Translations:Insulin (medication)/28/ja: Difference between revisions

Slight variations of the human insulin molecule are called [[insulin analog]]ues, (technically "insulin receptor [[ligand]]s") so named because they are not technically insulin, rather they are analogues which retain the hormone's glucose management functionality. They have absorption and activity characteristics not currently possible with subcutaneously injected insulin proper. They are either absorbed rapidly in an attempt to mimic real beta cell insulin (as with [[insulin lispro]], [[insulin aspart]], and [[insulin glulisine]]), or steadily absorbed after injection instead of having a 'peak' followed by a more or less rapid decline in insulin action (as with [[insulin detemir]] and [[insulin glargine]]), all while retaining insulin's glucose-lowering action in the human body. However, a number of [[meta-analysis|meta-analyses]], including those done by the [[Cochrane Collaboration]] in 2005, Germany's Institute for Quality and Cost Effectiveness in the Health Care Sector [IQWiG] released in 2007, and the Canadian Agency for Drugs and Technology in Health (CADTH) also released in 2007 have shown no unequivocal advantages in clinical use of insulin analogues over more conventional insulin types.