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DEL'TALICIN

Ask a doctor about a prescription for DEL'TALICIN

5.0(96)
Doctor

Alina Tsurkan

Family medicine12 years of experience

Dr. Alina Tsurkan is a licensed family medicine physician based in Portugal, offering online consultations for adults and children. She provides professional primary care, with a focus on prevention, accurate diagnosis, and long-term management of acute and chronic conditions.

Dr. Tsurkan supports patients with a wide range of health issues, including:

  • Respiratory infections: cold, flu, bronchitis, pneumonia, and lingering coughs.
  • ENT conditions: sinusitis, tonsillitis, otitis (ear infections), sore throat, allergic rhinitis.
  • Eye conditions: allergic or infectious conjunctivitis, red eyes, irritation.
  • Digestive issues: acid reflux (GERD), gastritis, irritable bowel syndrome (IBS), constipation, bloating, nausea.
  • Urinary and reproductive health: urinary tract infections (UTIs), cystitis, prevention of recurrent infections.
  • Chronic diseases: hypertension, elevated cholesterol, weight management.
  • Neurological complaints: headaches, migraines, sleep disturbances, fatigue, general weakness.
  • Children’s health: fever, infections, digestive issues, follow-ups, vaccination guidance.

She also provides:

  • IMT medical certificates for driving licence exchange in Portugal.
  • Personalised preventive care and wellness consultations.
  • Interpretation of test results and medical reports.
  • Follow-up care and medication review.
  • Support in managing multiple coexisting conditions.
  • Remote prescription management and medical documentation.

Dr. Tsurkan’s approach is evidence-based and holistic. She works closely with each patient to develop an individualised care plan that addresses both symptoms and root causes. Her goal is to empower patients to take control of their health and maintain well-being through lifestyle adjustments, routine check-ups, and early intervention.

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This page is for general information. Consult a doctor for personal advice. Call emergency services if symptoms are severe.
About the medicine

How to use DEL'TALICIN

INSTRUCTIONS FOR MEDICAL USE OF THE MEDICINAL PRODUCT PENTASA (PENTASA®)

Composition

active substance: mesalazine; 1 tablet contains mesalazine 500 mg; excipients: povidone, ethylcellulose, magnesium stearate, talc, microcrystalline cellulose.

Pharmaceutical Form

Prolonged-release tablets.

Main Physical and Chemical Properties

Round tablets with inclusions from white-gray to pale brown in color. With a notch, a line, and an imprint of "500" and "mg" on both sides of the line on one side of the tablet, and "PENTASA" on the other side of the tablet. Diameter: 13.5 mm.

Pharmacotherapeutic Group

Anti-inflammatory agents used in diseases of the intestine. Aminosalicylic acid and similar agents.

ATC Code A07E C02.

Pharmacological Properties

Pharmacodynamics

Mesalazine is the active component of sulfasalazine, which is used to treat ulcerative colitis and Crohn's disease.

Clinical studies indicate that the therapeutic properties of mesalazine when taken orally and rectally are due to its local action on the inflamed areas of the intestine, rather than a systemic effect. Available information suggests that the severity of intestinal inflammation in patients with ulcerative colitis is inversely correlated with the concentration of mesalazine in the mucous membrane.

In patients with inflammatory bowel diseases, increased migration of leukocytes, abnormal production of cytokines, increased production of arachidonic acid metabolites (especially leukotriene B4), and increased concentration of free radicals in the inflamed tissues of the intestine are observed.

The mechanism of action of mesalazine is not fully understood, although it may involve mechanisms such as stimulation of the gamma form of peroxisome proliferator-activated receptors (PPAR-γ) and inhibition of nuclear factor kappa-B (NF-κB) in the intestinal mucosa.

The pharmacological effect of mesalazine in in vitro and in vivo studies is the suppression of leukocyte chemotaxis, reduction of cytokine and leukotriene production, and neutralization of free radicals. Although this is not definitively established, the above processes are likely to play a key role in the clinical efficacy of mesalazine.

