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    Home > Active Ingredient News > Endocrine System > Understanding "GLP-1 Receptor Agonists"

    Understanding "GLP-1 Receptor Agonists"

    • Last Update: 2023-01-06
    • Source: Internet
    • Author: User
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    Author: Wang Jianhua, chief physician of the Diabetes Diagnosis and Treatment Center of Jinan Hospital of Shandong Province

    This article is published with the author's permission, please do not reprint
    without permission.


    Clinical examples

     

    Sugar patient Li, male, 50 years old, height 172cm, weight 100kg, body mass index (BMI) 33.
    8kg/m^2
    .
    Treatment regimen: insulin glargine 26 U, iH, qn, metformin 1000 mg 2 times / day, acarbose 50 mg 3 times / day
    .
    Fasting blood glucose (FPG) 9.
    2mmol/L, postprandial blood glucose (PPG) 14.
    8mmol/L, glycated hemoglobin (HbA1c) 8.
    7%, poor glycemic control
    .
    After that, on the basis of the original treatment plan, add semeglutide, 0.
    5mg, iH, 1 time / week, according to the patient's tolerance, the dose is adjusted to 1mg, iH, 1 time / week after two weeks, and re-examination after 1 month, the patient's fasting and postprandial blood glucose are generally normal, glycated hemoglobin (HbA1c) 6.
    8%, and the weight is reduced by 8 kg
    compared with before the drug adjustment.

     

    GLP-1 receptor agonist (GLP-1RA) has become a remarkable and sought after hypoglycemic rookie
    in recent years with its excellent hypoglycemic and weight-reducing effects and cardiorenal protective effects.
    As a new drug, many sugar friends, even some grassroots doctors, generally lack understanding
    of the drug.
    Because these drugs are also injections, some patients often confuse them with insulin, and even some people with type 1 diabetes want to stop insulin and switch to a weekly preparation of GLP-1RA.

    Below, the author answers some representative questions frequently consulted by GLP-1RA patients
    .

     

    First, the life history of glucagon-like peptide-1 (GLP-1).

     

    As early as the 60s of the 20th century, foreign scholars found in the study of diabetes that the insulin secretion effect of oral glucose was significantly stronger than that of intravenous glucose, suggesting that there may be a substance in the intestine that can promote insulin secretion, and then found that this mysterious substance is a hypoglycemic hormone secreted by L cells in small intestinal epithelial cells (i.
    e.
    "incretin"), the main component of which is glucagon-like peptide-1 (GLP-1), The amount of insulin secretion it stimulates accounts for about 50%~70%
    of the total insulin secretion.

     

    Regarding the pathogenesis of type 2 diabetes, in addition to the well-known "insufficient insulin secretion" and "insulin resistance (IR)", it is currently believed that the decrease in intestinal GLP-1 production and the resulting weakening of incretin effect is also a very important cause
    .

     

    Because the GLP-1 secreted by its own physiology exists in the body for a short time, it will be degraded and inactivated by an enzyme (dipeptidyl peptidase) within a few minutes, so natural GLP-1 is not suitable for direct clinical treatment, but the discovery of GLP-1 provides a new idea
    for the treatment of type 2 diabetes.

     

    Second, how do GLP-1 receptor agonists lower glucose?

     

    After unremitting efforts, researchers finally developed a glucagon-like polypeptide-1 receptor agonist (GLP-1RA)
    for clinical use at the beginning of this century.
    As a new hypoglycemic drug, GLP-1RA is partially or completely homologous to the amino acid sequence of GLP-1 in vivo, and has the same biological activity, but it is not easily degraded by enzymes and the maintenance time is significantly prolonged, so it can better meet the needs
    of clinical treatment.

     

    GLP-1RA mainly exerts hypoglycemic effects
    by stimulating insulin secretion by pancreatic islet β cells, inhibiting islet α cells from secreting glucagon, suppressing appetite, and delaying gastric emptying.

     

    Happily, because the hypoglycemic effect of GLP-1RA is glucose-dependent, when the blood glucose concentration is lower than 4~5mmol/L, it no longer plays a role, therefore, the application alone generally does not cause hypoglycemia, in other words, it only reduces hyperglycemia but does not increase the risk of hypoglycemia, so it is known as "intelligent" hypoglycemic drugs
    .

     

    Fig.
    1 Mechanism of action and multiple efficacy of GLP-1RA

     

    What is the difference between GLP-1 receptor agonists and insulin? Can it replace insulin?

     

    First of all, the two sources are different, natural GLP-1 is secreted by intestinal L cells after food stimulation, while insulin is secreted by human islet β cells; Secondly, the mechanism of action of the two is not exactly the same, GLP-1RA can not only stimulate the islet β cells to secrete insulin, but also inhibit the secretion of glucagon by pancreatic α cells, in addition to other multiple benefits, such as blood pressure, lipid reduction, weight loss, cardiorenal protection, etc.
    ; The biggest advantage of insulin is that it has excellent hypoglycemic effect, and the disadvantage is that it can cause weight gain and the risk of hypoglycemia is relatively high; Third, because GLP-1RA mainly lowers glucose by stimulating insulin secretion, it is not suitable for diabetics with complete loss of islet function (such as type 1 diabetes), while insulin is suitable for all types of diabetic patients, including type 1 diabetes patients
    .

