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PROJECT TITLE
PRODUCTION OF ERYTHROMYCIN
GROUP MEMBERS
UMESH VERMA 17BTBIOCE003
HARSHITA RAI 17BTBIOCE004
TUSHAR MISHRA 17BTBIOCE005
ATAUL ADNANI 17BTBIOCE009
NITINJAY SINGH 17BTBIOCE011
CONTENT
1. INTRODUCTION
HISTORY OF ERYTHROMYCIN
GENRAL CHARACTERISTIC ( UMESH VERMA )
2. MECHANISM OF ACTION ,PHARMACOKINETICS
BIOSYNTHESIS OF ERYTHROMYCIN ( HARSHITA RAI )
3. INDUSTRIAL PRODUCTION ( TUSHAR MISHRA )
INNOCULUM DEVELOPMENT, FERMENTATION
4. ISOLATION & EXTRACTION ( ATAUL ADNANI )
5. IMPROVEMENT OF STRAIN & CLINICAL USES
( NITINJAY SINGH )
INTRODUCTION
 Erythromycin belongs to the group of Macrolide antibiotics.
 Macrolide antibiotics slow the growth of, or sometimes kill
sensitive bacteria by reducing the production of important
proteins needed by the bacteria to survive.
 It has an antimicrobial spectrum similar to or slightly wider
than that of penicillin and is often used for people who have
allergy to penicillin.
CONTINUED…
 Erythromycin is produced using Streptomyces.
 Streptomyces is a genus of Gram-positive bacteria that grows in
various environments, with a filamentous form similar to fungi.
 The commonly used macrolides are:
 Erythromycin.
 Clarithromycin.
 Roxithromycin
 Azithromycin
HISTORY
 Erythromycin was discovered in 1952 .
 Eli Lilly’s research team, led by J. M. McGuire managed
to isolate erythromycin from the metabolic products of a
strain of Streptomyces erythreus.
 Found in a soil sample from the Philippines.
GENERAL CHARACTERISTICS
 Erythromycin contains three characteristics parts in the molecule:
 A highly substituted macrocyclic lactone: aglycone
 It is a macrocyclic compound containing 14-membered lactone ring
with 10 asymmetric centers.
 A ketone group.
 An amino deoxysugar: glycon
 Its chemical formula is C37 H67NO13
 Molecular Weight 733.937 g/mol
Physical and Chemical properties
 It is a crystalline, colorless compound .
 Slightly soluble in water but dissolves easily in most of the common organic
solvents.
 Crystals are obtained readily from aqueous acetone, aqueous alcohol or
chloroform.
 Odorless
 Taste is Bitter
MECHANISM OF ACTION
 Erythromycin displays a bacteriocidal activity particularly at
higher concentrations.
 It prevents the growth of bacteria by inhibiting their protein
synthesis.
 Erythromycin binds to the 23s rRNA molecule in the 50S
ribosomal subunit.
 Binding site near the peptidyl transferase center.
 This binding blocks the exit of the growing peptide thus inhibiting
the translocation of the peptides.
MECHANISM
Pharmacokinetics
 Erythromycin is easily inactivated by gastric acids, therefore all
orally administered formulations are given as either enteric
coated or more stable salts or esters, such as erythromycin
ethyl succinate.
 It is rapidly absorbed and diffused into most tissues and
phagocytes.
 Due to high concentration in phagocytes, erythromycin is
actively transported to the site of infection, where during active
phagocytosis, large concentration of erythromycin is released
Erythromycin Biosynthesis.
 The three genes eryAI–III encode for the multidomain proteins DEBS1–3.
 The first protein, DEBS1, consist of a loading module with an
actyltransferase (AT) and acyl carrier protein (ACP) domain, followed by
module 1 with the ketosynthase (KS), AT, ketoreductase (KR), and an ACP
domain, followed by module 2 with KS, AT, KR, and ACP domains.
 The second protein, DEBS2, consists of two modules, with a KS, AT, ACP
domain and a KS, AT, dehydrogenase (DH), enoylreductase (ER), KR, ACP
domain, respectively.
 The third protein, DEBS3, also consists of two modules and a thioesterase
(TE) domain to release the polyketide from the module.
INDUSTRIAL PRODUCTION
 Erythromycin is produced from Streptomyces and
Micromonospora.
