What is the value of faster acting prandial insulin? Focus on ultra rapid lispro

Heise, Tim; Oliveira, Carolina Piras de; Juneja, Rattan; Ribeiro, Anderson Orzari; Chigutsa, Farai; Blevins, Thomas

doi:10.1111/dom.14773

Cited by 22 publications

(15 citation statements)

References 44 publications

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…One might argue that accelerating absorption via an IVM is an unnecessary redundancy now that ultra-rapid acting insulins are available. However, the very rapid peak plasma insulin concentrations achieved with regular insulin via IVM more closely mimic the normal human pancreas and are likely superior to even ultra-rapid acting insulins injected SC [16, 49, 50]. The insulin kinetic curves (Fig 2 B, D) are compatible with an “inject-eat continuum” strategy: this would, first, synchronize the insulin peak with the prandial requirement; and second, avoid the pitfalls of inopportune delays of a meal by simply postponing the injection.…”

Section: Discussionmentioning

confidence: 99%

“…Another argument sometimes made is that rapid uptake of insulin confers more risk than benefit, for example, by triggering hypoglycemic episodes. However, the clinical safety and efficacy, especially in post-prandial control, of ultra-rapid acting insulins is now supported by many studies [15, 16, 52, 53]. The factitious “too rapid” assertion also deflects the many advances in continuous glucose monitoring (CGM) devices, insulin dosage-predicting algorithms, precision-dosing insulin pumps, open and closed loop systems, and the “artificial pancreas” (AP) [6].…”

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

Accelerated absorption of regular insulin administered via a vascularizing permeable microchamber implanted subcutaneously in diabeticRattus norvegicus

Steyn

Drew

Vlachos

et al. 2022

Preprint

View full text Add to dashboard Cite

In Type 1 diabetes patients, even ultra-rapid acting insulins injected subcutaneously reach peak concentrations in 45 minutes or longer. The lag time between dosing and peak concentration, as well as intra- and inter-subject variability, render prandial glucose control and dose consistency difficult. We postulated that insulin absorption from subcutaneously implantable vascularizing microchambers would be significantly faster than conventional subcutaneous injection. Male athymic nude R. norvegicus rendered diabetic with streptozotocin were implanted with vascularizing microchambers (single chamber; 1.5 cm2 surface area per side; nominal volume, 22.5 µL). Plasma insulin was assayed after a single dose (1.5 U/kg) of diluted insulin human (Humulin®R U-100), injected subcutaneously or via microchamber. Microchambers were also implanted in additional animals and retrieved at intervals for histologic assessment of vascularity. Following conventional subcutaneous injection, the mean peak insulin concentration was 22.7 (SD 14.2) minutes. By contrast, when identical doses of insulin were injected via subcutaneous microchamber 28 days after implantation, the mean peak insulin time was shortened to 7.50 (SD 4.52) minutes. Peak insulin concentrations were similar by either route; however, inter-subject variability was reduced when insulin was administered via microchamber. Histologic examination of tissue surrounding microchambers showed mature vascularization on days 21 and 40 post-implantation. Implantable vascularizing microchambers of similar design may prove clinically useful for insulin dosing, either intermittently by needle, or continuously by pump including in “closed loop” systems, such as the artificial pancreas.

show abstract

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Accelerated absorption of regular insulin administered via a vascularizing permeable microchamber implanted subcutaneously in diabeticRattus norvegicus

Steyn

Drew

Vlachos

et al. 2022

Preprint

View full text Add to dashboard Cite

show abstract

“…Wegen des schnelleren Wirkungseintritts ist es noch besser steuerbar, insbesondere bei Menschen mit Typ-1-Diabetes und solchen mit einer Insulinpumpentherapie [294]. Die Insulinwirkung von ultraschnell wirkendem Insulin lispro (URLI = Ultra Rapid Lispro Insulin) führte zu einer deutlich besseren postprandialen Glukosekontrolle, ganz gleich ob dieses Insulin vor, während oder nach der Mahlzeit (-15 bis + 15 Minuten) s. c. gespritzt wurde [296]. Die postprandialen Glukose-Exkursionen über 5 Stunden wurden mit URLI um 29 % bis 105 % gesenkt.…”