The risk of developing colorectal cancer is slightly increased in patients with ulcerative colitis. A comparative analysis of 9 non-experimental studies (3 group studies and 6 case-control studies) of 334 cases of colorectal cancer and 140 cases of dysplasia in 1932 patients with ulcerative colitis showed that in patients treated with mesalazine, the risk of developing colorectal cancer decreased by 50%, and also showed a combined clinical outcome for colorectal cancer and dysplasia. The reduction in the risk of developing colorectal cancer depends on the dosage, as evidenced by a comparative analysis of studies of daily dosage records, according to which mesalazine has a chemopreventive effect at a dose of ≥ 1.2 g/day. Additionally, chemoprevention is associated with the lifetime dose of mesalazine. It has been found that maintenance treatment with mesalazine reduces the risk of developing colorectal cancer.

The action of mesalazine, as revealed by experimental models and patient biopsies, confirms the role of the drug in preventing colorectal cancer caused by ulcerative colitis, as well as reducing the number of signaling pathways associated with and not associated with the inflammatory process involved in the development of colorectal cancer caused by colitis. However, the data from the meta-analysis, which included reference and general populations, provided ambiguous clinical information regarding the benefits of mesalazine in reducing the risk of carcinogenesis associated with ulcerative colitis.

Pharmacokinetics

The therapeutic effect of mesalazine is primarily determined by its local contact with the inflamed area of the intestinal mucosa.

Pentasa, prolonged-release tablets, is a microgranule of mesalazine coated with ethylcellulose. After administration and dissolution, mesalazine is gradually released from each microgranule during the passage of the tablet through the gastrointestinal tract from the duodenum to the rectum at any pH values of the intestinal environment. Within an hour after oral administration of the drug, microgranules are found in the duodenum, regardless of food intake. The average passage time through the intestine in healthy volunteers is 3-4 hours.

Absorption. 30 to 50% of the orally administered drug is absorbed in the small intestine of healthy volunteers. Mesalazine is detected in plasma 15 minutes after administration, and the maximum concentration of mesalazine in plasma is reached 1-6 hours after administration. The concentration of mesalazine in plasma gradually decreases and is no longer detectable 12 hours after administration. The curve of acetylmesalazine concentration in plasma has the same character, but is generally characterized by higher concentrations and slower elimination.

Dosing regimens of mesalazine 1 time per day (1 × 4 g/day) and 2 times per day (2 × 2 g/day) lead to comparable systemic exposure (AUC) over 24 hours and indicate continuous release of mesalazine from the drug form during the treatment period. With oral administration, a steady state is reached within 5 days.

MesalazineSingle doseSteady state
Cmax(ng/mL)AUC0–24(h·ng/mL)Cmax(ng/mL)AUC0–24(h·ng/mL)
2 g 2 times a day5103.5136,4566803.7057,519
4 g 1 time a day8561.3635,6579742.5150,742

The molecular weight of mesalazine is 153.13 g/mol; acetylmesalazine is 195.17 g/mol.

The release and absorption of mesalazine after oral administration do not depend on food intake, while systemic exposure may increase.

Distribution. The binding of mesalazine to plasma proteins is approximately 50%, and acetylmesalazine is approximately 80%. Mesalazine and acetylmesalazine do not pass through the blood-brain barrier.

Biodegradation. Mesalazine is converted to N-acetylmesalazine (acetylmesalazine) both presystemically in the intestinal mucosa and systemically in the liver, mainly by N-acetyltransferase-1 (NAT-1). Minor acetylation is carried out by bacteria in the large intestine. The acetylation of mesalazine is likely not related to the patient's acetylation phenotype. The metabolic ratio in plasma of acetylmesalazine to mesalazine is 3.5 and 1.3, respectively, after oral administration at a dose of 500 mg 3 times a day and 2 g 3 times a day, which reflects dose-dependent acetylation that may be caused by saturation with the drug. It is also believed that acetylmesalazine is clinically and toxicologically inactive.

Excretion. The half-life of mesalazine is approximately 40 minutes, and acetylmesalazine is approximately 70 minutes. Due to the gradual release of mesalazine from the drug form during passage through the gastrointestinal tract, the half-life after oral administration cannot be determined. However, a steady state is reached after oral administration within 5 days.

Mesalazine and acetylmesalazine are excreted in the urine and feces. The urine mainly contains acetylmesalazine.

In patients with impaired liver and kidney function, due to decreased excretion rates and increased systemic concentrations of mesalazine, the risk of kidney damage may increase.

Special Patient Groups

Pathophysiological changes, such as diarrhea and increased intestinal activity, observed in active inflammatory bowel disease, have only a minor effect on the penetration of mesalazine into the intestinal mucosa after oral administration. In patients with accelerated intestinal transit, an increase in the excretion of the daily dose with urine by 20-25% was observed. Similarly, excretion with feces increased.