 Erythromycin is produced mainly by submerged
fermentation.
 During fermentation, different types of erythromycin
are produced like erythromycin A, B, C, and D.
 The steps for erythromycin production are as follows:
Inoculum Development
 Inoculum is prepared from suspension of at least 108 cells/ml.
 Sporulation of S.erythraeus is done on tryptone agar slant.
 Cells are harvested from agar plates and suspension is taken in sterile water and
stored at 4ºC .
2. Medium:
 Sucrose/ starch
 Corn steep liquor
 Soyabean oil meal
 Yeast
 NaCl
 CaCo3 precipitate
 pH
 Water
S. erythraea Fermentation
 Fermentation is carried out in stirred tank fermenter.
 The batch starts with sterilization followed by pumping
deionized water into the fermenter.
 The organism is grown in the broth for 4 days at a
temperature of 26° C
Cont..
 Addition of n-propanol increases the production of erythromycin.
 Samples were drawn aseptically through a cross flow filter assembly .
 Production of Erythromycin production occurs when froth reaches
stationary phase.
 Daily samples of 50 or 100 mL were drawn to determine the
erythromycin concentration.
 Samples were stored at -20 °C.
Isolation & Extraction of Erythromycin
 Mycelium is separated from the broth by filter press,
centrifugation or drum filtration.
 Acidic condition helps to separate mycelium the broth.
 Acidic condition is maintained by addition of Butyl acetate which
favors the separation of the mycelium. Also it dissolves the
antibiotic.
 It is then washed with water.
Extraction
 It is extracted using methyl iso butyl ketone or ethyl acetate.
 It is then transferred to acidic water.
 pH is adjusted with HCl, acetic acid and citric acid.
 Purification and concentration is carried out in ion exchange
resin amberlite 50.
 Elution is carried out by a mixture of organic solvents and water
at pH 3 to 8.
 Erythromycin is obtained as dihydrate salt.
 The dehydrate crystals of erythromycin are filtered and dried on
vacum tray dryer..
IMPROVEMENT OF STRAIN
 Saccharopolyspora erythraea MTCC 1103 is used for the enhanced
production of erythromycin.
 Strain improvement was done by random UV-mutagenesis.
 Mutant strain showed 40 % higher yield in production medium as
compared to wild strain.
 Erythromycin potency assay and HPLC analysis were performed to confirm
the presence of erythromycin in the partially purified samples.
 Effects of various parameters such as bagasse concentration, organic
nitrogen source, inorganic nitrogen source, pH and temperature.
CARBON SOURCE
 Bagasse can be used as an alternate carbon source in erythromycin
medium.
 Erythromycin production medium was found to be 512 mg/L which was 28 %
higher than glucose based medium.
NITROGEN SOURCE
 It was found that corn steep liquor was best as compared to yeast extract,
malt extract, casein and peptone.
 For corn steep liquor, concentration of erythromycin 416 mg/L.
 Yeast extract and malt extract 356 and 310 mg/L
 Peptone added medium 120 mg/L
ERYTHROMYCIN CONCENTRATION
CONT…
pH
 Erythromycin production rate was high at pH 7
 At pH 7, the concentration of erythromycin was found to be 461 mg/L
and dry weight of cell biomass as 500 mg/L.
Temperature
 The optimum temperature for erythromycin production was found to be 28
°C
CLINICAL USES
 Erythromycin is an antibiotic useful for the treatment of a number of
bacterial infections.
 This includes respiratory tract infections, skin infections, chlamydia infections,
pelvic inflammatory disease, and syphilis.
 Erythromycin may be used to improve delayed stomach emptying.
 It can be given intravenously and by mouth. An eye ointment is routinely
recommended after delivery to prevent eye infections in the newborn.
CONT…
 Penicillin substitute in penicillin allergic individuals
 In respiratory, neonatal, ocular, or genital chlamydial infections.
 Treatment of community-acquired pneumonia.
 Used in covid 19 with hydroxychloroquine.
 It may also be used during pregnancy to prevent Group B streptococcal
infection in the newborn.
 Prophylaxis against endocarditis during dental procedures in individuals with
valvular heart disease.
SIDE EFFECTS OF ERYTHROMYCIN
 Inflammation of the liver.
 Confusion or hallucinations.
