数量	カタログ番号	注文内容	Qty/Pk	価格
			96-Well Plate

数量	カタログ番号	注文内容	Qty/Pk	価格
	48-602MAG	Buffer Detection Kit for Magnetic Beads	1 Kit

PF024 Sigma-AldrichMMP-9, Active, Human, Recombinant

MMP-9, Active, Human, Recombinant: のSDS（安全データシート）、CoA（試験成績書）およびCoQ（品質証明書）、カタログなど製品関連の技術資料を入手いただけます。

(M)SDS
試験成績書（CoA）
参考資料
Data Sheet

同義語: Gelatinase B, 83 kDa Gelatinase, Matrix Metalloproteinase 9

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概要

Replacement Information

価格＆在庫状況

カタログ番号	在庫状況	包装	Qty/Pk	価格	数量
PF024-5UGCN	在庫状況検索中… — 現在国内在庫なし現在国内在庫有り販売中止在庫僅少現在国内在庫あり在庫を照会するにはログインしてください現在国内在庫有り現在国内在庫なし現在国内在庫有り Remaining : Will advise Remaining : Will advise 注文対象外お問合せください Contact Customer Service お問合せくださいお問合せください	樹脂ｱﾝﾌﾟﾙ	5 μg	価格を検索中… 価格が見つかりません Minimum Quantity needs to be mulitiple of Maximum Quantity is 弊社照会詳細を表示　値引 () — 弊社照会納入価格を閲覧するにはログインしてください	在庫状況を照会 —	お気に入り/ショッピングリストに追加お気に入り/ショッピングリストに追加お気に入りに追加されました

Description
Overview	Recombinant, human MMP-9 purified from transfected mammalian cells and activated with APMA. Active MMP-9 enzyme is APMA-free.
Catalogue Number	PF024
Brand Family	Calbiochem®
Synonyms	Gelatinase B, 83 kDa Gelatinase, Matrix Metalloproteinase 9

References
References	Parsons, S.L., et al. 1997. Br. J. Surg. 84, 160. Backstrom, J.R., et al. 1996. J. Neuro. 16, 7910. Lim, G.P., et al. 1996. J. Neurochem. 67, 251. Xia, T., et al. 1996. Biochim. Biophys. Acta 1293, 259. Sang, Q.X., et al. 1995. Biochim. Biophys. Acta 1251, 99. Zempo, N., et al. 1994. J. Vasc. Surg. 20, 217. Birkedal-Hansen, H. 1993. J. Periodontol. 64, 484. Stetler-Stevenson, W.G., et al. 1993. FASEB J. 7, 1434. Jeffrey, J.J. 1991. Semin. Perinatol. 15, 118. Liotta, L.A., et al. 1991. Cell 64, 327. Harris, E. 1990. N. Engl. J. Med. 322, 1277.

References

Parsons, S.L., et al. 1997. Br. J. Surg. 84, 160.
Backstrom, J.R., et al. 1996. J. Neuro. 16, 7910.
Lim, G.P., et al. 1996. J. Neurochem. 67, 251.
Xia, T., et al. 1996. Biochim. Biophys. Acta 1293, 259.
Sang, Q.X., et al. 1995. Biochim. Biophys. Acta 1251, 99.
Zempo, N., et al. 1994. J. Vasc. Surg. 20, 217.
Birkedal-Hansen, H. 1993. J. Periodontol. 64, 484.
Stetler-Stevenson, W.G., et al. 1993. FASEB J. 7, 1434.
Jeffrey, J.J. 1991. Semin. Perinatol. 15, 118.
Liotta, L.A., et al. 1991. Cell 64, 327.
Harris, E. 1990. N. Engl. J. Med. 322, 1277.

Product Information
Activity	ΔA₄₀₅/hour/µg protein ≥8.0 in standard thiopeptolide hydrolysis assays.
EC number	3.4.24.35
Form	Liquid
Formulation	In 50 mM HEPES, 10 mM CaCl₂, 20% glycerol, 0.005% BRIJ^®-35 Detergent, pH 7.5.
Preservative	None
Quality Level	MQ200

Applications
Application References	Zymography Xia, T., et al. 1996. Biochim. Biophys. Acta 1293, 259. Kleiner, D.E. and Stetler-Stevenson W.G. 1994. Anal. Biochem. 218, 325. Heussen, C. and Dowdle, E.B. 1980. Anal. Biochem. 102, 196. Substrate cleavage assay Xia, T., et al. 1996. Biochim. Biophys. Acta 1293, 259.

Biological Information
Purity	≥90% by SDS-PAGE
Concentration Label	Please refer to vial label for lot-specific concentration

Physicochemical Information

Dimensions

Materials Information

Toxicological Information

Safety Information according to GHS

Safety Information

Product Usage Statements

Storage and Shipping Information
Ship Code	Dry Ice Only
Toxicity	Standard Handling
Storage	≤ -70°C
Avoid freeze/thaw	Avoid freeze/thaw
Do not freeze	Ok to freeze
Special Instructions	Following initial use, aliquot into siliconized vials and freeze (-70°C).

