研究者業績

稲毛 一秀

イナゲ  (Kazuhide Inage)

基本情報

所属
千葉大学 大学院医学研究院 整形外科学 助教

研究者番号
80793629
J-GLOBAL ID
202101008138224648
researchmap会員ID
R000028120

主要な研究キーワード

 4

学歴

 1

論文

 1127
  • Soichiro Tokeshi, Miyako Suzuki‐Narita, Ikuko Tajiri, Kazuhide Inage, Jun Takeuchi, Takahito Arai, Yuya Kawarai, Hiroakira Terakawa, Seiji Ohtori, Sumihisa Orita
    Journal of Orthopaedic Research 2024年11月11日  
    Abstract Diclofenac etalhyaluronate (DF‐HA) sustained diclofenac release with the effects of hyaluronic acid (HA), offering long‐term analgesia in osteoarthritis. In this study, the effects of DF‐HA on pain improvement and osteoarthritis were evaluated in a rat knee monoiodoacetate‐induced osteoarthritis model compared to HA. Eight rats per group had been injected with monoiodoacetate (2.0 mg) or saline in the right knee for 4 weeks and were injected with either DF‐HA (1.25 mg/kg; 0.5 mg), HA (0.5 mg), vehicle which was a substrate without DF‐HA (50 μL), or saline and followed for 4 weeks. Mechanical plantar skin sensitivity was assessed weekly using the von Frey assay. Osteoarthritis changes were monitored with Larsen scores via CT imaging at every 2 weeks. The articular cartilage was analyzed using OARSI scores through H&E, Safranin‐O staining at 8 weeks. The percentage of Iba‐1 positive microglia in the spinal dorsal horn and of FG + CGRP‐labeled cells among FG‐positive cells in the dorsal root ganglion were evaluated by immunohistochemical staining. TNF‐α and IL‐6 mRNA expression levels in the knee synovium were evaluated by PCR. The DF‐HA showed significantly improved pain hypersensitivity compared with the HA at 6–8 weeks. The percentage of Iba‐1‐positive microglia was significantly lower than that in the vehicle and the percentage of FG + CGRP/FG was significantly lower than that in the HA. OARSI scores did not differ among treatment groups, Larsen scores indicated lower in the DF‐HA than in the vehicle. DF‐HA was as effective as HA in joint protection and significantly improved inflammatory pain compared to HA.
  • Hiroto Chikubu, Kazuhide Inage, Sumihisa Orita, Yasuhiro Shiga, Masahiro Inoue, Keisuke Shimizu, Miyako Suzuki-Narita, Ikuko Tajiri, Michiaki Mukai, Natsuko Nozaki-Taguchi, Seiji Ohtori
    Journal of orthopaedic research : official publication of the Orthopaedic Research Society 2024年9月22日  
    Co-administration of mirogabalin besylate and nonsteroidal anti-inflammatory drugs is effective for neuropathic pain; however, mechanism of its action remains unknown. We aimed to evaluate the mechanism of this synergistic effect of the concomitant administration for neuropathic pain using chronic constriction injury model rats. Fifty male Wister rats of 7-week-old were used. Right sciatic nerve ligation was performed in 40 rats and they were sub-divided into four groups: vehicle, mirogabalin, diclofenac sodium and co-administration of them. Ten rats underwent sham surgery. Fluorogold was attached to sciatic nerve during surgery. Von Frey filament and weight bearing tests were performed on postoperative Day 6 as behavioral assessments and drug was administrated intraperitoneally. Half rats in each group underwent behavioral assessment and perfusion fixation using 4% paraformaldehyde on postoperative Day 7 and remaining on postoperative Day 14. Subsequently, dorsal root ganglion at L4 to L6 was collected and examined immunohistochemistry for calcitonin gene-related peptide, and their immunoreactivity in fluorogold-labeled neurons was measured. Spinal cord at lumbar swelling was resected, immunostained for ionized-calcium-binding adapter molecule-1 and glial fibrillary acidic protein, and immunoreactive neurons in dorsal horn of spinal cords were calculated as the occupancy of them. Mirogabalin suppresses the neuropeptide-release from presynaptic afferent neuron directly and it resulted in suppressing glia cells activation. Diclofenac sodium inhibits cyclooxygenase-2 and prostaglandin production, related to allodynia. These effects of mirogabalin and diclofenac sodium, respectively, inhibited glia cells strongly, which is presumed to be one of the mechanisms for the effectiveness of their co-administration for neuropathic pain.
  • Masahiro Inoue, Shiro Sugiura, Taiki Takeda, Takato Hoshino, Keisuke Shimizu, Kazuhide Inage, Yasuhiro Shiga, Kohei Okuyama, Seiji Ohtori, Sumihisa Orita
    Cureus 2024年8月26日  
  • 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  
    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.
  • Takahito Arai, Yasuhiro Shiga, Michiaki Mukai, Naoya Takayama, Susumu Tashiro, Ikuko Tajiri, Kentaro Kosaka, Masashi Sato, Sou Nakamura, Haruki Okamoto, Seiji Kimura, Kazuhide Inage, Miyako Suzuki-Narita, Yawara Eguchi, Sumihisa Orita, Koji Eto, Seiji Ohtori
    Regenerative therapy 26 850-858 2024年6月  
    INTRODUCTION: Platelet-rich plasma obtained by centrifuging peripheral blood can promote osteogenesis owing to its abundant growth factors but has drawbacks, including rapid growth factor loss and inconsistent effects depending on donor factors. To overcome these issues, we were the first in the world to use freeze-dried human induced pluripotent stem cell-derived megakaryocytes and platelets (S-FD-iMPs) and found that they have osteogenesis-promoting effects. Since turbulence was found to activate platelet biogenesis and iPS cell-derived platelets can now be produced on a clinical scale by a device called VerMES, this study examined the osteogenesis-promoting effect and safety of clinical-scale FD-iMP (V-FD-iMPs) for future human clinical application. METHOD: We administered either S-FD-iMPs, V-FD-iMPs, or saline along with artificial bone to the lumbar spine of 8-week-old male Sprague-Dawley rats (n = 4 each) and evaluated bone formation by computed tomography (CT) and pathology. Next, we administered V-FD-iMPs or saline along with artificial bone to the lumber spines of 5-week-old male New Zealand White rabbits (n = 4 each) and evaluated the bone formation by CT and pathology. Rats (n = 10) and rabbits (n = 6) that received artificial bone and V-FD-iMPs in the lumbar spine were also observed for 6 months for adverse events, including infection, tumor formation, and death. RESULTS: Both V-FD-iMPs and S-FD-iMPs significantly enhanced osteogenesis in the lumber spines of rats in comparison with the controls 8 weeks postoperatively, with no significant differences between them. Furthermore, V-FD-iMPs vigorously promoted osteogenesis in the lumber spines of rabbits 8 weeks postoperatively. In rats and rabbits, V-FD-iMPs showed no adverse effects, including infection, tumor formation, and death, over 6 months. CONCLUSION: These results suggest that V-FD-iMPs promote safe osteogenesis.