 Kidney inflammation or infection.
 Abdominal pain.
 vomiting
THANK YOU

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Production of erythromycin

  • 1. PROJECT TITLE PRODUCTION OF ERYTHROMYCIN GROUP MEMBERS UMESH VERMA 17BTBIOCE003 HARSHITA RAI 17BTBIOCE004 TUSHAR MISHRA 17BTBIOCE005 ATAUL ADNANI 17BTBIOCE009 NITINJAY SINGH 17BTBIOCE011
  • 2. CONTENT 1. INTRODUCTION HISTORY OF ERYTHROMYCIN GENRAL CHARACTERISTIC ( UMESH VERMA ) 2. MECHANISM OF ACTION ,PHARMACOKINETICS BIOSYNTHESIS OF ERYTHROMYCIN ( HARSHITA RAI ) 3. INDUSTRIAL PRODUCTION ( TUSHAR MISHRA ) INNOCULUM DEVELOPMENT, FERMENTATION 4. ISOLATION & EXTRACTION ( ATAUL ADNANI ) 5. IMPROVEMENT OF STRAIN & CLINICAL USES ( NITINJAY SINGH )
  • 3. INTRODUCTION  Erythromycin belongs to the group of Macrolide antibiotics.  Macrolide antibiotics slow the growth of, or sometimes kill sensitive bacteria by reducing the production of important proteins needed by the bacteria to survive.  It has an antimicrobial spectrum similar to or slightly wider than that of penicillin and is often used for people who have allergy to penicillin.
  • 4. CONTINUED…  Erythromycin is produced using Streptomyces.  Streptomyces is a genus of Gram-positive bacteria that grows in various environments, with a filamentous form similar to fungi.  The commonly used macrolides are:  Erythromycin.  Clarithromycin.  Roxithromycin  Azithromycin
  • 5. HISTORY  Erythromycin was discovered in 1952 .  Eli Lilly’s research team, led by J. M. McGuire managed to isolate erythromycin from the metabolic products of a strain of Streptomyces erythreus.  Found in a soil sample from the Philippines.
  • 6. GENERAL CHARACTERISTICS  Erythromycin contains three characteristics parts in the molecule:  A highly substituted macrocyclic lactone: aglycone  It is a macrocyclic compound containing 14-membered lactone ring with 10 asymmetric centers.  A ketone group.  An amino deoxysugar: glycon  Its chemical formula is C37 H67NO13  Molecular Weight 733.937 g/mol
  • 7. Physical and Chemical properties  It is a crystalline, colorless compound .  Slightly soluble in water but dissolves easily in most of the common organic solvents.  Crystals are obtained readily from aqueous acetone, aqueous alcohol or chloroform.  Odorless  Taste is Bitter
  • 8. MECHANISM OF ACTION  Erythromycin displays a bacteriocidal activity particularly at higher concentrations.  It prevents the growth of bacteria by inhibiting their protein synthesis.  Erythromycin binds to the 23s rRNA molecule in the 50S ribosomal subunit.  Binding site near the peptidyl transferase center.  This binding blocks the exit of the growing peptide thus inhibiting the translocation of the peptides.
  • 10. Pharmacokinetics  Erythromycin is easily inactivated by gastric acids, therefore all orally administered formulations are given as either enteric coated or more stable salts or esters, such as erythromycin ethyl succinate.  It is rapidly absorbed and diffused into most tissues and phagocytes.  Due to high concentration in phagocytes, erythromycin is actively transported to the site of infection, where during active phagocytosis, large concentration of erythromycin is released
  • 11. Erythromycin Biosynthesis.  The three genes eryAI–III encode for the multidomain proteins DEBS1–3.  The first protein, DEBS1, consist of a loading module with an actyltransferase (AT) and acyl carrier protein (ACP) domain, followed by module 1 with the ketosynthase (KS), AT, ketoreductase (KR), and an ACP domain, followed by module 2 with KS, AT, KR, and ACP domains.  The second protein, DEBS2, consists of two modules, with a KS, AT, ACP domain and a KS, AT, dehydrogenase (DH), enoylreductase (ER), KR, ACP domain, respectively.  The third protein, DEBS3, also consists of two modules and a thioesterase (TE) domain to release the polyketide from the module.