     

    It can be seen that although GLP-1 receptor agonists (GLP-1RA) and insulin are both injections, they belong to two completely different classes of hypoglycemic drugs
    .
    Whether GLP-1RA can replace insulin cannot be generalized, and needs to be treated
    on a case-by-case basis.
    For those patients with type 2 diabetes who still retain some islet function, GLP-1RA can be tried instead of insulin according to the specific situation; A combination of the two may also be considered while reducing the original amount of
    insulin.

     

    4.
    What are the outstanding advantages of GLP-1 receptor agonists?

     

    The biggest highlight of GLP-1 receptor agonist is "one specialized, multi-functional", in addition to hypoglycemia, it can also reduce weight (especially visceral fat), lower blood pressure, improve blood lipid disorders, reduce fatty liver, especially for the heart and kidneys has a protective effect, can significantly reduce the risk of cardiovascular events, delay the progression of diabetic nephropathy, improve the long-term prognosis
    of diabetic patients.

     

    Data show that GLP-1 receptor agonists can reduce glycated hemoglobin (HbA1c) by 1.
    0%~1.
    5%, reduce body weight by 3~5kg on average, and reduce systolic blood pressure by 2~6mmHg
    .

     

    5.
    What are the adverse reactions of GLP-1 receptor agonists?

     

    The main adverse reactions of GLP-1 receptor agonists are:

     

    1.
    Gastrointestinal reactions
    .
    It is relatively common, including loss of appetite, nausea, vomiting, bloating, abdominal pain, diarrhea, etc.
    , and is generally mild to moderate
    .

    2.
    GLP-1RA alone generally does not cause hypoglycemia, but if combined with insulin secretagogues or insulin, hypoglycemia
    may occur.

    3.
    Rare adverse reactions include pancreatitis, rash, etc
    .

     

    6.
    How to deal with gastrointestinal reactions caused by GLP-1 receptor agonists?

     

    GLP-1RA-induced gastrointestinal reactions are transient (usually disappear within 4 weeks) and usually lessen
    with prolonged treatment.
    At the same time, there are also dose-dependent characteristics, in order to reduce gastrointestinal reactions, small doses can be started, gradually increased, can enhance the patient's tolerance to the drug
    .

     

    7.
    Who are GLP-1 receptor agonists suitable for?

     

    It is suitable for adult patients with type 2 diabetes who are still poorly controlled with oral hypoglycemic agents alone or basal insulin
    injections.
    In view of its obvious weight loss effect and benefit the heart and kidneys, it is especially suitable for obese, combined with cardiovascular disease or chronic kidney disease type 2 diabetes patients, but also suitable for those who do not have cardiovascular disease but have cardiovascular risk factors, such as age ≥ 55 years old, hypertension, dyslipidemia, atherosclerosis (carotid artery, lower extremity artery, coronary artery, etc.
    ) and microalbuminuria
    .

     

    In addition, in view of the superior weight loss effect and good safety of GLP-1 receptor agonists, some of these products have been officially approved by the US FDA for weight management
    in obese or overweight adults.

     

    8.
    The use of GLP-1RA is contraindicated

     

    1.
    GLP-1RA mainly plays a hypoglycemic effect by promoting insulin secretion, and cannot replace insulin, so type 1 diabetes, patients with type 2 diabetes with severe islet failure, and diabetic ketoacidosis patients are banned;

    2.
    Those with a history or family history of medullary thyroid cancer (MTC), or multiple endocrine tumor syndrome type 2 (MEN2);

    3.
    Diabetic patients with acute and chronic pancreatitis;

    4.
    Those who are allergic to the active ingredients or any other excipients of such products are banned;

    5.
    Severe renal insufficiency (creatinine clearance <30ml/min) is banned;

    6
    .
    Due to the lack of relevant medication experience, it is currently not recommended for use in pregnancy, lactating women and people under 18 years old.


    9.
    Classification and use of GLP-1 receptor agonists

     

    According to the duration of the action, GLP-1RA can be divided into:


    1) Short-acting preparations: such as benaglutide (trade name: Yishengtai), exenatide (trade name: Baiyuda), etc.
    , focusing on reducing postprandial blood sugar;

    2) Medium-acting preparations: such as liraglutide (trade name: Novoliol), risnatide (trade name: Lexamine), etc.
    ;

    3) Long-acting preparations, that is, weekly "weekly preparations", including semeglutide (trade name: Novotec), dulaglutide (Duyida), exenatide microspheres (trade name: Patek Yang), which are effective for fasting and postprandial blood sugar, and reduce fasting blood sugar more obviously
    .

     

    GLP-1RA can be used alone or in combination with oral hypoglycemic agents (eg, biguanides, SGLT-2 inhibitors, α-glycosidase inhibitors, etc.
    ) or insulin
    .
    When GLP-1RA is used in combination with a sulfonylurea or basal insulin (e.
    g.
    , insulin detemir or glargine), the dose of sulfonylurea or insulin should be reduced as appropriate to reduce the risk of
    hypoglycemia.
    In addition, a compound preparation consisting of GLP-1RA and basal insulin (degusulin liraglutide injection, trade name "Novo Yi") has recently been launched
    in China.