Section: Schnellwirkende Insulin-analogaunclassified

Therapie des Typ-2-Diabetes

Landgraf

Aberle

Birkenfeld

et al. 2022

Diabetologie und Stoffwechsel

View full text Add to dashboard Cite

Dieses Dokument wurde zum persönlichen Gebrauch heruntergeladen. Vervielfältigung nur mit Zustimmung des Verlages. ▶ Abb. 3 Algorithmus zur Insulintherapie. Quelle: Nationale VersorgungsLeitlinien. NVL-2-Diabetes -Teilpublikation, 2. Auflage: www.leitlinien. de/themen/diabetes. [rerif]. Diese Abbildung dient als Ergänzung zu Abb. 2. Der Algorithmus bezieht sich nicht auf Menschen mit schwerer Stoffwechseldekompensation bzw. Notfallsituationen. Aktuelle Fachinformationen sind zu berücksichtigen. Überprüfung der Therapiestrategie und des Therapieziels in spätestens 3-6 Monaten.

show abstract

“…Ultra rapid lispro (URLi; Lyumjev ® ) is a formulation of insulin lispro with a faster onset and shorter duration of action compared to Lispro (Humalog ® ) and was developed to more closely match physiological insulin secretion and improve PPG control [ 12 ]. URLi has demonstrated non-inferiority to Lispro in HbA1c change from baseline after 26 weeks in people with type 1 diabetes (T1D) (PRONTO-T1D) and T2D (PRONTO-T2D) while providing superior PPG control when dosed at mealtime [ 13 , 14 ].…”

Section: Introductionmentioning

confidence: 99%

“…Studies have shown that introducing a rapid-acting prandial insulin as part of a basal-bolus multiple daily injection (MDI) regimen is more effective at managing PPG than a basal-only regimen [9][10][11]. Nevertheless, rapid-acting insulins still may not have fast enough onset to match carbohydrate absorption resulting in inadequate control of PPG [12].…”

Section: Introductionmentioning

confidence: 99%

Increased Time in Range with Ultra Rapid Lispro Treatment in Participants with Type 2 Diabetes: PRONTO-Time in Range

et al. 2023

View full text Add to dashboard Cite

Introduction To evaluate time in range metrics and HbA1c in people with type 2 diabetes (T2D) treated with ultra rapid lispro (URLi) using continuous glucose monitoring (CGM) for the first time in this population. Methods This was a Phase 3b, 12-week, single-treatment study in adults with T2D on basal-bolus multiple daily injection (MDI) therapy using basal insulin glargine U-100 along with a rapid-acting insulin analog. Following a 4-week baseline period, 176 participants were newly treated with prandial URLi. Participants used unblinded CGM (Freestyle Libre). Primary endpoint was time in range (TIR) (70–180 mg/dl) during the daytime period at Week 12 compared to baseline with gated secondary endpoints of HbA1c change from baseline and 24-h TIR (70–180 mg/dl). Results Improved glycemic control was observed at Week 12 versus baseline including mean daytime TIR (change from baseline [Δ] 3.8%; P = 0.007), HbA1c (Δ − 0.44%; P < 0.001), and 24-h TIR (Δ 3.3%; P = 0.016) with no significant difference in time below range (TBR). After 12 weeks, there was a statistically significant decrease in postprandial glucose incremental area under curve, overall, across all meals, within 1 h ( P = 0.005) or 2 h ( P < 0.001) after the start of a meal. Basal, bolus, and total insulin dose were intensified with increased bolus/total dose ratio at Week 12 (50.7%) versus baseline (44.5%; P < 0.001). There were no severe hypoglycemia events during the treatment period. Conclusions In people with T2D, URLi in an MDI regimen was efficacious with improved glycemic control including TIR, HbA1c, and postprandial glucose without increased hypoglycemia/TBR. Clinical Trial registration number NCT04605991. Supplementary Information The online version contains supplementary material available at 10.1007/s13300-023-01400-w.

show abstract

What is the value of faster acting prandial insulin? Focus on ultra rapid lispro

Cited by 22 publications

References 44 publications

Accelerated absorption of regular insulin administered via a vascularizing permeable microchamber implanted subcutaneously in diabeticRattus norvegicus

Accelerated absorption of regular insulin administered via a vascularizing permeable microchamber implanted subcutaneously in diabeticRattus norvegicus

Therapie des Typ-2-Diabetes

Increased Time in Range with Ultra Rapid Lispro Treatment in Participants with Type 2 Diabetes: PRONTO-Time in Range

Contact Info

Product

Resources

About