Clinical Characteristics

Indications

Nonspecific ulcerative colitis of mild to moderate severity, Crohn's disease.

Contraindications

Hypersensitivity to mesalazine, to any of the components of the drug, or to salicylates. Severe liver and/or kidney dysfunction. Gastric or duodenal ulcer. Hemorrhagic diathesis.

Interactions with Other Medicinal Products and Other Forms of Interactions

Concomitant treatment with Pentasa and azathioprine, 6-mercaptopurine, or thioguanine in studies led to an increased frequency of myelosuppressive effects; an interaction between these agents is likely. The mechanism of this interaction is not definitively established. It is recommended to regularly monitor the white blood cell count and adjust the doses of thiopurines accordingly.

According to unconfirmed data, mesalazine may weaken the anticoagulant effect of warfarin.

Possible enhancement of the hypoglycemic effect of sulfonylurea derivatives, toxic effect of methotrexate. The activity of furosemide, spironolactone, sulfonamides, rifampicin, and uricosuric agents (probenecid and sulfinpyrazone) may be weakened. Mesalazine may potentiate the undesirable effect of glucocorticoids on the gastric mucosa and may reduce the absorption of digoxin.

Special Warnings and Precautions

Most patients with intolerance or hypersensitivity to sulfasalazine can use the Pentasa drug without the risk of similar reactions. However, the drug should be used with caution in patients with an allergy to sulfasalazine (risk of allergy to salicylates).

In case of acute symptoms of intolerance, such as spasms and acute abdominal pain, constipation, severe headache, and rash, treatment should be discontinued immediately.

The drug should be used with caution in patients with impaired liver function.

Before starting or during treatment, the doctor may decide to monitor liver function tests, such as ALT or AST.

The drug is not recommended for patients with renal insufficiency. It is necessary to regularly monitor kidney function (e.g., serum creatinine level, serum urea level, urine sedimentation, and methemoglobin concentration), especially at the beginning of treatment. It is necessary to determine the urological status of the patient (test strips) before and during treatment, at the doctor's discretion. In patients who develop kidney dysfunction during treatment, mesalazine-induced nephrotoxicity should be suspected.

Concomitant use of other drugs with a known nephrotoxic effect requires more frequent monitoring of kidney function.

When using mesalazine, patients have reported nephrolithiasis, including the formation of stones consisting 100% of mesalazine. Patients should be advised to drink sufficient fluids during treatment.

Patients with respiratory function disorders, including bronchial asthma, should be under close medical supervision during the treatment course (see "Adverse Reactions" section).

Mesalazine-induced hypersensitivity reactions from the heart (myocarditis and pericarditis) occur rarely. Very rarely, pathological changes in the blood system have been observed during mesalazine treatment. Before starting and during treatment, the doctor may recommend a blood test with a leukocyte formula.

When treating concomitantly with azathioprine, 6-mercaptopurine, or thioguanine, the risk of developing pathological changes in the blood may increase (see "Interactions with Other Medicinal Products and Other Forms of Interactions"). If signs or suspicion of such adverse reactions occur, treatment should be discontinued.

It is recommended to perform additional blood and urine tests 14 days after the start of treatment, and then 2-3 tests at 4-week intervals. If the results are within normal limits, subsequent tests should be performed every 3 months. If additional symptoms appear, these tests should be performed immediately.

Interference with Laboratory Tests

There have been several reports of a possible effect on the determination of normetanephrine in urine using liquid chromatography, which led to the receipt of false-positive results in patients with exposure to sulfasalazine or its metabolite, mesalamine/mesalazine.

Severe Skin Reactions

Severe skin reactions (SSR), including drug-induced eosinophilia with systemic symptoms (DRESS syndrome), Stevens-Johnson syndrome (SJS), and toxic epidermal necrolysis (TEN), have been reported in association with mesalazine treatment.

Treatment with mesalazine should be discontinued at the first signs of severe skin reactions, such as rash, mucosal lesions, or any other signs of hypersensitivity.

Mesalazine may cause a red-brown discoloration of urine after contact with sodium hypochlorite bleach (e.g., in toilets cleaned with sodium hypochlorite-containing bleach).