     

    Examples are as follows:


    1) Benaglutide: short-acting preparation, specification 4.
    2mg/2.
    1ml/branch, 0.
    1~0.
    2mg each time, 3 times / day, subcutaneous injection 5 minutes before meals, mainly to reduce postprandial blood sugar, weight loss effect is better
    .

    2) Listatide: medium-acting preparation, specification 0.
    10mg/ml * 3ml/branch
    .
    Usage: 10~20μg, 1 time / day, subcutaneous injection
    1 hour before any meal.
    Once-daily administration is effective in controlling blood glucose
    after three meals.

    3) Liraglutide: medium-acting preparation, specification of 18mg/3ml, the alternative injection dose is 0.
    6mg/1.
    2mg/1.
    8mg, once a day, can be injected subcutaneously at any time, no need to administer according to the meal time, it is recommended to inject
    at the same time every day.
    The recommended starting dose is 0.
    6 mg, after one week, the dose can be increased to 1.
    2 mg, and the maximum daily dose does not exceed 1.
    8 mg
    .
    It can take into account both fasting and postprandial blood glucose
    .

    4) Dulaglutide: long-acting preparation, two specifications: 0.
    75 mg: 0.
    5 ml (pre-filled injection pen), 1.
    5 mg: 0.
    5 ml (pre-filled injection pen).

    Usage: 0.
    75~1.
    5mg, 1 time / week, subcutaneous injection at any time, can effectively control fasting and postprandial blood sugar
    .

    5) Semeglutide: long-acting preparation, 1.
    34mg/ml, 1.
    5ml/stick or 3ml/tube, injected once a
    week.
    The starting dose is 0.
    25 mg once weekly, after four weeks, it is increased to 0.
    5 mg once weekly, and after 4 weeks of treatment, the dose can be increased to 1 mg once weekly depending on patient tolerance to further improve glycaemic control
    .
    The drug can take into account both fasting and postprandial blood glucose, and the weight loss effect is the best
    among all GLP-1RAs currently.

    6) Degludec insulin liraglutide injection: is a mixture of long-acting basal insulin (degurutide) and GLP-1 receptor agonist (liraglutide), specification: 3ml/branch (300, 10.
    8mg), only once a day injection, can safely and smoothly control basal and postprandial blood glucose
    throughout the day.


    10.
    What drugs can GLP-1 receptor agonists be used in combination?


    GLP-1RA combined with other drugs can complement each other's strengths, complement each other's mechanisms, and help achieve high-quality and safe blood glucose standards, such as:

     

    1.
    GLP-1RA in combination with biguanides
    .
    Metformin can enhance the incretin effect of GLP-1RA, more safely and effectively control blood sugar, and the two have a synergistic effect on weight loss and insulin resistance, especially suitable for obese diabetics
    .
    When GLP-1RA is added to metformin therapy, the current dose of metformin can be maintained
    .

     

    2.
    GLP-1RA in combination with sulfonylureas
    .
    The two have a synergistic effect in promoting insulin release, and the weight loss effect of GLP-1RA can counteract sulfonylurea-induced weight gain, which is suitable for patients
    with type 2 diabetes who still have partial islet secretion function.
    Since GLP-1RA and sulfonylureas have insulin secretagogue effects, the dose of sulfonylureas should be reduced as appropriate when the two drugs are combined to reduce the risk of
    hypoglycemia.

     

    3.
    GLP-1RA in combination with basal insulin
    .
    The mechanism of action of the two drugs is complementary, the combination can optimize blood sugar control, effectively reduce basal blood sugar throughout the day and blood sugar after three meals, the risk of hypoglycemia is small, no increase can even reduce body weight, and can also reduce the amount of
    insulin.
    Therefore, in patients with type 2 diabetes mellitus who have poor glycaemic control with basal insulin, a combination with GLP-1RA may be considered
    .

     

    11.
    How to choose GLP-1RA for patients with liver and kidney dysfunction?

     

    The pharmacokinetic characteristics of various GLP-1RAs vary greatly, and their use in patients with renal insufficiency is also different
    .
    All kinds of GLP-1RA can be used in patients with mild and moderate renal insufficiency, severe renal insufficiency (glomerular filtration rate < 30ml/min), liraglutide and dulaglutide can be used with caution, and patients with end-stage renal disease are banned<b11>.
    Liraglutide can be used in patients with mild to moderate hepatic insufficiency, and the use of risnatide and dulaglutide is not limited
    by liver function.

     

    How to preserve GLP-1 receptor agonists

     

    Unopened GLP-1RA should be stored in the refrigerator (2~8 °C) and should not be frozen
    .
    The drug should not be used
    after freezing.
    After opening, it should be stored below 30 °C or refrigerated in the refrigerator (2~8 °C), and used up for
    1 month.
    Pay attention to protect from light to prevent repeated shaking
    .

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