Mbkacin

Mbkacin Uses, Dosage, Side Effects, Food Interaction and all others data.

Mbkacin Sulfate is a semi-synthetic aminoglycoside antibiotic. Mbkacin is active in vitro against Pseudomonas species, Escherichia coli, Proteus species, Providencia species, Klebsiella-Enterobacter species, Acinetobacter species, and Citrobacter freundii. When strains of the above organisms are found to be resistant to other aminoglycosides, including Gentamicin, TobrAmykin and KanAmykin, many are susceptible to Mbkacin. Mbkacin sulfate is active in vitro against penicillinase and nonpenicillinase-producing Staphylococcus species including methicillin-resistant strains.

Mbkacin is an aminoglycoside antibiotic. Aminoglycosides bind to the bacteria, causing misreading of t-RNA, leaving bacteria unable to synthesize proteins vital to their growth. Aminoglycosides are useful mainly in the treatment infections involving aerobic, Gram-negative bacteria, such as Pseudomonas, Acinetobacter, and Enterobacter. In addition, some mycobacteria, including the bacteria that cause tuberculosis, are susceptible to aminoglycosides. Infections caused by Gram-positive bacteria can also be treated with aminoglycosides, however, other antibiotics may be more potent and less toxic to humans.

Trade Name Mbkacin
Availability Prescription only
Generic Amikacin
Amikacin Other Names Amikacin, Amikacina, Amikacine, Amikacinum
Related Drugs amoxicillin, doxycycline, ciprofloxacin, cephalexin, metronidazole, azithromycin, clindamycin, ceftriaxone, levofloxacin, Augmentin
Type Injection
Formula C22H43N5O13
Weight Average: 585.6025
Monoisotopic: 585.285736487
Protein binding

The protein binding of amikacin in serum is ≤ 10%.

Groups Approved, Investigational, Vet approved
Therapeutic Class Aminoglycosides
Manufacturer Abbott Healthcare Pvt Ltd
Available Country India
Last Updated: September 19, 2023 at 7:00 am
Mbkacin
Mbkacin

Uses

Mbkacin is used for the short-term treatment of serious infections due to susceptible strains of Gram-negative bacteria. It is effective in bacterial septicemia (including neonatal sepsis); in serious infections of the respiratory tract, bones and joints, central nervous system (including meningitis) and skin and soft tissue; intra abdominal infections (including peritonitis); and in bums and post operative infections (including post-vascular surgery). Mbkacin is also effective in serious complicated and recurrent urinary tract infections due to susceptible Gram-negative organisms. It may be considered as initial therapy in suspected Gram-negative infections and therapy may be instituted before obtaining the results of susceptibility. Mbkacin is also effective in infections caused by Gentamycln and/or TobrAmykin resistant strains of Gram-negative organisms. Mbkacin has also been shown to be effective in Staphylococcal infection and may be considered as initial therapy under certain condition in the treatment of known suspected Staphylococcal disease such as, severe infections where the causative organism may either a Gram-negative bacterium or Staphylococcus infection due to susceptible strains of Staphylococcal I Gram-negative infections. In certain severe infections such as neonatal sepsis, concomitant therapy with a penicillin type drug may be used because of the possibility of infections due to Gram positive organism such as streptococci or pneumococci.

Mbkacin is also used to associated treatment for these conditions: Bacterial Peritonitis, Bacterial Sepsis, Bone and Joint Infections, Burns, Central Nervous System Infections, Endophthalmitis, Infection caused by staphylococci, Infective pulmonary exacerbation of cystic fibrosis, Intra-Abdominal Infections, Lung Infection, Meningitis, Bacterial, Mycobacterium avium complex infection, Neonatal Sepsis, Nosocomial Pneumonia, Postoperative Infections, Respiratory Tract Infection Bacterial, Skin and Subcutaneous Tissue Bacterial Infections, Tuberculosis (TB), Grade 1, grade 2, grade 3, grade 4 Urinary Tract Infection, Severe Bacterial Infections

How Mbkacin works

The primary mechanism of action of amikacin is the same as that for all aminoglycosides. It binds to bacterial 30S ribosomal subunits and interferes with mRNA binding and tRNA acceptor sites, interfering with bacterial growth. This leads to disruption of normal protein synthesis and production of non-functional or toxic peptides. Other actions have been postulated for drugs of this class. Mbkacin, as well as the rest of the aminoglycosides, are generally bacteriocidal against gram-positive and gram-negative bacteria.