Use During Pregnancy or Breastfeeding

Pregnancy

It is known that mesalazine passes through the placental barrier. The concentration of the drug in the umbilical cord blood is lower than the concentration in the maternal blood. The same concentrations of the acetylmesalazine metabolite are found in the umbilical cord and maternal blood.

In several non-experimental studies, no teratogenic effects or significant risk of application to humans were found. Animal studies of oral mesalazine administration did not reveal direct or indirect harmful effects on pregnancy, embryonic and fetal development, childbirth, or postnatal development.

There are limited published data on the use of the Pentasa drug in pregnant women, which suggest no increase in the overall rate of congenital malformations.

Some data suggest an increased risk of premature birth, stillbirth, and low birth weight; however, these adverse outcomes of pregnancy may also be associated with active inflammatory bowel disease.

There have been reports of blood system disorders (pancytopenia, leukopenia, thrombocytopenia, anemia) in newborns whose mothers used mesalazine.

In one case, after prolonged use of mesalazine in high doses (2-4 g orally) during pregnancy, kidney failure was reported in a newborn.

Mesalazine can be used during pregnancy only when, in the doctor's opinion, the potential benefit to the mother outweighs the potential risk to the fetus. The underlying disease (inflammatory bowel disease) may increase the risk of an adverse pregnancy outcome.

Breastfeeding

Mesalazine passes into breast milk. The concentration of mesalazine in breast milk is lower than in the mother's blood, while the metabolite formed (acetylmesalazine) appears in the milk in the same or higher concentrations.

Data on the oral administration of the drug during breastfeeding are limited. Controlled studies of the effect of the Pentasa drug during breastfeeding have not been conducted. It cannot be ruled out that hypersensitivity reactions, such as diarrhea, may occur in infants. If diarrhea occurs in a breastfed infant, breastfeeding should be discontinued.

The Pentasa drug can be taken during breastfeeding, but only when, in the doctor's opinion, the potential benefit to the mother outweighs the potential risk to the child.

Fertility

Animal studies have shown no effect of mesalazine on fertility in males and females.

Ability to Affect the Speed of Reaction When Driving or Operating Other Mechanisms

Mesalazine does not affect or has a minor effect on the ability to drive or work with other mechanisms. If dizziness is observed during treatment, one should refrain from driving.

Method of Administration and Dosage

Adults Individual dosage.
Ulcerative colitisCrohn's disease
Exacerbation stageUp to 4 g of mesalazine 1 time a day or in several doses (divided into 2-3 doses).Up to 4 g of mesalazine per day in several doses (divided into 2-3 doses).
Maintenance therapyRecommended intake of 2 g of mesalazine 1 time a day.Up to 4 g of mesalazine per day in several doses.
Children (≥ 6 years) Individual dosage. There are only limited documented data on the effectiveness for children aged 6-18 years.
Ulcerative colitisCrohn's disease
Exacerbation stageInitial dose - 30-50 mg/kg/day in several doses. Maximum dose - 75 mg/kg/day in several doses. Total dose - no more than 4 g/day (maximum dose for adults).
Maintenance therapyInitial dose - 15-30 mg/kg/day in several doses. Total dose - no more than 2 g/day (recommended dose for adults).Initial dose - 15-30 mg/kg/day in several doses. Total dose - no more than 4 g/day (recommended dose for adults).

As a rule, children with a body weight of less than 40 kg are prescribed half the dose for adults, and children with a body weight of more than 40 kg are prescribed the full dose for adults.

Tablets should be taken orally, without chewing. To facilitate swallowing, the tablet can be dissolved in 50 mL of cold water. The mixture should be stirred and taken immediately.

The duration of treatment is determined by the doctor, depending on the course of the disease.

Children

The drug should not be used to treat children under the age of 6.

Overdose

There is only limited clinical experience with overdose of the Pentasa drug, which does not indicate the presence of kidney or liver toxicity. There is no specific antidote; treatment should be symptomatic and supportive. There have been reports of patients taking daily doses of the drug up to 8 g for a month without any adverse effects.

Due to the development of prolonged-release granules and the specific pharmacokinetic properties of mesalazine, poisoning is not expected even with high doses of the drug.

Generally, symptoms are expected to correspond to the symptoms of salicylate poisoning: acid-base imbalance, hyperventilation, and pulmonary edema, dehydration caused by sweating and vomiting, hypoglycemia.

