JP2009527570A - セルライト処置用コラゲナーゼ - Google Patents
セルライト処置用コラゲナーゼ Download PDFInfo
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Abstract
Description
本願は、2006年2月22日に米国特許商標庁に出願された出願番号60/775,690号に対して優先権を主張する。
本発明は、国立衛生研究所からの助成金M01RR10710によって、一部支持された。米国政府は、本発明に対して一定の権利を有する。
大腿部および臀部の皮膚の陥凹形成、すなわち「マットレス現象」は、一般的にセルライトといわれる。この状態は共通であり、そうでなければ健康な個体に現れ、男性よりはるかに高い頻度で女性が罹患する。セルライト除去のための、処方箋が不要な局所療法が多くある。これらの製品および処方箋が不要な局所への適用は、役に立たず、費用がかかり、実際に、適切なプラセボコントロールされた臨床試験を経たことがない。局所レチノールならびにカフェインおよびルスコゲニン(ruscogenine)を含むレチノールの、最近のランダム化されたプラセボコントロールされた試験(trail)はまた、セルライトの除去に関する価値を示せなかった。
本発明は、コラゲナーゼ注射が、ヒトのセルライトのコラーゲンセプタエネットワークを溶解し、セルライトを処置し、および平坦な皮膚の外観を回復するのに有効であるという発見に関する。本発明は、処置を必要とする被験体においてセルライトを処置する方法に関し、該方法は、セルライトを処置するための医薬の製造において有効量の精製されたコラゲナーゼを注入する工程を含む。コラゲナーゼは、好ましくは、精製されており、プロテアーゼおよび/またはヒアルロニダーゼ等の他の酵素を実質的に含まない。
本発明は、コラゲナーゼ注射が、ヒトのセルライトのコラーゲンセプタエネットワークを溶解し、セルライトを処置し、および平坦な皮膚の外観を回復するのに有効であるという発見に関する。本発明は、処置を必要とする被験体においてセルライトを処置する方法に関し、該方法は、大腿部および/または臀部に有効量のコラゲナーゼを注入する工程を含む。本発明はまた、セルライトを処置するための医薬の製造におけるコラゲナーゼの使用に関する。
切断されるペプチド結合の数は、ニンヒドリンとの反応によって測定される。可溶化消化コントロールによって放出されるアミノ基は、減算される。正味の1ABC単位のコラゲナーゼは、1分あたり1.09ナノモルのロイシンに等価なニンヒドリン反応性物質を可溶化する。1SRC単位は、約6.3ABC単位と等しい。
方法
十名の患者が研究プロトコールに参加した。全てが女性で、平均年齢は41歳=10歳。平均ボディマス指数(BMI)は28であった。
全ての患者が、コラゲナーゼの注入後に標的大腿部のセルライトの減少を体験した。表1は、処置された患者の大腿部の四半部におけるセルライトが減少するという結果を示す。注入された領域(are)のセルライトの出現の有意な減少があった。セルライト領域(are)は、1日目までにベースラインと比較して77%減少した。この結果はより長期間維持された。ベースラインと比較して、セルライトの領域は1週間で74%、1ヶ月で89%、3ヶ月で86%、そして6ヶ月で76%減少した。
Claims (16)
- 処置を必要としている被験体においてセルライトを処置する方法であって、有効量の精製されたコラゲナーゼをセルライトのコラーゲン性隔膜ネットワーク(collagenous septa network)に送達する工程を含む方法。
- コラゲナーゼ(クロストリジオペプチダーゼA)が細菌クロストリジウム・ヒストリチカム(Clostridium hisolyticum)に由来する、請求項1記載の方法。
- 精製されたコラゲナーゼが単独で投与される、請求項1記載の方法。
- 精製されたコラゲナーゼが、トリアムシノロン(traimcinolone)または他のコルチコステロイドの非存在下で投与される、請求項1記載の方法。
- 精製されたコラゲナーゼが少なくとも約700SRC単位を含む投与量で注入され、一回以上の注入で加えられる、請求項1記載の方法。
- 精製されたコラゲナーゼが少なくとも約1000SRC単位を含む投与量で注入され、一回以上の注入で加えられる、請求項1記載の方法。
- 精製されたコラゲナーゼが少なくとも約1500SRC単位を含む投与量で注入され、一回以上の注入で加えられる、請求項1記載の方法。
- 精製されたコラゲナーゼが少なくとも約10000ABC単位を含む投与量で注入され、一回以上の注入で加えられる、請求項1記載の方法。
- 精製されたコラゲナーゼが、約1.0mLの体積で注入される、請求項1記載の方法。
- 精製されたコラゲナーゼが複数の部位で注入される、請求項1記載の方法。
- 精製されたコラゲナーゼがコラゲナーゼIおよびコラゲナーゼIIから構成される、請求項1記載の方法。
- 注入が、皮膚の陥凹形成を特徴とするセルライトの領域に送達される、請求項9記載の方法。
- 被験体がヒト患者である、請求項1記載の方法。
- 処置が約4〜6週間後に繰り返される、請求項1記載の方法。
- コラゲナーゼの少なくとも一回の投与を受けた1ヵ月後に、患者がセルライトの出現の目視による有意な減少を達成する、請求項1記載の方法。
- 精製されたコラゲナーゼが約500SRC単位/mg〜約15,000SRC単位/mgを含む投与量で注入され、一回以上の注入で加えられる、請求項1記載の方法。
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PCT/US2007/004752 WO2007100675A2 (en) | 2006-02-22 | 2007-02-22 | Collagenase for treating cellulite |
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JP4967081B2 (ja) * | 2005-01-21 | 2012-07-04 | ザ リサーチ ファウンデーション オブ ステート ユニバーシティ オブ ニューヨーク | 癒着性関節包炎の処置方法 |
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TWI395593B (zh) | 2008-03-06 | 2013-05-11 | Halozyme Inc | 可活化的基質降解酵素之活體內暫時性控制 |
JP5649589B2 (ja) * | 2009-03-06 | 2015-01-07 | ハロザイム インコーポレイテッド | マトリックスメタロプロテアーゼ1の温度感受性突然変異体およびその使用 |
FR2966734B1 (fr) | 2010-10-29 | 2014-07-18 | Max Rombi | Composition comprenant au moins une enzyme proteolytique pour son utilisation pour empecher la synthese des triglycerides |
DK2802652T3 (da) | 2012-01-12 | 2019-07-15 | Endo Global Ventures | Clostridium histolyticum enzym |
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US20150196625A9 (en) | 2013-01-07 | 2015-07-16 | Rudolph D. Paladini | Metal Sensitive Mutants of Matrix Metalloproteases and uses thereof |
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KR20240001279A (ko) | 2017-03-28 | 2024-01-03 | 엔도 벤쳐즈 리미티드 | 개선된 콜라게나제 생성 방법 |
WO2020021330A2 (en) * | 2018-07-12 | 2020-01-30 | Endo Global Aesthetics Limited | Injection techniques for the treatment of cellulite |
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AU2019341663A1 (en) * | 2018-09-18 | 2021-04-22 | Endo Global Aesthetics Limited | Compositions and methods for treating cellulite |
AU2020204922A1 (en) * | 2019-01-06 | 2021-07-01 | Endo Global Aesthetics Limited | Collagenase formulations and methods of producing the same |
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US20220409511A1 (en) * | 2019-11-26 | 2022-12-29 | Standard Of Care Corporation | Hyaluronidase compositions and methods of using same to treat cellulite |
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