Dosage

Mbkacin dosage

Adults and children: 15mg/kg/day in two equally- divided doses (equivalent to 500 mg bid in adults). Use of the 100 mg/2 ml strength is recommended for children for the accurate measurement of the appropriate dose.

Neonates and premature children: An initial loading dose of 10 mg/kg followed by 15 mg/kg/day in two equally divided doses.

Elderly: Doses should be adjusted under impaired renal function in elderly.

Life-threatening infections and/or those caused by pseudomonas: The adult dose may be increased to 500 mg every eight hours but should neither exceed 1.5 gm/day nor be administered for a period longer than 10 days. A maximum total adult dose of 15 gm should not be exceeded.

Urinary tract infections (Other than pseudomonal infections): 7.5 mg/kg/day in two equally divided doses (equivalent to 250 mg bid in adults).

Impaired renal function: In patient with impaired renal function the daily dose should be reduced and/or the intervals between doses increased to avoid accumulation of the drug. Simple doses schedule for renal impairment is given below:

Renal function Dosage schedule

Mild impairment 500 mg every 18 hours

Moderate impairment 500 mg every 24 hours

Severe impairment 250 mg every 24 hours.

Administration:

Intramuscular or intravenous administration: For most infections the intramuscular route is preferred, but in life threatening infections, or in patients in whom intramuscular injection route is not feasible the intravenous route may be used.

Intraperitoneal use: Mbkacin may be used as an irrigant after recovery from anesthesia in concentration of 0.25%.

Other routes of administration: Mbkacin in concentration of 0.25% may be used satisfactorily as an irrigating solution in abscess cavities, the pleural space, the peritoneum and the cerebral ventricles.

Intramuscular or intravenous administration: For most infections the intramuscular route is preferred, but in life threatening infections, or in patients in whom intramuscular injection route is not feasible the intravenous route may be used.

Intraperitoneal use: Mbkacin may be used as an irrigant after recovery from anesthesia in concentration of 0.25%.

Other routes of administration: Mbkacin in concentration of 0.25% may be used satisfactorily as an irrigating solution in abscess cavities, the pleural space, the peritoneum and the cerebral ventricles.

Side Effects

When the recommended precautions and dosages are followed the incidence of toxic reactous, such as tinnitus vertigo, and partial reversible or irreversible deafness, skin rash, drug fever, headache, paraesthesia, nausea and vomiting is low. Urinary signs of renal irritation, azotaemia and oliguria have been reported.

Toxicity

Oral (LD50): 6000 mg/kg (Mouse) . No antidote for toxicity is currently available. This drug is only 20% dialyzable; however, this is variable based on the type hemodialysis filter used.

Nephrotoxicity

Mild and reversible nephrotoxicity may be observed in 5 - 25% of patients. Mbkacin accumulates in the proximal renal tubular cells. Tubular cell regeneration occurs despite continued drug exposure. Toxicity most commonly occurs several days following initiation of therapy. Mbkacin may exacerbate pre-existing renal disease.

Ototoxicity

May cause irreversible ototoxicity. Ototoxicity appears to be correlated to cumulative exposure. Drug accumulation in the endolymph and perilymph of the inner ear causes irreversible damage to hair cells of the cochlea or summit of ampullar cristae in the vestibular complex. High- frequency hearing is lost first with progression leading to loss of low-frequency hearing. Further toxicity may lead to retrograde degeneration of the 8th cranial (vestibulocochlear) nerve. Vestibular toxicity may cause vertigo, nausea, vomiting, dizziness, and loss of balance.