Treatment of overdose: in case of acidosis or alkalosis, restoration of acid-base and electrolyte balance; in case of dehydration, rehydration; in case of hypoglycemia, administration of glucose. Additionally, intravenous infusion of electrolyte solutions should be performed to increase diuresis. Close monitoring of kidney function is necessary.

Adverse Reactions

Adverse reactions that were most frequently observed during clinical trials: diarrhea, nausea, abdominal pain, headache, vomiting, and rash. Hypersensitivity reactions and drug fever are occasionally observed.

In connection with mesalazine treatment, severe skin reactions (SSR), including drug-induced eosinophilia with systemic symptoms (DRESS syndrome), Stevens-Johnson syndrome (SJS), and toxic epidermal necrolysis (TEN), have been reported (see "Special Warnings and Precautions" section).

The frequency of adverse effects reported during clinical trials and post-marketing surveillance has been determined as follows: common (from ≥ 1/100 to < 1/10), rare (from ≥ 1/10000 to < 1/1000), very rare (< 1/10000), frequency unknown (cannot be established based on available data).

From the blood and lymphatic system: very rare - eosinophilia (as part of an allergic reaction), anemia, aplastic anemia, leukopenia (including granulocytopenia and neutropenia), thrombocytopenia, agranulocytosis, pancytopenia.

From the immune system: very rare - pancolitis, hypersensitivity reactions, including anaphylactic reactions, drug reactions with eosinophilia and systemic symptoms (DRESS syndrome).

From the nervous system: common - headache; rare - dizziness; very rare - peripheral neuropathy, benign intracranial hypertension (in children during puberty).

From the heart: rare - myocarditis and pericarditis.

From the respiratory system, thoracic cavity, and mediastinum: very rare - allergic and fibrotic changes in the lungs (including shortness of breath, cough, bronchospasm, allergic alveolitis, pulmonary eosinophilia, interstitial lung disease, pulmonary infiltration, pneumonitis).

From the gastrointestinal tract: common - diarrhea, abdominal pain, nausea, vomiting, flatulence; rare - increased amylase level, acute pancreatitis; very rare - pancolitis.

From the liver and bile ducts: very rare - liver dysfunction, including increased liver enzyme levels, signs of cholestasis (e.g., increased alkaline phosphatase, gamma-glutamyltransferase, and bilirubin levels), hepatotoxicity (including hepatitis, cholestatic hepatitis, cirrhosis, liver failure).

From the skin and subcutaneous tissue: common - rash (including urticaria, erythematous rash); rare - photosensitivity reactions; very rare - reversible alopecia, Quincke's edema, allergic dermatitis, multiform erythema; frequency unknown - Stevens-Johnson syndrome, toxic epidermal necrolysis, drug-induced eosinophilia with systemic symptoms (DRESS syndrome).

From the musculoskeletal system and connective tissue: very rare - myalgia, arthralgia, reactions similar to lupus erythematosus.

From the kidneys and urinary system: very rare - kidney dysfunction (including acute and chronic interstitial nephritis, nephrotic syndrome, kidney failure (acute and chronic), which may disappear after withdrawal of the drug); frequency unknown - nephrolithiasis, change in urine color.

From the reproductive system and breast: very rare - oligospermia (reversible).

General disorders: very rare - drug fever.

*The mechanism of development of mesalazine-induced myocarditis and pericarditis, pancreatitis, nephritis, and hepatitis is unknown, but may be of an allergic nature.

**Photosensitization: more severe reactions have been reported in patients with existing skin pathology, such as atopic dermatitis and atopic eczema.

***See "Special Warnings and Precautions" for detailed information.

It is important to note that some of these disorders may be associated with inflammatory bowel disease.

Reporting Adverse Reactions

Reporting suspected adverse reactions after the approval of a medicinal product is important. This allows for the continued monitoring of the benefit/risk ratio of the medicinal product. Healthcare professionals are asked to report any suspected adverse reactions through the national reporting system.

Shelf Life

3 years.

Storage Conditions

Store in a place inaccessible to children. Store at a temperature not exceeding 25 °C in a light-protected place.

Packaging

10 tablets in a blister pack, 5 or 10 blister packs in a carton box.

Release Category

By prescription.

Manufacturer

Ferring GmbH, Germany.

Manufacturer's Location and Address

Wittland 11, 24109 Kiel, Germany.

Online doctors for DEL'TALICIN

Discuss dosage, side effects, interactions, contraindications, and prescription renewal for DEL'TALICIN – subject to medical assessment and local rules.