Packaging Information

Transport Information

Supplemental Information

Specifications

Global Trade Item Number
カタログ番号	GTIN
PF024-5UGCN	07790788056438

Documentation

MMP-9, Active, Human, Recombinant (M)SDS

タイトル
英語版製品安全データシート（(M)SDS）

MMP-9, Active, Human, Recombinant 試験成績書（CoA）

タイトル	ロット番号
PF024	ロット番号を入力

参考資料

参考資料の概要
Parsons, S.L., et al. 1997. Br. J. Surg. 84, 160. Backstrom, J.R., et al. 1996. J. Neuro. 16, 7910. Lim, G.P., et al. 1996. J. Neurochem. 67, 251. Xia, T., et al. 1996. Biochim. Biophys. Acta 1293, 259. Sang, Q.X., et al. 1995. Biochim. Biophys. Acta 1251, 99. Zempo, N., et al. 1994. J. Vasc. Surg. 20, 217. Birkedal-Hansen, H. 1993. J. Periodontol. 64, 484. Stetler-Stevenson, W.G., et al. 1993. FASEB J. 7, 1434. Jeffrey, J.J. 1991. Semin. Perinatol. 15, 118. Liotta, L.A., et al. 1991. Cell 64, 327. Harris, E. 1990. N. Engl. J. Med. 322, 1277.

参考資料の概要

データシート

Note that this data sheet is not lot-specific and is representative of the current specifications for this product. Please consult the vial label and the certificate of analysis for information on specific lots. Also note that shipping conditions may differ from storage conditions.

Revision	06-July-2010 JSW
Synonyms	Gelatinase B, 83 kDa Gelatinase, Matrix Metalloproteinase 9
Description	Recombinant, human MMP-9 purified from transfected mammalian cells and activated with APMA. Active MMP-9 enzyme is APMA-free. Supplied as the ~83 kDa active enzyme. The proenzyme form of MMP-9 was purified from transfected mammalian cells and activated using the organomercurial compound, 4-aminophenyl mercuric acetate (APMA). APMA is removed through a desalting column. The substrate specificity for MMP-9 is collagen (types IV, V, VII, and X), elastin, and gelatin (type I). Useful for immunoblotting, substrate cleavage, and zymography. Titration is recommended for optimal results in individual systems. Matrix metalloproteinases are members of a unique family of proteolytic enzymes that have a zinc ion at their active sites and can degrade collagens, elastin and other components of the extracellular matrix (ECM). These enzymes are present in normal healthy individuals and have been shown to have an important role in processes such as wound healing, pregnancy, and bone resorption. However, overexpression and activation of MMPs have been linked with a range of pathological processes and disease states involved in the breakdown and remodeling of the ECM. Such diseases include tumor invasion and metastasis, rheumatoid arthritis, periodontal disease, and vascular processes such as angiogenesis, intimal hyperplasia, atherosclerosis, and aneurysms. Recently, MMPs have been linked to neurodegenerative diseases such as Alzheimer's, and amyotrophic lateral sclerosis (ALS). Natural inhibitors of MMPs, tissue inhibitor of matrix metalloproteinases (TIMPs) exist and synthetic inhibitors have been developed which offer hope of new treatment options for these diseases. Regulation of MMP activity can occur at the level of gene expression, including transcription and translation, level of activation, or at the level of inhibition by TIMPs. Thus, perturbations at any of these points can theoretically lead to alterations in ECM turnover. Expression is under tight control by pro- and anti-inflammatory cytokines and/or growth factors and, once produced the enzymes are usually secreted as inactive zymograms. Upon activation (removal of the inhibitory propeptide region of the molecules) MMPs are subject to control by locally produced TIMPs. All MMPs can be activated in vitro with organomercurial compounds (e.g. 4-aminophenylmercuric acetate), but the agents responsible for the physiological activation of all MMPs have not been clearly defined. Numerous studies indicate that members of the MMP family have the ability to activate one another. The activation of the MMPs in vivo is likely to be a critical step in terms of their biological behavior, because it is this activation that will tip the balance in favor of ECM degradation. The hallmark of diseases involving MMPs appear to be stoichiometric imbalance between active MMPs and TIMPs, leading to excessive tissue disruption and often degradation. Determination of the mechanisms that control this imbalance may open up some important therapeutic options of specific enzyme inhibitors.
Form	Liquid
Formulation	In 50 mM HEPES, 10 mM CaCl₂, 20% glycerol, 0.005% BRIJ^®-35 Detergent, pH 7.5.
Concentration Label	Please refer to vial label for lot-specific concentration
EC number	3.4.24.35
Purity	≥90% by SDS-PAGE
Activity	ΔA₄₀₅/hour/µg protein ≥8.0 in standard thiopeptolide hydrolysis assays.
Preservative	None
Storage	Avoid freeze/thaw ≤ -70°C
Do Not Freeze	Ok to freeze
Special Instructions	Following initial use, aliquot into siliconized vials and freeze (-70°C).
Toxicity	Standard Handling
References	Parsons, S.L., et al. 1997. Br. J. Surg. 84, 160. Backstrom, J.R., et al. 1996. J. Neuro. 16, 7910. Lim, G.P., et al. 1996. J. Neurochem. 67, 251. Xia, T., et al. 1996. Biochim. Biophys. Acta 1293, 259. Sang, Q.X., et al. 1995. Biochim. Biophys. Acta 1251, 99. Zempo, N., et al. 1994. J. Vasc. Surg. 20, 217. Birkedal-Hansen, H. 1993. J. Periodontol. 64, 484. Stetler-Stevenson, W.G., et al. 1993. FASEB J. 7, 1434. Jeffrey, J.J. 1991. Semin. Perinatol. 15, 118. Liotta, L.A., et al. 1991. Cell 64, 327. Harris, E. 1990. N. Engl. J. Med. 322, 1277.
Application references	Zymography Xia, T., et al. 1996. Biochim. Biophys. Acta 1293, 259. Kleiner, D.E. and Stetler-Stevenson W.G. 1994. Anal. Biochem. 218, 325. Heussen, C. and Dowdle, E.B. 1980. Anal. Biochem. 102, 196. Substrate cleavage assay Xia, T., et al. 1996. Biochim. Biophys. Acta 1293, 259.

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Life Science Research > タンパク質と酵素 > Other Enzymes

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