Neuromuscular blockade

In addition to the above, amikacin may exacerbate neuromuscular blockade, however, this is less common.

Use in Pregnancy

Category D. Gentamicin and other aminoglycosides are known to cross the placenta. There is evidence of selective uptake of gentamicin by the fetal kidney resulting in damage to immature nephrons. Eighth cranial nerve damage has also been reported after in-utero exposure to some of the aminoglycosides. Because of the chemical similarity, all aminoglycosides should be considered potentially nephrotoxic and ototoxic to the developing fetus. Therapeutic blood amikacin levels in the mother do not equate with safety for the fetus. In reproductive toxicity studies in mice and rats, no effects on fertility or fetal toxicity were observed.

Use in Lactation

It is not known whether amikacin is excreted in breast milk. Since the possible harmful effect on the infant is not known, it is recommended that if nursing mothers must be given amikacin, the infants should not be breastfed during therapy.

Precaution

Since Mbkacin is present in high concentrations in the renal excretory system, patients should be well hydrated to minimize chemical irritation of the renal tubules. If azotemia increases, treatment should be stopped. Monitoring of renal function during treatment with aminoglycosides is particularly important.

Interaction

Concurrent administration of Mbkacin with myorelaxants leads to potentiation of their effects and there is a possibility of cessation of the breathing. The combination with other Aminoglycoside antibiotics should be avoided because of the augmentation of their ototoxic and nephrotoxic effects. Concurrent administration of Mbkacin with fast acting diuretics increases the risk of ototoxicity in patients with renal failure. Combination with Cephalosporins or Polymixins increases the risk of nephrotoxicity.

Food Interaction

No interactions found.

Volume of Distribution

  • 24 L (28% of body weight healthy adult subjects).

Following administration of usual dosages of amikacin, amikacin has been found in bone, heart, gallbladder, and lung tissue. Mbkacin is also distributed into bile, sputum, bronchial secretions, and interstitial, pleural, and synovial fluids.

Elimination Route

Rapidly absorbed after intramuscular administration. Rapid absorption occurs from the peritoneum and pleura. Poor oral and topical absorption. Poorly absorbed from bladder irrigations and intrathecal administration.

The bioavailability of this drug is expected to vary primarily from individual differences in nebulizer efficiency and airway pathology.

Following IM administration of a single dose of amikacin of 7.5 mg/kg in adults with normal renal function, peak plasma amikacin concentrations of 17-25 micrograms/mL are attained within 45 minutes to 2 hours.

Following IV infusion of the same dose given over 1 hour peak plasma concentrations of the drug average 38 micrograms/mL immediately following the infusion, 5.5 micrograms/mL at 4 hours, and 1.3 micrograms/mL at 8 hours.

Half Life

The plasma elimination half-life of amikacin is usually 2-3 hours in adults with normal renal function and is reported to range from 30-86 hours in adults with severe renal impairment.

Clearance

The mean serum clearance rate is about 100 mL/min and the renal clearance rate is 94 mL/min in subjects with normal renal function.

Elimination Route

This drug is eliminated by the kidneys. In adults with normal renal function, 94-98% of a single IM or IV dose of amikacin is excreted unchanged by glomerular filtration in the kidney within 24 hours. Mbkacin can be completely recovered within approximately 10-20 days in patients with normal, healthy renal function.

In patients with impaired renal function, the clearance of amikacin is found to be decreased; the more severe the impairment, the slower the clearance. The interval between doses of amikacin should be adjusted according to the level of renal impairment. Endogenous creatinine clearance rate and serum creatinine which have a high correlation with serum half-life of amikacin, may be used as a guide for dosing.

Pregnancy & Breastfeeding use

The safety of Mbkacin in pregnancy has not yet been established.

Contraindication

Mbkacin injection is contraindicated in patients with a known history of hypersensitivity to Mbkacin.

