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  • Ribbing, JakobUppsala universitet,Institutionen för farmaceutisk biovetenskap (author)

A model for glucose, insulin, and beta-cell dynamics in subjects with insulin resistance and patients with type 2 diabetes.

  • Article/chapterEnglish2010

Publisher, publication year, extent ...

  • 2013-03-07
  • Wiley,2010
  • electronicrdacarrier

Numbers

  • LIBRIS-ID:oai:gup.ub.gu.se/135393
  • https://gup.ub.gu.se/publication/135393URI
  • https://doi.org/10.1177/0091270009349711DOI
  • https://urn.kb.se/resolve?urn=urn:nbn:se:uu:diva-95985URI

Supplementary language notes

  • Language:English

Part of subdatabase

Classification

  • Subject category:ref swepub-contenttype
  • Subject category:art swepub-publicationtype

Notes

  • Type 2 diabetes mellitus (T2DM) is a progressive, metabolic disorder characterized by reduced insulin sensitivity and loss of beta-cell mass (BCM), resulting in hyperglycemia. Population pharmacokinetic-pharmacodynamic (PKPD) modeling is a valuable method to gain insight into disease and drug action. A semi-mechanistic PKPD model incorporating fasting plasma glucose (FPG), fasting insulin, insulin sensitivity, and BCM in patients at various disease stages was developed. Data from 3 clinical trials (phase II/III) with a peroxisome proliferator-activated receptor agonist, tesaglitazar, were used to develop the model. In this, a modeling framework proposed by Topp et al was expanded to incorporate the effects of treatment and impact of disease, as well as variability between subjects. The model accurately described FPG and fasting insulin data over time. The model included a strong relation between insulin clearance and insulin sensitivity, predicted 40% to 60% lower BCM in T2DM patients, and realistic improvements of BCM and insulin sensitivity with treatment. The treatment response on insulin sensitivity occurs within the first weeks, whereas the positive effects on BCM arise over several months. The semi-mechanistic PKPD model well described the heterogeneous populations, ranging from nondiabetic, insulin-resistant subjects to long-term treated T2DM patients. This model also allows incorporation of clinical-experimental studies and actual observations of BCM.

Subject headings and genre

  • Alkanesulfonates
  • pharmacology
  • Blood Glucose
  • metabolism
  • Clinical Trials
  • Phase II as Topic
  • Clinical Trials
  • Phase III as Topic
  • Diabetes Mellitus
  • Type 2
  • physiopathology
  • Fasting
  • blood
  • Humans
  • Hypoglycemic Agents
  • pharmacology
  • Insulin
  • metabolism
  • Insulin Resistance
  • physiology
  • Insulin-Secreting Cells
  • drug effects
  • metabolism
  • Models
  • Biological
  • Peroxisome Proliferator-Activated Receptors
  • agonists
  • Phenylpropionates
  • pharmacology
  • Predictive Value of Tests
  • Time Factors
  • type-2 diabetes
  • PHARMACY

Added entries (persons, corporate bodies, meetings, titles ...)

  • Hamrén, BengtUppsala universitet,Institutionen för farmaceutisk biovetenskap (author)
  • Svensson, M.K,1965Gothenburg University,Göteborgs universitet,Institutionen för medicin, avdelningen för molekylär och klinisk medicin,Institute of Medicine, Department of Molecular and Clinical Medicine(Swepub:gu)xsmara (author)
  • Karlsson, Mats O.Uppsala universitet,Institutionen för farmaceutisk biovetenskap(Swepub:uu)matskarl (author)
  • Uppsala universitetInstitutionen för farmaceutisk biovetenskap (creator_code:org_t)

Related titles

  • In:Journal of clinical pharmacology: Wiley50:8, s. 861-721552-46040091-2700

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