MISC

 65
  • 大鳥 精司, 志賀 康浩, 折田 純久, 江口 和, 稲毛 一秀, 牧 聡, 古矢 丈雄
    関節外科 41(7) 728-740 2022年7月  
    <文献概要>腰椎疾患は多岐にわたり保存治療が最優先であるが,症状が軽快しない場合,侵襲的な治療が選択される。腰痛や長期的に障害を受けた場合の下肢筋力の低下や萎縮,足底のしびれなどは残存する可能性が高い。また,多数回手術後のfailed back surgery syndromeは難治性であり,注意を要する。
  • 江口 和, 折田 純久, 稲毛 一秀, 志賀 康浩, 大鳥 精司
    整形外科 73(6) 590-596 2022年5月  
    <文献概要>はじめに 社会の高齢化に伴い,脊椎疾患患者が増加の一途をたどっており,米国では国民の約3割が慢性疼痛を有し,年間8兆円の医療損失を生じているとされ医療費高騰の一因となっている.痛みは局所の刺激から末梢神経,脊髄を経由して大脳に伝わり,痛みとして認識される.近年,神経機能イメージングとして,脳機能に関してはfunctional MRI(fMRI)やMR spectroscopyが盛んに行われている.一方,腰神経障害は腰痛・下肢痛の原因となるが,無症候性の椎間板変性およびヘルニアがしばしば散見され,従来のMRIでは画像上の神経根圧迫が必ずしも痛みの原因とはならないことも多く,画像診断が進歩した現代でも,損傷神経の可視化,痛みの定量化など機能評価は不可能であった.もう一つ,画像診断のなかで解決されていない課題に,腰椎椎間孔狭窄の画像診断がある.腰椎椎間孔狭窄は脊椎退行性変化により椎間孔内外で神経根・腰神経が絞扼を受ける病態であり,同部位には痛覚受容器である後根神経節が存在し,激しい下肢痛を生じ,難治性である.この領域はMacnabがhidden zoneと紹介したごとく,画像診断法が進歩した現代でも見落とされやすく,手術成績を悪化させる一因となる.特に椎間孔狭窄の手術は固定術となることが多く,診断が重要となる(図1a).腰椎椎間孔狭窄の画像診断は,単純X線検査,CT,MRI,さらに選択的神経根造影・ブロックなど機能的診断を組み合わせ総合的に診断する.従来のMRIでは脂肪像の消失として診断されるが,偽陽性率は30〜40%と報告され診断困難である(図1b).このように現在のMRIでは脊髄を分岐した脊髄神経,腕神経叢,腰神経など外側病変を画像診断することは困難であり,新しい画像診断法が望まれている.近年,MRI装置の高磁場化やパルスシーケンスの改良に伴い,より高分解能のニューロイメージングが可能になった.MR neurogaraphyは,造影剤を用いることなく非侵襲的かつ選択的に末梢神経を描出する方法として,拡散テンソル画像(diffusion tensor imaging:DTI),拡散強調MR neurography,などさまざまな手法が報告されている.本稿では,DTI,拡散強調MR neurographyによる脊髄神経由来の痛みを可視化する手法について紹介する.
  • 大鳥 精司, 金 勤東, 新井 隆仁, 穂積 崇史, 小田切 拓磨, 向畑 智仁, 俊 徳保, 古矢 丈雄, 折田 純久, 稲毛 一秀, 牧 聡, 志賀 康浩, 江口 和
    関節外科 41(4月増刊) 116-124 2022年4月  
    <文献概要>Point ▼脊髄造影の適応,手技を提示する。▼神経根ブロックや神経根造影の適応,手技,治療効果を提示する。▼脊髄造影,神経根ブロック,神経根造影の合併症を提示する。
  • 宮城 正行, 村田 幸佑, 藤巻 寿子, 高橋 真治, 堀 悠介, 星野 雅俊, 中村 博亮, 稲毛 一秀, 大鳥 精司, 井上 玄, 高相 晶士
    日本整形外科学会雑誌 96(2) S6-S6 2022年3月  
  • 田中 慶秀, 宮城 正行, 高橋 真治, 稲毛 一秀, 星野 雅俊, 堀 悠介, 折田 純久, 井上 玄, 大鳥 精司, 中村 博亮, 高相 晶士
    日本整形外科学会雑誌 96(2) S301-S301 2022年3月  

共同研究・競争的資金等の研究課題

 7

産業財産権

 1