SPINA-GBeta

SPINA-GBeta
SPINA-GBeta
Reference range	0.64–3.73 pmol/s
Calculator	https://doi.org/10.5281/zenodo.7479856
Purpose	Medical diagnosis, research
Test of	Pancreatic beta cell function

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SPINA-GBeta is a calculated biomarker for pancreatic beta cell function.^[1]^[a] It represents the maximum amount of insulin that beta cells can produce per time-unit (e.g. in one second).

How to determine G_Beta

The index is derived from a mathematical model of insulin-glucose homeostasis.^[2] For diagnostic purposes, it is calculated from fasting insulin and glucose concentrations with:

${\widehat {G}}_{\beta }={\frac {[I](\infty )({D}_{\beta }+\left[G\right](\infty ))}{{G}_{3}[G](\infty )}}$ .^[1]

[I](∞): Fasting Insulin plasma concentration (μU/mL)
[G](∞): Fasting blood glucose concentration (mg/dL)
D_β: EC₅₀ for glucose at beta cells (7 mmol/L)
G₃: Parameter for pharmacokinetics (58,8 s/L)

Clinical significance

Validity

SPINA-GBeta significantly correlates with the M value in glucose clamp studies and (better than HOMA-Beta) with the two-hour value in oral glucose tolerance testing (OGTT), glucose rise in OGTT, subscapular skinfold, truncal fat content and the HbA1c fraction.^[1]

It has the additional advantage that it circumvents the HOMA-blind zone, which renders the calculation of HOMA-Beta impossible if the fasting glucose concentration is 3.5 mmol/L (63 mg/dL) or below.^[3] Unlike HOMA-Beta, SPINA-Beta can be sensibly calculated in the whole range of measurements.^[1]

Reliability

In repeated measurements, SPINA-GBeta had higher retest reliability than HOMA-Beta, a measurement for beta cell function from the homeostasis model assessment.^[1]^[4]

Clinical utility

In the FAST study, an observational case-control sequencing study including 300 persons from Germany, SPINA-GBeta differed more clearly between subjects with and without diabetes than the corresponding HOMA-Beta index.^[4]

Scientific implications and other uses

Together with the reconstructed insulin receptor gain (SPINA-GR), SPINA-GBeta provides the foundation for the definition of a fasting based disposition index of insulin-glucose homeostasis (SPINA-DI).^[4]

In combination with SPINA-GR and whole-exome sequencing, calculating SPINA-GBeta helped to identify a new form of monogenetic diabetes (MODY) that is characterised by primary insulin resistance and results from a missense variant of the type 2 ryanodine receptor (RyR2) gene (p.N2291D).^[5]

Pathophysiological implications

In several populations, SPINA-GBeta correlated with the area under the glucose curve and 2-hour concentrations of glucose, insulin and proinsulin in oral glucose tolerance testing, concentrations of free fatty acids, ghrelin and adiponectin, and the HbA1c fraction.^[4]

Notes

^ SPINA is an acronym for "structure parameter inference approach".

References

^ ^a ^b ^c ^d ^e Dietrich, JW; Dasgupta, R; Anoop, S; Jebasingh, F; Kurian, ME; Inbakumari, M; Boehm, BO; Thomas, N (21 October 2022). "SPINA Carb: a simple mathematical model supporting fast in-vivo estimation of insulin sensitivity and beta cell function". Scientific Reports. 12 (1): 17659. Bibcode:2022NatSR..1217659D. doi:10.1038/s41598-022-22531-3. PMC 9587026. PMID 36271244.
^ Dietrich, Johannes W.; Böhm, Bernhard (27 August 2015). "Die MiMe-NoCoDI-Plattform: Ein Ansatz für die Modellierung biologischer Regelkreise". GMDS 2015; 60. Jahrestagung der Deutschen Gesellschaft für Medizinische Informatik: Biometrie und Epidemiologie e.V. (GMDS). doi:10.3205/15gmds058.
^ Cersosimo, E; Solis-Herrera, C; Trautmann, ME; Malloy, J; Triplitt, CL (January 2014). "Assessment of pancreatic β-cell function: review of methods and clinical applications". Current Diabetes Reviews. 10 (1): 2–42. doi:10.2174/1573399810666140214093600. PMC 3982570. PMID 24524730.
^ ^a ^b ^c ^d Dietrich, Johannes W.; Abood, Assjana; Dasgupta, Riddhi; Anoop, Shajith; Jebasingh, Felix K.; Spurgeon, R.; Thomas, Nihal; Boehm, Bernhard O. (2 January 2024). "A novel simple disposition index ( SPINA-DI ) from fasting insulin and glucose concentration as a robust measure of carbohydrate homeostasis". Journal of Diabetes. doi:10.1111/1753-0407.13525. PMID 38169110. S2CID 266752689.
^ Bansal, Vikas; Winkelmann, Bernhard R.; Dietrich, Johannes W.; Boehm, Bernhard O. (20 February 2024). "Whole-exome sequencing in familial type 2 diabetes identifies an atypical missense variant in the RyR2 gene". Frontiers in Endocrinology. 15. doi:10.3389/fendo.2024.1258982. PMC 10913019. PMID 38444585.

