0.022). CONCLUSIONS: Both cup and stem alignments were better in the ALS group than the DAA group.

MISC

 146
  • 溝口 貴大, 山縣 寛之, 平沢 累, 瓦井 裕也, 萩原 茂生, 中村 順一
    関東整形災害外科学会雑誌 55(臨増号外) 225-225 2024年3月  
  • 平沢 累, 山縣 寛之, 瓦井 裕也, 萩原 茂生, 中村 順一
    関東整形災害外科学会雑誌 55(臨増号外) 228-228 2024年3月  
  • 萩原 茂生, 瓦井 裕也, 中村 順一, 大鳥 精司
    別冊整形外科 (84) 50-53 2023年10月  
    <文献概要>はじめに メトトレキサート(MTX)は関節リウマチ(RA)治療のアンカードラッグとして位置づけられ,RA診断後すみやかな投与がすすめられている.本邦では2022年にMTXの皮下注射製剤が承認され,本年『関節リウマチにおけるメトトレキサート(MTX)使用と診療の手引き2023年版』が発刊された.MTXの作用機序や,現在のRA治療における役割,有効性や安全性などについて解説する.
  • 瓦井 裕也, 中村 順一, 萩原 茂生, 大鳥 精司
    別冊整形外科 (84) 54-57 2023年10月  
    <文献概要>はじめに 関節リウマチ(RA)の治療にメトトレキサート(MTX)に代表される従来型合成疾患修飾性抗リウマチ薬(conventional synthetic disease-modifying antirheumatic drugs:csDMARDs)に加え,生物学的疾患修飾性抗リウマチ薬(biological DMARDs:bDMARDs)が使用されるようになり,疾患活動性は大きく改善した.2003年にインフリキシマブが発売されたのを皮切りに,現在では9種類のbDMARDsが使用可能で,3種類のバイオシミラー(biosimilar:BS)も登場した(表1).すべてのbDMARDsに共通する特徴として,(1)静注または皮下注製剤であること,(2)RA患者の臨床症状の改善,骨関節破壊の進行防止,身体機能の改善といった作用を有すること,(3)有効性は発症早期例,生物学的製剤未使用例,MTX併用例で高いことがあげられる.一方で強力な免疫抑制効果に伴い,重篤な感染症を中心とする副作用のリスクが高まることや,高額な医療費が患者や社会保障費上の問題となることに留意する必要がある.したがってbDMARDsを選択する際には,表2にある項目を検討する必要がある.本稿では,各bDMARDsについて当院での治療経験も交え解説する.
  • 中村 順一, 萩原 茂生, 瓦井 裕也, 正田 純平, 鶴見 要介, 寺川 寛朗, 米屋 貴史, 賀 鵬, 平沢 累
    Hip Joint 49(1) 32-36 2023年8月  
    当院で2012~2021年に牽引手術台を用いてDAA-THAを施行した906例(うち初回THA 870例、再置換術36例)の脱臼率と危険因子について検討した。危険因子の候補は「股関節手術歴」「股関節の原疾患(OA/ONFH/外傷/高位脱臼)」「性別」「神経筋疾患の併存」「骨頭径」「Crowe分類」とし、ロジスティック回帰分析を行った。脱臼率は全体で2.2%、初回THA群では1.8%、再置換術群では11.1%であった。有意な危険因子として「股関節手術歴」「股関節の原疾患(ONFHまたは外傷)」「神経筋疾患の併存」が抽出された。

書籍等出版物

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共同研究・競争的資金等の研究課題

 4