Benzpee 100mg Injection

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Benzpee 100mg Injection 1 1 शीशी ₹ 1139
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Benzpee 100mg Injection

Benzpee 100mg Injection 1 | 1 शीशी
₹ 1139
Benzpee 500mg Injection 1 | 1 शीशी
₹ 4776
people have bought this recently
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Benzpee Information

Benzpee, consists of Pegylated liposomal doxorubicin (PLD) is a specialized formulation of doxorubicin, an anthracycline chemotherapy drug used to treat various types of cancer. The pegylation (attachment of polyethylene glycol molecules) and liposomal encapsulation enhance the drug's pharmacokinetics, improving efficacy while reducing toxicity.

PLD is primarily used in the treatment of:

  • Ovarian Cancer (Platinum-resistant or recurrent cases)

  • Breast Cancer (Particularly in HER2-negative, metastatic cases)

  • Multiple Myeloma (In combination with bortezomib)

  • Kaposi’s Sarcoma (Especially in HIV-associated cases)

Doxorubicin works by intercalating into DNA, inhibiting topoisomerase II, and generating free radicals, leading to cell cycle arrest and apoptosis (cell death) in rapidly dividing cancer cells. However, the liposomal pegylation alters its properties:

Liposomal Encapsulation:

  • Protects doxorubicin from being rapidly cleared from circulation.

  • Reduces uptake by healthy tissues, minimizing cardiotoxicity.

Pegylation (Attachment of Polyethylene Glycol - PEG):

  • Increases circulation time in the bloodstream.

  • Enhances tumor penetration via the Enhanced Permeability and Retention (EPR) effect, where leaky tumor vasculature allows drug accumulation.

This formulation reduces the classic cardiotoxicity of doxorubicin while maintaining its anti-cancer efficacy. However, it introduces hand-foot syndrome (palmar-plantar erythrodysesthesia, PPE) as a notable side effect.

Pegylated liposomal doxorubicin (PLD) represents a significant advancement in chemotherapy, offering improved tumor targeting and reduced toxicity, especially in terms of cardiac side effects. It has established itself as a key treatment in ovarian cancer, breast cancer, multiple myeloma, and Kaposi’s sarcoma. However, hand-foot syndrome and myelosuppression remain dose-limiting toxicities, requiring careful monitoring and supportive care. Overall, PLD is a valuable option for patients requiring doxorubicin therapy but with a need for reduced toxicity and better tolerability.

Pharmacokinetics & Advantages:

  • Half life : 50-60 hours

  • Clearance : Slow (liposomes prevent rapid metabolism)

  • Tissue accumulation : Higher in tumors, lower in heart tissue

  • Cardiotoxicity risk : Lower

  • Dosing schedule : Less frequent due to extended half-life

The pegylated formulation allows for higher drug concentration at the tumor site while sparing healthy organs, particularly the heart, from toxic effects.

Indications & Clinical Use

1. Ovarian Cancer

  • Indicated for platinum-resistant ovarian cancer (when cancer recurs within six months of platinum-based chemotherapy).

  • Administered as monotherapy or in combination with bevacizumab.

  • Shows better tolerability and similar efficacy compared to topotecan or paclitaxel.

2. Breast Cancer

  • Used in HER2-negative metastatic breast cancer, particularly in patients at risk for cardiotoxicity.

  • Sometimes used as an alternative to conventional anthracyclines to reduce heart damage.

  • PLD reduces alopecia (hair loss) compared to standard doxorubicin.

3. Multiple Myeloma

  • Combined with bortezomib in relapsed/refractory multiple myeloma.

  • Improves progression-free survival (PFS) without significantly increasing toxicity.

4. Kaposi’s Sarcoma (KS)

  • First-line treatment for AIDS-related Kaposi’s sarcoma.

  • Preferred due to better skin penetration and lower systemic toxicity.

  • Effective in reducing lesion size and improving quality of life in KS patients.

Dosing & Administration

PLD is administered via intravenous infusion with a slow infusion rate to minimize infusion reactions.

Typical Dosage Guidelines:

  • Ovarian Cancer & Breast Cancer: 40-50 mg/m² every 4 weeks.

  • Multiple Myeloma (with Bortezomib): 30 mg/m² every 3 weeks.

  • Kaposi’s Sarcoma: 20 mg/m² every 3 weeks.

Dose adjustments may be needed in patients with:

  • Hepatic impairment (as doxorubicin is metabolized in the liver).

  • Severe myelosuppression (to reduce the risk of neutropenia and infections).

Side Effects & Toxicity

Common Side Effects:

  • Fatigue

  • Nausea/Vomiting

  • Mucositis (Mouth Sores)

  • Hand-Foot Syndrome (PPE)

  • Neutropenia (Low WBCs)

Serious Side Effects & Warnings:

Cardiotoxicity (Heart Damage)

  • Risk lower than conventional doxorubicin, but still present.