Special Warning

Impaired renal function: In patient with impaired renal function the daily dose should be reduced and/or the intervals between doses increased to avoid accumulation of the drug. Simple doses schedule for renal impairment is given below:

  • Mild impairment: 500 mg every 18 hours
  • Moderate impairment: 500 mg every 24 hours
  • Severe impairment: 250 mg every 24 hours.

Pediatric Use: Safety and effectiveness of Mbkacin for injection in children or adolescents under 16 years have not been established

Acute Overdose

In the event of overdose or toxic reaction, peritoneal dialysis or hemodialysis will aid in the removal of Mbkacin from the blood.

Interaction with other Medicine

No information regarding drug interaction of Mbkacin is available.

Storage Condition

Store in a cool dry place protected from light. Keep out of reach of children.

Innovators Monograph

You find simplified version here Mbkacin

Mbkacin contains Amikacin see full prescribing information from innovator Mbkacin Monograph, Mbkacin MSDS, Mbkacin FDA label

FAQ

What is Mbkacin used to treat?

Mbkacin is a semi-synthetic aminoglycoside antibiotic derived from Kanamycin.It is used to treat certain serious infections that are caused by bacteria such as meningitis and infections of the blood, abdomen (stomach area), lungs, skin, bones, joints, and urinary tract.

What are the common side effects of Mbkacin?

Common side effects of Mbkacin include:

  • diarrhea,
  • hearing loss,
  • spinning sensation (vertigo),
  • numbness,
  • skin tingling,
  • muscle twitching and convulsions,
  • dizziness,
  • ringing or roaring in the ears,
  • allergic reactions,
  • Clostridium difficile associated diarrhea (CDAD),
  • skin rash,
  • drug fever,
  • headache,
  • numbness and tingling,
  • tremor,
  • nausea,
  • vomiting,
  • increase in white blood cells (eosinophilia),
  • joint pain,
  • anemia,
  • low blood pressure, and
  • low blood magnesium.

Is Mbkacin safe for pregnancy?

Mbkacin is harmful to the fetus and should not be used during pregnancy unless there are not safer options.

Is Mbkacin safe for breastfeeding?

brfand is poorly excreted into breastmilk. it is best to be cautious before using it while breastfeeding.

Can Mbkacin damage kidneys?

Mbkacin can harm your kidneys, and may also cause nerve damage or hearing loss, especially if you have kidney disease or use certain other medicines.

When should I take Mbkacin?

You should take Mbkacin if  you are not allergic to amikacin or similar antibiotics such as gentamicin, kanamycin, neomycin, paromomycin, streptomycin, or tobramycin.

Is Mbkacin toxic?

Mbkacin can cause neurotoxicity if used at a higher dose or for longer than recommended.

How long is Mbkacin used for?

The recommended dose in prematures is 7.5 mg/kg in every 12 hours .The usual duration of treatment is 7 to 10 days.The total daily dose by all routes of administration should not exceed 15-20 mg/kg/day.

Can Mbkacin be given alone?

Mbkacin is rarely used alone and often combined with other antimicrobials.

What is indication of Mbkacin?

Mbkacin sulfate injection is indicated in the short-term treatment of serious infections due to susceptible strains of Gram-negative bacteria including Pseudomonas species, Escherichia coli, species of indole-positive and indole-negative Proteus, Providencia species, Klebsiella-Enterobacter-Serratia species.

Can Mbkacin cause hearing loss?

amikacin or kanamycin is likely to result in the development of permanent hearing loss

How long does it take for Mbkacin to work?

recommended dosage level, uncomplicated infections due to sensitive organisms should respond to therapy within 24 to 48 hours.

Can Mbkacin be given orally?

There is no oral form available, as Mbkacin is not absorbed orally.

How long does Mbkacin stay in the body?

In adults with normal renal function the plasma elimination half-life of amikacin is usually 2-3 hours.

Can I drink alcohol with Mbkacin?

Using alcohol certain medicines may also cause interactions to occur. 

Can I drive after taking Mbkacin?

 Do not drive, use machinery after taking Mbkacin.You may get drowsy or dizzy.

*** Taking medicines without doctor's advice can cause long-term problems.
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