  • 12. INDUSTRIAL PRODUCTION  Erythromycin is produced from Streptomyces and Micromonospora.  Erythromycin is produced mainly by submerged fermentation.  During fermentation, different types of erythromycin are produced like erythromycin A, B, C, and D.  The steps for erythromycin production are as follows:
  • 13. Inoculum Development  Inoculum is prepared from suspension of at least 108 cells/ml.  Sporulation of S.erythraeus is done on tryptone agar slant.  Cells are harvested from agar plates and suspension is taken in sterile water and stored at 4ºC . 2. Medium:  Sucrose/ starch  Corn steep liquor  Soyabean oil meal  Yeast  NaCl  CaCo3 precipitate  pH  Water
  • 14. S. erythraea Fermentation  Fermentation is carried out in stirred tank fermenter.  The batch starts with sterilization followed by pumping deionized water into the fermenter.  The organism is grown in the broth for 4 days at a temperature of 26° C
  • 15. Cont..  Addition of n-propanol increases the production of erythromycin.  Samples were drawn aseptically through a cross flow filter assembly .  Production of Erythromycin production occurs when froth reaches stationary phase.  Daily samples of 50 or 100 mL were drawn to determine the erythromycin concentration.  Samples were stored at -20 °C.
  • 16. Isolation & Extraction of Erythromycin  Mycelium is separated from the broth by filter press, centrifugation or drum filtration.  Acidic condition helps to separate mycelium the broth.  Acidic condition is maintained by addition of Butyl acetate which favors the separation of the mycelium. Also it dissolves the antibiotic.  It is then washed with water.
  • 17. Extraction  It is extracted using methyl iso butyl ketone or ethyl acetate.  It is then transferred to acidic water.  pH is adjusted with HCl, acetic acid and citric acid.  Purification and concentration is carried out in ion exchange resin amberlite 50.  Elution is carried out by a mixture of organic solvents and water at pH 3 to 8.  Erythromycin is obtained as dihydrate salt.  The dehydrate crystals of erythromycin are filtered and dried on vacum tray dryer..
  • 18. IMPROVEMENT OF STRAIN  Saccharopolyspora erythraea MTCC 1103 is used for the enhanced production of erythromycin.  Strain improvement was done by random UV-mutagenesis.  Mutant strain showed 40 % higher yield in production medium as compared to wild strain.  Erythromycin potency assay and HPLC analysis were performed to confirm the presence of erythromycin in the partially purified samples.  Effects of various parameters such as bagasse concentration, organic nitrogen source, inorganic nitrogen source, pH and temperature.
  • 19. CARBON SOURCE  Bagasse can be used as an alternate carbon source in erythromycin medium.  Erythromycin production medium was found to be 512 mg/L which was 28 % higher than glucose based medium. NITROGEN SOURCE  It was found that corn steep liquor was best as compared to yeast extract, malt extract, casein and peptone.  For corn steep liquor, concentration of erythromycin 416 mg/L.  Yeast extract and malt extract 356 and 310 mg/L  Peptone added medium 120 mg/L
  • 21. CONT… pH  Erythromycin production rate was high at pH 7  At pH 7, the concentration of erythromycin was found to be 461 mg/L and dry weight of cell biomass as 500 mg/L. Temperature  The optimum temperature for erythromycin production was found to be 28 °C
  • 22. CLINICAL USES  Erythromycin is an antibiotic useful for the treatment of a number of bacterial infections.  This includes respiratory tract infections, skin infections, chlamydia infections, pelvic inflammatory disease, and syphilis.  Erythromycin may be used to improve delayed stomach emptying.  It can be given intravenously and by mouth. An eye ointment is routinely recommended after delivery to prevent eye infections in the newborn.
  • 23. CONT…  Penicillin substitute in penicillin allergic individuals  In respiratory, neonatal, ocular, or genital chlamydial infections.  Treatment of community-acquired pneumonia.  Used in covid 19 with hydroxychloroquine.  It may also be used during pregnancy to prevent Group B streptococcal infection in the newborn.  Prophylaxis against endocarditis during dental procedures in individuals with valvular heart disease.
  • 24. SIDE EFFECTS OF ERYTHROMYCIN  Inflammation of the liver.  Confusion or hallucinations.  Kidney inflammation or infection.  Abdominal pain.  vomiting