External links

Functions for R and S for calculating SPINA-GBeta and SPINA-GR. (Permanent DOI)

[2] SPINA is an acronym for "structure parameter inference approach".

[Dietrich_et_al_2022-1] Dietrich, JW; Dasgupta, R; Anoop, S; Jebasingh, F; Kurian, ME; Inbakumari, M; Boehm, BO; Thomas, N (21 October 2022). "SPINA Carb: a simple mathematical model supporting fast in-vivo estimation of insulin sensitivity and beta cell function". Scientific Reports. 12 (1): 17659. Bibcode:2022NatSR..1217659D. doi:10.1038/s41598-022-22531-3. PMC 9587026. PMID 36271244.

[3] Dietrich, Johannes W.; Böhm, Bernhard (27 August 2015). "Die MiMe-NoCoDI-Plattform: Ein Ansatz für die Modellierung biologischer Regelkreise". GMDS 2015; 60. Jahrestagung der Deutschen Gesellschaft für Medizinische Informatik: Biometrie und Epidemiologie e.V. (GMDS). doi:10.3205/15gmds058.

[4] Cersosimo, E; Solis-Herrera, C; Trautmann, ME; Malloy, J; Triplitt, CL (January 2014). "Assessment of pancreatic β-cell function: review of methods and clinical applications". Current Diabetes Reviews. 10 (1): 2–42. doi:10.2174/1573399810666140214093600. PMC 3982570. PMID 24524730.

[Dietrich_JDiab_2024-5] Dietrich, Johannes W.; Abood, Assjana; Dasgupta, Riddhi; Anoop, Shajith; Jebasingh, Felix K.; Spurgeon, R.; Thomas, Nihal; Boehm, Bernhard O. (2 January 2024). "A novel simple disposition index ( SPINA-DI ) from fasting insulin and glucose concentration as a robust measure of carbohydrate homeostasis". Journal of Diabetes. doi:10.1111/1753-0407.13525. PMID 38169110. S2CID 266752689.

[Bansal_2024-6] Bansal, Vikas; Winkelmann, Bernhard R.; Dietrich, Johannes W.; Boehm, Bernhard O. (20 February 2024). "Whole-exome sequencing in familial type 2 diabetes identifies an atypical missense variant in the RyR2 gene". Frontiers in Endocrinology. 15. doi:10.3389/fendo.2024.1258982. PMC 10913019. PMID 38444585.

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v t e Diabetes
Types	Type 1 (SAID cluster) Type 1 diabetes (LADA cluster) Type 2 (SIDD, SIRD, MOD and MARD clusters) Type 4 (Gestational diabetes) Diabetes and pregnancy Prediabetes Impaired fasting glucose Impaired glucose tolerance Insulin resistance Ketosis-prone diabetes (KPD) Type 3a (MODY) Type 1 2 3 4 5 6 Neonatal Transient Permanent Type 3c (pancreatogenic) Type 3 MIDD
Blood tests	Blood sugar level Biomarkers Glycated hemoglobin Glucose tolerance test Postprandial glucose test Fructosamine Glucose test C-peptide Noninvasive glucose monitor Insulin tolerance test Metabolic Score for Insulin Resistance (METS-IR) Homeostatic model assessment SPINA-GBeta SPINA-GR Disposition index
Management	Prevention Metabolic assessment and monitoring Blood glucose monitoring Ambulatory glucose profile Diet in diabetes Diabetes medication Insulin therapy intensive conventional pulsatile Diabetic shoes Cure Embryonic stem cells Artificial pancreas Other Gastric bypass surgery
Complications	Diabetic comas Hypoglycemia Ketoacidosis Hyperosmolar hyperglycemic state Diabetic foot ulcer Neuropathic arthropathy Organs in diabetes Blood vessels Muscle Kidney Nerves Retina Heart Diabetes-related skin disease Diabetic dermopathy Diabetic bulla Diabetic cheiroarthropathy Diabetic foot ulcer Hyperglycemia Hypoglycemia
Advocacy & Organizations	T1International Open Insulin Project JDRF International Diabetes Federation World Diabetes Day Diabetes UK
Other	Outline of diabetes Glossary of diabetes Epidemiology of diabetes History of diabetes Notable people with type 1 diabetes

How to determine GBeta