5.0(96)
Doctor

Alina Tsurkan

Family medicine12 years of experience

Dr. Alina Tsurkan is a licensed family medicine physician based in Portugal, offering online consultations for adults and children. She provides professional primary care, with a focus on prevention, accurate diagnosis, and long-term management of acute and chronic conditions.

Dr. Tsurkan supports patients with a wide range of health issues, including:

  • Respiratory infections: cold, flu, bronchitis, pneumonia, and lingering coughs.
  • ENT conditions: sinusitis, tonsillitis, otitis (ear infections), sore throat, allergic rhinitis.
  • Eye conditions: allergic or infectious conjunctivitis, red eyes, irritation.
  • Digestive issues: acid reflux (GERD), gastritis, irritable bowel syndrome (IBS), constipation, bloating, nausea.
  • Urinary and reproductive health: urinary tract infections (UTIs), cystitis, prevention of recurrent infections.
  • Chronic diseases: hypertension, elevated cholesterol, weight management.
  • Neurological complaints: headaches, migraines, sleep disturbances, fatigue, general weakness.
  • Children’s health: fever, infections, digestive issues, follow-ups, vaccination guidance.

She also provides:

  • IMT medical certificates for driving licence exchange in Portugal.
  • Personalised preventive care and wellness consultations.
  • Interpretation of test results and medical reports.
  • Follow-up care and medication review.
  • Support in managing multiple coexisting conditions.
  • Remote prescription management and medical documentation.

Dr. Tsurkan’s approach is evidence-based and holistic. She works closely with each patient to develop an individualised care plan that addresses both symptoms and root causes. Her goal is to empower patients to take control of their health and maintain well-being through lifestyle adjustments, routine check-ups, and early intervention.

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Mar Tabeshadze

Endocrinology10 years of experience

Dr. Mar Tabeshadze is a licensed endocrinologist and general practitioner in Spain. She provides online consultations for adults, offering medical support for a wide range of endocrine conditions and related health concerns.

  • Diagnostic consultations for suspected endocrine disorders
  • Management of thyroid conditions, including in pregnant women
  • Early detection and treatment of type 1 and type 2 diabetes, with personalised therapy plans
  • Obesity treatment: identifying underlying causes of weight gain, combining medication and non-pharmacological strategies, and long-term support
  • Diagnosis and treatment of endocrine-related skin, hair, and nail issues
  • Ongoing care for patients with osteoporosis, pituitary, and adrenal gland disorders
Dr. Tabeshadze takes a patient-centred approach based on evidence-based medicine. Her goal is to help patients achieve hormonal balance, manage chronic conditions effectively, and improve overall well-being through targeted, personalised care.
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Giorgi Eremeishvili

Urology21 years of experience

Giorgi Eremeishvili is a top-category urologist, a Candidate of Medical Sciences, and a licensed physician in Spain. He provides expert assistance in the diagnosis and treatment of a wide range of urological conditions in both men and women, employing a comprehensive approach and evidence-based principles.

Key areas of expertise:

  • Erectile dysfunction, decreased libido, premature ejaculation.
  • Male infertility: comprehensive diagnosis and modern treatment methods.
  • Prostate gland diseases: acute and chronic prostatitis, prostatic adenoma (benign prostatic hyperplasia), prostate cancer.
  • Inflammatory diseases of the genitourinary system: acute and chronic cystitis, pyelonephritis, epididymitis, orchitis, urethritis.
  • Sexually transmitted infections (STIs): chlamydia, ureaplasmosis, mycoplasmosis, gardnerellosis, candidiasis, herpetic infections, HPV, CMV, trichomoniasis, and others.
  • Urination disorders: urinary retention, frequent urination, urinary incontinence, overactive bladder, neurogenic bladder.
  • Neoplasms: cysts, tumors of the kidneys, bladder, testicles, prostate gland (including prostate cancer).
  • Surgical interventions: determining indications and selecting optimal minimally invasive methods.

Dr. Eremeishvili applies an integrated approach to each case. This includes thorough preoperative preparation, postoperative observation, and regular dynamic follow-up during the treatment process to achieve the best possible outcomes. All diagnostic and therapeutic recommendations are based on current evidence-based medicine and comply with the recommendations of the European Association of Urology, guaranteeing high-quality and effective care.

