FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2028080517> ?p ?o ?g. }

• W2028080517 endingPage "181" @default.
• W2028080517 startingPage "172" @default.
• W2028080517 abstract "The growth hormone (GH)-insulin-like growth factor (IGF) axis and insulin are major anabolic effectors in promoting weight gain and linear growth. These two anabolic systems are interlinked at many levels, thus abnormalities in one of these systems effect the other causing disordered metabolic homeostasis. Insufficient portal insulinization in insulin dependent diabetes mellitus (IDDM) results in hepatic GH resistance and increased production of IGF-binding proteins-1 (IGFBP-1) and IGFBP-2. GH resistance is reflected by decreased hepatic IGF-I production. In addition, changes in other GH-dependent proteins are also observed in IDDM. Increased proteolysis of IGFBP-3 results in reduction of intact IGFBP-3. Serum ALS levels are also slightly diminished in untreated diabetic patients. Hepatic resistance to GH is, at least in part, caused by diminished GH receptors as reflected by diminished circulating GHBP levels. In addition, there is also evidence from experimental and human studies suggesting post-receptor defect(s) in GH action. As a result of these changes, circulating total and free IGF-I levels are decreased during insulinopenia. Lack of negative feed-back effect of IGF-I on GH secretion causes GH hypersecretion which increases hyperglycemia by decreasing sensitivity to insulin. GH hypersecretion in poorly controlled diabetic patients may play a role in the pathogenesis of diabetic vascular complications. Most of these abnormalities in the GH-IGF axis in diabetes are reversed by effective insulinization of the patient. Addition of IGF-I treatment to insulin in adolescents with IDDM allows correction of GH hypersecretion, improves insulin sensitivity and glycemic control, and decreases insulin requirements. The effect of IGF-I treatment on diabetic complications has yet to be seen." @default.
• W2028080517 created "2016-06-24" @default.
• W2028080517 creator A5055397658 @default.
• W2028080517 creator A5063065558 @default.
• W2028080517 creator A5073807348 @default.
• W2028080517 date "1999-01-01" @default.
• W2028080517 modified "2023-10-13" @default.
• W2028080517 title "Alterations in the Growth Hormone-Insulin-Like Growth Factor Axis in Insulin Dependent Diabetes Mellitus" @default.
• W2028080517 doi "https://doi.org/10.1055/s-2007-978716" @default.
• W2028080517 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/10226799" @default.
• W2028080517 hasPublicationYear "1999" @default.
• W2028080517 type Work @default.
• W2028080517 sameAs 2028080517 @default.
• W2028080517 citedByCount "143" @default.
• W2028080517 countsByYear W20280805172012 @default.
• W2028080517 countsByYear W20280805172013 @default.
• W2028080517 countsByYear W20280805172014 @default.
• W2028080517 countsByYear W20280805172015 @default.
• W2028080517 countsByYear W20280805172016 @default.
• W2028080517 countsByYear W20280805172017 @default.
• W2028080517 countsByYear W20280805172018 @default.
• W2028080517 countsByYear W20280805172019 @default.
• W2028080517 countsByYear W20280805172020 @default.
• W2028080517 countsByYear W20280805172021 @default.
• W2028080517 countsByYear W20280805172022 @default.
• W2028080517 crossrefType "journal-article" @default.
• W2028080517 hasAuthorship W2028080517A5055397658 @default.
• W2028080517 hasAuthorship W2028080517A5063065558 @default.
• W2028080517 hasAuthorship W2028080517A5073807348 @default.
• W2028080517 hasConcept C1008401 @default.
• W2028080517 hasConcept C126322002 @default.
• W2028080517 hasConcept C134018914 @default.
• W2028080517 hasConcept C170493617 @default.
• W2028080517 hasConcept C2775960820 @default.
• W2028080517 hasConcept C2777391703 @default.
• W2028080517 hasConcept C2779306644 @default.
• W2028080517 hasConcept C2780689927 @default.
• W2028080517 hasConcept C2780942790 @default.
• W2028080517 hasConcept C555293320 @default.
• W2028080517 hasConcept C71924100 @default.
• W2028080517 hasConceptScore W2028080517C1008401 @default.
• W2028080517 hasConceptScore W2028080517C126322002 @default.
• W2028080517 hasConceptScore W2028080517C134018914 @default.
• W2028080517 hasConceptScore W2028080517C170493617 @default.
• W2028080517 hasConceptScore W2028080517C2775960820 @default.
• W2028080517 hasConceptScore W2028080517C2777391703 @default.
• W2028080517 hasConceptScore W2028080517C2779306644 @default.
• W2028080517 hasConceptScore W2028080517C2780689927 @default.
• W2028080517 hasConceptScore W2028080517C2780942790 @default.
• W2028080517 hasConceptScore W2028080517C555293320 @default.
• W2028080517 hasConceptScore W2028080517C71924100 @default.
• W2028080517 hasIssue "02/03" @default.
• W2028080517 hasLocation W20280805171 @default.
• W2028080517 hasLocation W20280805172 @default.
• W2028080517 hasOpenAccess W2028080517 @default.
• W2028080517 hasPrimaryLocation W20280805171 @default.
• W2028080517 hasRelatedWork W2014231481 @default.
• W2028080517 hasRelatedWork W2058160713 @default.
• W2028080517 hasRelatedWork W2094821865 @default.
• W2028080517 hasRelatedWork W2101723988 @default.
• W2028080517 hasRelatedWork W2121592873 @default.
• W2028080517 hasRelatedWork W2130733926 @default.
• W2028080517 hasRelatedWork W2132766762 @default.
• W2028080517 hasRelatedWork W2590769241 @default.
• W2028080517 hasRelatedWork W2800670286 @default.
• W2028080517 hasRelatedWork W2189320406 @default.
• W2028080517 hasVolume "31" @default.
• W2028080517 isParatext "false" @default.
• W2028080517 isRetracted "false" @default.
• W2028080517 magId "2028080517" @default.
• W2028080517 workType "article" @default.