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Management of Blood Glucose with non-Insulin therapies in DM type 2

Jorge De Jesus MD FACE

april 23, 2016

Disclosures

• Dr Jorge De Jesús has received honorariums as speaker for the following pharmaceutical companies: Merck; Janssen; Sanofi -Aventis

• Dr Jorge De Jesús has no conflicts of interests with any entity for the information included in this presentation

Jorge De Jesús MD FACE

ObjectivesDuring this 30 minutes presentation the audience will be able to :

• Recognize that DM 2 is a multifactorial disease

• DM is a progressive disease and eventually many patients will need insulin in their therapies

• Oral therapies included in the presentation:

• Metformin; DPP4 inhibitors; SGLT2 inhibitors

• Parenteral, non insulin therapies: GLP-1 RA

• Some non FDA approved therapies will be discussed

The organizers of the activity have been authorized to distribute handouts of this

presentation

Pre- Test

• Treatment of Diabetes Mellitus should be centered in the patient and individualized.

• Due to the multifactorial nature of the disease combination therapy is needed early in the treatment of this condition

• Efforts should me made to prevent DM in high risk individuals.

The Ominous Octet

Islet b-cell

ImpairedInsulin Secretion

Neurotransmitter

Dysfunction

Decreased Glucose

Uptake

Islet a-cell

Increased

Glucagon Secretion

IncreasedLipolysis

Increased Glucose

Reabsorption

Increased

HGP

DecreasedIncretin Effect

Diabetes type 2 is a polygenic and multifactorial disease

3A=45-59; 3B=30-44

contraindicated GFR< 30 ml/min

SGLT1

(180 L/day) (900 mg/L)=162 g/day

10%

Glucose

No Glucose

S1

S3

Renal Handling of Glucose

SGLT2

90%

Rationale for SGLT2 Inhibitors

• Inhibit glucose reabsorption in the renal proximal tubule

• Resultant glucosuria leads to a decline in plasma glucose and reversal of glucotoxicity

• This therapy is simple and nonspecific

• Even patients with refractory type 2 diabetes are likely to respond

SGLT2 and DKA

Class effect??

Many patients with type 2 diabetes continue to have poor control and would benefit from insulin therapy . However, resistance to the introduction of insulin therapy can be high on both the part of the healthcare provider and the patient . A number of new, long acting basal insulins are in development that provide good metabolic control , with lower a risk of hypoglycemia , than the currently available insulins.Providing greater flexibility in dosing time from day to day.

These attributes may address some of the current barriers to insulin initiation and intensification that currently limit the effectiveness of diabetes care.

New Long acting basal Insulins

The Ominous Octet

Islet b-cell

ImpairedInsulin Secretion

Neurotransmitt

er

Dysfunction

Decreased

Glucose

Uptake

Islet a-cell

Increased

Glucagon

Secretion

IncreasedLipolysis

Increased

Glucose

Reabsorption

Increased

HGP

DecreasedIncretin Effect

Diabetes type 2 is a polygenic and multifactorial disease

Glp-1 receptor agonists

Short acting

• Exenatide ( twice a day)

• Liraglutide ( once daily)

• Lixisenatide* (once daily)

Long acting ( one a week)

• Exenatide QW (Bydureon)

• Albiglutide (Tanzeum)

• Dilaglutide (Trulicity)

• *Semaglutide

• *ITCA 650 pump ( exenatidecontinuous)

*not yet approved by FDA

Degludec and liraglutide

Lixenatide GLP-1 RA

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