If you are seeking qualified assistance in diagnosing or treating urological conditions, book an online consultation with Dr. Giorgi Eremeishvili. Get expert support, accurate diagnosis, and a personalized treatment plan from the comfort of your home.

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Oleksandr Babushkin

Orthopedics and traumatology17 years of experience

Dr Oleksandr Babushkin is an orthopaedic and trauma specialist providing online consultations for adults with joint, muscle, and spine-related concerns. He helps patients accurately assess symptoms, manage chronic and acute musculoskeletal conditions, and build effective recovery strategies through evidence-based care.

Online consultations include:

  • Evaluation of musculoskeletal symptoms: acute or chronic pain, stiffness, and reduced mobility.
  • Diagnosis and treatment advice for joint pain (knees, hips, shoulders, elbows), back and neck pain.
  • Support for conditions such as osteoarthritis, bursitis, tendinitis, and nerve compression syndromes.
  • Guidance after injuries: strains, sprains, bruises, suspected fractures, and overuse injuries.
  • Recovery support following orthopaedic surgery or trauma.
  • Monitoring treatment progress and adjusting therapy based on your symptoms and test results.

You can book a consultation if you experience:

  • Joint pain, limited mobility, or cracking sounds during movement.
  • Back or neck pain, especially with prolonged sitting or physical activity.
  • Chronic discomfort that affects your daily life or sleep.
  • Need for post-surgical follow-up or rehabilitation planning.

Dr Babushkin combines his expertise in orthopaedics and trauma care with a personalised, structured approach — helping patients regain mobility, reduce pain, and improve quality of life.

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Anna Moret

Dermatology18 years of experience

Dr. Anna Moret is a board-certified dermatologist and dermatovenereologist. She specialises in adult and pediatric dermatology, venereology, aesthetic skin care, and general medicine. Her consultations are evidence-based and tailored to each patient’s dermatological needs.

Dr. Moret provides expert evaluation and treatment for:

  • Skin conditions such as eczema, acne, rosacea, dermatitis, and psoriasis.
  • Hair and scalp issues including hair loss, dandruff, and seborrheic dermatitis.
  • Pediatric skin problems — from newborns to adolescents.
  • Sexually transmitted infections (STIs) and dermatovenereology.
  • Aesthetic concerns: skin ageing, non-invasive cosmetic treatments.
  • Skin allergies and hypersensitivity reactions.
  • Mole checks, lesion evaluation, and skin cancer screening.
  • Skincare advice and personalised cosmeceutical routines.

Combining dermatology with general medical knowledge, Dr. Moret offers comprehensive care that addresses both skin health and underlying conditions. She also holds certification from the Canadian Board of Aesthetic Medicine, ensuring an internationally aligned approach to aesthetic dermatology.

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Katia Benko

Pediatrics9 years of experience

Dr Katia Benko is a paediatrician with over 9 years of clinical experience and international training. She completed her medical education and residency in Argentina and is fully licensed to practise in Spain. Her work spans newborns, children and adolescents, with a focus on whole-person care that integrates physical, emotional and developmental health.

Areas of expertise:

  • online consultations for newborns, children and teens
  • evaluation and treatment of acute symptoms: fever, cough, infections, bronchiolitis, earache, etc.
  • long-term care for chronic paediatric conditions
  • preventive care at every stage of growth and development
  • child wellness visits and routine health check-ups
  • vaccination guidance according to standard and special schedules
  • assessment of neurodevelopment in infants and toddlers
  • feeding concerns: picky eating, food refusal, healthy habits, eating disorders
  • parental support in everyday health, emotional wellbeing and prevention
  • guidance for teenagers on healthy habits, self-care and risk prevention
Dr Benko sees paediatrics as a space for partnership with families – not only to treat illness, but to guide each child’s health journey with clarity, empathy and trust. Her goal is for every family to feel supported in making confident, informed decisions for their child’s wellbeing.
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Dmytro Horobets

Family medicine6 years of experience

Dr. Dmytro Horobets is a licensed family medicine physician in Poland, specialising in endocrinology, diabetology, obesity management, gastroenterology, pediatrics, general surgery, and pain medicine. He offers online consultations for adults and children, providing personalised medical support for a wide range of acute and chronic health concerns.