  • Cumulative lifetime dose should not exceed 450-500 mg/m².

  • Monitor Left Ventricular Ejection Fraction (LVEF) regularly.

Hand-Foot Syndrome (PPE)

  • A characteristic toxicity of PLD.

  • Presents as redness, swelling, pain, or peeling on palms and soles.

  • Managed by dose modification, emollients, cooling therapy.

Myelosuppression (Bone Marrow Suppression)

  • May cause neutropenia (low white blood cells), increasing infection risk.

  • Requires regular blood monitoring and dose adjustments.

Infusion-Related Reactions

  • Includes fever, chills, rash, and hypotension.

  • Pre-treatment with antihistamines and corticosteroids may reduce risk.

Contraindications

PLD is contraindicated in:

  • Severe cardiac disease (heart failure, low LVEF).

  • Severe hepatic dysfunction (as metabolism occurs in the liver).

  • Pregnancy & Breastfeeding (potential teratogenic effects).

  • Severe bone marrow suppression.



Benzpee Benefits & Uses

Benzpee is used to treat the following -

Main Benefits

  • Non-Small Cell Lung Cancer

Other Benefits

Benzpee Dosage & How to Take

This is the usual dosage recommended in most common treatment cases. Please remember that every patient and their case is different, so the dosage can be different based on the disease, route of administration, patient's age and medical history.

Find the right dosage based on disease and age

Age Group Dosage
Adult
  • Disease: Head and neck cancer
  • Before or After Meal: As advised by a physician
  • Single Maximum Dose: 830 mg
  • Dosage Route: Parenteral
  • Frequency: doctor administered
  • Course Duration: As directed by the doctor
  • Special Instructions: 500 mg/m² IV over 10 minutes on Day 1 of each 21-days cycle, given in combination with cisplatin
Geriatric
  • Disease: Head and neck cancer
  • Before or After Meal: As advised by a physician
  • Single Maximum Dose: 830 mg
  • Dosage Route: Parenteral
  • Frequency: doctor administered
  • Course Duration: As directed by the doctor
  • Special Instructions: 500 mg/m² IV over 10 minutes on Day 1 of each 21-days cycle, given in combination with cisplatin

Benzpee Related Warnings

  • Is the use of Benzpee safe for pregnant women?


    Pregnant women may get severe side effects after taking Benzpee. If you are pregnant, do not take Benzpee without a doctor's advice.

    Severe
  • Is the use of Benzpee safe during breastfeeding?


    Benzpee may cause serious side effects in breastfeeding women, so do not take this drug without doctor's advice.

    Severe
  • What is the effect of Benzpee on the Kidneys?


    Benzpee may cause harmful effects on kidney. if you feel its having any such effect, then stop taking this drug, and restart only on your doctor's advice.

    Moderate
  • What is the effect of Benzpee on the Liver?


    Benzpee does not damage the liver.

    Safe
  • What is the effect of Benzpee on the Heart?


    Benzpee is completely safe for the heart.

    Safe


Severe Interaction of Benzpee with Other Drugs

Benzpee should not be taken with following medicines due to severe side effects it may cause to patients -

Severe

Moderate



Benzpee Contraindications

If you are suffering from any of the following diseases, you should not take Benzpee unless your doctor advises you to do so -



Frequently asked Questions about Benzpee

  • Is this Benzpee habit forming or addictive?


    Forming a habit of Benzpee has not been reported.

    No
  • Is it safe to drive or operate heavy machinery when consuming?


    You may feel sleepy or tired after taking Benzpee. So it is best to avoid driving.

    Dangerous
  • Is it safe?


    Benzpee should be used only after doctor's advice.

    Safe, but take only on Doctor's advise
  • Is it able to treat mental disorders?


    No, Benzpee cannot treat any kind of mental disorder.

    No

Benzpee Interactions with Food and Alcohol

  • Interaction between Food and Benzpee


    Taking Benzpee with food is safe.

    Safe
  • Interaction between Alcohol and Benzpee


    Information about the interaction of Benzpee and alcohol is not currently available because this topic has not been researched yet.

    Unknown


See all substitutes for Benzpee


This medicine data has been created by -

Vikas Chauhan

B.Pharma, Pharmacy
5 Years of Experience


References

April Hazard Vallerand, Cynthia A. Sanoski. [link]. Sixteenth Edition. Philadelphia, China: F. A. Davis Company; 2019: Page No 999-1000

KD Tripathi. [link]. Seventh Edition. New Delhi, India: Jaypee Brothers Medical Publishers; 2013: Page No 863

US Food and Drug Administration (FDA) [Internet]. Maryland. USA; Package leaflet information for the user; Alimta (pemetrexed disodium)



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