Recombinant Human Gastric Lipase/LIPF HA-tag His-tag, CF

R&D Systems, part of Bio-Techne | Catalog # 11772-GL

R&D Systems, part of Bio-Techne
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11772-GL-050
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Key Product Details

Source

CHO

Accession #

P07098.1

Conjugate

Unconjugated

Applications

Enzyme Activity

View all Gastric Lipase Proteins and Enzymes »

Product Specifications

Source

Chinese Hamster Ovary cell line, CHO-derived human Gastric Lipase protein
Leu20-Lys398 with N-terminal HA (YPYDPDYA) and 6-His tags

Purity

>95%, by SDS-PAGE visualized with Silver Staining and quantitative densitometry by Coomassie® Blue Staining.

Endotoxin Level

<0.10 EU per 1 μg of the protein by the LAL method.

N-terminal Sequence Analysis

Tyr

Predicted Molecular Mass

45 kDa

SDS-PAGE

49-54 kDa, under reducing conditions

Activity

Measured by its ability to cleave a fluorogenic substrate, 4-Methylumbelliferyl oleate (4-MUO).
The specific activity is >4500 pmol/min/μg as measured under the described conditions.

Scientific Data Images for Recombinant Human Gastric Lipase/LIPF HA-tag His-tag, CF

Recombinant Human Gastric Lipase/LIPF HA-tag His-tag Enzyme Activity.

Recombinant Human Gastric Lipase/LIPF HA-tag His-tag (Catalog # 11772-GL) is measured by its ability to cleave a fluorogenic substrate, 4-Methylumbelliferyl oleate (4-MUO).

Recombinant Human Gastric Lipase/LIPF HA-tag His-tag SDS-PAGE.

2 μg/lane of Recombinant Human Gastric Lipase/LIPF HA-tag His-tag (Catalog # 11772-GL) was resolved with SDS-PAGE under reducing (R) and non-reducing (NR) conditions and visualized by Coomassie® Blue staining, showing bands 49-54 kDa, under reducing conditions.

Formulation, Preparation and Storage

11772-GL
Formulation Supplied as a 0.2 μm filtered solution in Tris, NaCl and Glycerol.
Shipping The product is shipped with polar packs. Upon receipt, store it immediately at the temperature recommended below.
Stability & Storage Use a manual defrost freezer and avoid repeated freeze-thaw cycles.
  • 6 months from date of receipt, -20 to -70 °C as supplied.
  • 3 months, -20 to -70 °C under sterile conditions after opening.

Background: Gastric Lipase

Recombinant human Gastric triacylglycerol lipase or gastric lipase (GL), from the gene LIPF, is a 379 residue mature, glycosylated, secreted serine hydrolase of a family of three mammalian acid lipases. Mature GL/LIPF contains a globular core domain typical of a/b hydrolase-fold family members and an extrusion domain that covers the core domain and functions like a lid. Beneath the lid region, the core domain contains the catalytic triad surrounded by a hydrophobic surface that promotes lipid substrate binding (1). The lid domain inhibits binding of substrate and requires conformational change for adsorption at the interface of emulsified triacylglycerol in the presence of phospholipids and proteins to facilitate activity (2). GL/LIPF is secreted by the mucosal cells of the stomach where it initiates the digestion of dietary triglyceride fat through its preference for hydrolysis at the ester bond at carbon 3 (1, 3, 4). Although GL/LIPF contributes to a lower effect in the hydrolysis of dietary fats in the stomach than pancreatic lipase (PL) in the small intestine, gastric lipolysis contributes significantly to overall lipolysis and has an important role in promoting the action of pancreatic lipolytic enzymes through its actions (2,5-8). Therefore, inhibition of GL/LIPF along with PL, such as through the action of Orlistat, has been identified as a target for the prevention and treatment of obesity-related disorders such as diabetes, dyslipidemia, nonalcoholic fatty liver disease and cardiovascular disease (8-12). With a few available lipase inhibitors already in use in the clinic to manage obesity and its related disorders, significant investigation and development of additional or alternative inhibitors with fewer side effects is underway (3, 8). Recombinant GL/LIPF is recognized as a good candidate for enzyme replacement therapies for pancreatic enzyme insufficiency observed in chronic pancreatitis and cystic fibrosis (CF) due to its unique properties; unlike PL, no cofactor is required for GL/LIPF activity, GL/LIPF retains activity at low pH and in the presence of proteases, and GL/LIPF is not inhibited by bile salts (2, 7). In cases of pancreatic exocrine insufficiency, compensation for the loss of hepatic PL by GL has been previously noted as a common compensation mechanism that occurs naturally (7). Processing by gastric lipase in the stomach can also impact the integrity of oral drug delivery systems with premature drug release into the gastrointestinal environment and exposure of the drug to alteration from proteases (2, 13, 14) such that gastric digestion models (6, 13) have been developed to better understand potential impacts to oral pharmaceutical drug delivery systems (2, 13, 14). 

References

  1. Canaan, S. et. al. (1999) Biochim. Biophys. Acta 1441:197. 
  2. Koziolek, M. et. al. (2018) Pharm. Res. 35:55.
  3. Kumar, A. and S. Chauhan (2021) Life Sci. 271:119115. 
  4. Lim, S.Y. et. al. (2022) Am. J. Vet Res. 83:1.
  5. Bernback, S. et. al. (1989) Biochim. Biophys. Acta 1001:286. 
  6. Basque, J.R. and D. Menard (2000) Microsc. Res. Tech.  48:293
  7. Aloulou, A. and F. Carriere (2008) Cell Mol. Life Sci. 65:851.
  8. Liu, T.T. et. al. (2020) Biomed. Pharmacother. 128:110314.
  9. Chatzigeorgiou, A. et. al. (2014) Hepatology 60:1196.
  10. Higgins, V. et. al. (2020) J. Clin. Endocrinol. Metab. 105:1228.
  11. Lee, S.S. and S. Kang (2015) J. Phys. Ther. Sci. 27:1903.
  12. Lopez-Jimenez, F. et. al. (2022) Eur. J. Prev. Cardiol. 29:2218.
  13. Li, C. et. al. (2020) Trends Food Sci. Technol. 96:114.
  14. Zupancic, O. et. al. (2023) J. Control Release 362:381.

Long Name

Gastric triacylglycerol lipase

Alternate Names

GL, LIPF

Entrez Gene IDs

8513 (Human)

Gene Symbol

LIPF

UniProt

P07098.1

Additional Gastric Lipase Products

Product Documents for Recombinant Human Gastric Lipase/LIPF HA-tag His-tag, CF

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Product Specific Notices for Recombinant Human Gastric Lipase/LIPF HA-tag His-tag, CF

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