Areas of expertise:

  • Endocrinology: diabetes type 1 and type 2, prediabetes, thyroid disorders, metabolic syndrome, hormonal imbalance.
  • Obesity medicine: structured weight management plans, nutritional counselling, obesity-related health risks.
  • Gastroenterology: acid reflux (GERD), gastritis, irritable bowel syndrome (IBS), liver and biliary conditions.
  • Pediatric care: infections, respiratory symptoms, digestive issues, growth and development monitoring.
  • General surgery support: pre- and post-surgical consultations, wound care, rehabilitation.
  • Pain management: chronic and acute pain, back pain, joint pain, post-traumatic pain syndromes.
  • Cardiovascular health: hypertension, cholesterol control, risk assessment for heart disease.
  • Preventive medicine: regular check-ups, health screenings, long-term management of chronic conditions.

Dr. Horobets combines evidence-based medicine with a patient-centred approach. He carefully evaluates each patient’s medical history and symptoms, offering clear explanations and structured treatment plans adapted to individual needs.

Whether you need help managing diabetes, tackling weight-related health issues, interpreting lab results, or receiving general family medicine support, Dr. Horobets provides professional online care tailored to your specific health goals.

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Doctor

Karim BenHarbi

General medicine8 years of experience

Dr. Karim Ben Harbi is a licensed general practitioner based in Italy. He provides online consultations for adults and children, combining international clinical experience with evidence-based medicine. His care approach is focused on accurate diagnosis, preventive care, and personalised health guidance.

Dr. Ben Harbi received his medical degree from Sapienza University in Rome. His training included hands-on experience in diverse settings — tropical medicine, rural healthcare, and urban outpatient practice. He also conducted clinical research in microbiology, exploring the role of the gut microbiome in chronic gastrointestinal issues.

You can consult Dr. Ben Harbi for:

  • General health concerns, prevention, and primary care.
  • Hypertension, type 1 and type 2 diabetes, metabolic issues.
  • Cold, cough, flu, respiratory infections, sore throat, fever.
  • Chronic digestive issues: bloating, gastritis, IBS, microbiome imbalance.
  • Skin rashes, mild allergic reactions, basic dermatological complaints.
  • Medication guidance, treatment adjustments, prescription review.
  • Paediatric concerns — fever, infections, general well-being.
  • Lifestyle optimisation: stress, sleep, weight, and diet counselling.

Dr. Ben Harbi offers reliable, accessible medical support through online consultations, helping patients make informed decisions about their health with a clear, structured, and compassionate approach.

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€79
November 811:00
November 811:30
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Doctor

Khrystyna Habrykevych

Gastroenterology6 years of experience

Dr Khrystyna Habrykevych is a gastroenterologist providing online consultations for adults with digestive and abdominal health concerns. She helps patients understand the causes of their symptoms, interpret test results, and choose appropriate next steps – whether it’s further investigation, treatment, or lifestyle adjustments.

Common reasons for consultation include:

  • abdominal pain, cramps, discomfort, painful bowel movements
  • heartburn, acid reflux, burping, bitter taste in the mouth
  • bloating, excessive gas, nausea or vomiting
  • diarrhoea, constipation, difficulty passing stool
  • unexplained changes in weight or appetite
  • concern about gut health or long-term digestive issues
  • changes in lab results, questions about test interpretation
  • digestive system cancer screening and prevention
  • general digestive check-ups and health assessments
Dr Habrykevych follows evidence-based medical standards and adapts each consultation to the patient’s individual situation. The online format allows for timely medical support without the need for an in-person visit.
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€60
November 906:00
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Doctor

Sergei Nalkin

Neurology11 years of experience

Dr. Sergei Nalkin, PhD, is a neurologist, specialising in sports medicine and rehabilitation. He provides expert care for patients with neurological, musculoskeletal, and post-traumatic conditions, focusing on functional recovery and long-term symptom relief.

Dr. Nalkin offers consultations and treatment for:

  • Neurological disorders including migraines, tension headaches, and peripheral neuropathies.
  • Rehabilitation after stroke, brain injury, and spinal cord trauma.
  • Chronic pain syndromes and musculoskeletal dysfunctions.
  • Sports-related injuries: prevention, treatment, and recovery planning.
  • Coordination and movement disorders affecting mobility and balance.
  • Custom rehabilitation programmes for neurological and orthopedic conditions.

With a personalised, evidence-based approach, Dr. Nalkin helps patients restore physical function, reduce pain, and improve quality of life through targeted therapy and long-term support.

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€55
November 913:00
November 913:40
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