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Post Translational Modifications (PTMs):
 Covalent or generally enzymatic modifications of proteins during or after
the synthesis of the proteins.
 Post translational modifications or PTMs are involved in modifying the
protein structure after they have been translated according to
information on the mRNA.
 The post translational modifications can be enzymatic or covalent.
 In the human body these PTMs increases the diversity and accuracy of
proteins.
Types of PTMs:
Trimming
Covalent Attachments
Protein Folding
Protein Degradation
Trimming:
Insulin is synthesized in the cells and it is in inactive form that it is can’t
perform it’s function. For the proper functioning of insulin its post
translational modifications occurs that have involve the removal of the part
of protein to convert it into a three dimensional and fully active form.
Covalent Attachments:
Covalent attachments refers to the addition or the transfer of the
polypeptide chain that acts as an acceptor region. In this way, proteins are
modified for the diversity of function. It includes:
 Phosphorylation
 Glycosylation
 Sulfation
 Methylation
 Hydroxylation
Phosphorylation:
 Phosphorylation is the addition of one or more phosphate groups to the
protein. Post Translational Phosphorylation is one of the most common
protein modifications that occur in animal cells. The vast majorities of
phosphorylation occur as a mechanism to regulate the biological activity
of a protein and as such are transient.
 In animal cells Serine, tyrosine and threonine are the amino acids that
subjected to the phosphorylation.
Glycosylation:
Glycosylation is the addition of carbohydrate molecules to the polypeptide
chain and modifying it into glycoproteins. Many of the proteins that are
destined to become a part of plasma membrane or to be secreted from the
cell, have carbohydrate chains attached to the amide nitrogen of
asparagine(N linked) or the hydroxyl groups of serine, threonine(O linked).
N glycosylation occurs in ER and O glycosylation occurs in the Golgi
Complex.
Sulfation:
Sulfate modification takes place by the addition of sulphate molecules and
these modifications of proteins occurs at tyrosine residues. Tyrosine
sulfation accomplished via the activity of tyrosyl protein sulfotransferases
(TPST) which are membrane associated enzymes of trans-Golgi network.
There are two known TPSTs.
1. TPST-1
2. TPST-2
The universal phosphate donor is 3’-phosphoadenosyl-5’-phosphosulphate
(PSPA).
Methylation:
The transfer of one-carbon methyl groups to nitrogen or oxygen to amino
acid side chains increases the hydrophobicity of the protein and can
neutralize a negative amino acid charge when bound to carboxylic acids.
Methylation is mediated by methyl transferases and S-adenosyl methionine
(SAM) is the primary methyl group donor.
Hydroxylation:
The biological process of addition of a hydroxy group to a protein amino acid
is called Hydroxylation. Protein hydroxylation is one type of PTM that
involves the conversion of –CH group into –COH group and these
hydroxylated amino acids are involved in the regulation of some important
factors called transcription factors. Among 20, the two amino acids can be
regulated these are proline and lysine.
Protein Degradation:
Proteins that are defective for example, misfolded or destined for rapid
turnover are often marked for destruction by ubi ubiquitination-the
attachment of chains of a small, highly conserved protein, called ubiquitin.
Proteins marked in this way are rapidly degraded by a cellular component
known as the proteasome, which is a macromolecular, ATP-dependent,
proteolytic system located in the cytosol.
Protein Folding:
Proteins must fold to assume their functional state. Folding can be
spontaneous or facilitated by proteins known as Chaperones.

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Molecular Biology Presentation.pptx

  • 1. Post Translational Modifications (PTMs):  Covalent or generally enzymatic modifications of proteins during or after the synthesis of the proteins.  Post translational modifications or PTMs are involved in modifying the protein structure after they have been translated according to information on the mRNA.  The post translational modifications can be enzymatic or covalent.  In the human body these PTMs increases the diversity and accuracy of proteins.
  • 2. Types of PTMs: Trimming Covalent Attachments Protein Folding Protein Degradation
  • 3. Trimming: Insulin is synthesized in the cells and it is in inactive form that it is can’t perform it’s function. For the proper functioning of insulin its post translational modifications occurs that have involve the removal of the part of protein to convert it into a three dimensional and fully active form.
  • 4.
  • 5. Covalent Attachments: Covalent attachments refers to the addition or the transfer of the polypeptide chain that acts as an acceptor region. In this way, proteins are modified for the diversity of function. It includes:  Phosphorylation  Glycosylation  Sulfation  Methylation  Hydroxylation
  • 6. Phosphorylation:  Phosphorylation is the addition of one or more phosphate groups to the protein. Post Translational Phosphorylation is one of the most common protein modifications that occur in animal cells. The vast majorities of phosphorylation occur as a mechanism to regulate the biological activity of a protein and as such are transient.  In animal cells Serine, tyrosine and threonine are the amino acids that subjected to the phosphorylation.
  • 7.
  • 8. Glycosylation: Glycosylation is the addition of carbohydrate molecules to the polypeptide chain and modifying it into glycoproteins. Many of the proteins that are destined to become a part of plasma membrane or to be secreted from the cell, have carbohydrate chains attached to the amide nitrogen of asparagine(N linked) or the hydroxyl groups of serine, threonine(O linked). N glycosylation occurs in ER and O glycosylation occurs in the Golgi Complex.
  • 9.
  • 10. Sulfation: Sulfate modification takes place by the addition of sulphate molecules and these modifications of proteins occurs at tyrosine residues. Tyrosine sulfation accomplished via the activity of tyrosyl protein sulfotransferases (TPST) which are membrane associated enzymes of trans-Golgi network. There are two known TPSTs. 1. TPST-1 2. TPST-2 The universal phosphate donor is 3’-phosphoadenosyl-5’-phosphosulphate (PSPA).
  • 11.
  • 12. Methylation: The transfer of one-carbon methyl groups to nitrogen or oxygen to amino acid side chains increases the hydrophobicity of the protein and can neutralize a negative amino acid charge when bound to carboxylic acids. Methylation is mediated by methyl transferases and S-adenosyl methionine (SAM) is the primary methyl group donor.
  • 13.
  • 14. Hydroxylation: The biological process of addition of a hydroxy group to a protein amino acid is called Hydroxylation. Protein hydroxylation is one type of PTM that involves the conversion of –CH group into –COH group and these hydroxylated amino acids are involved in the regulation of some important factors called transcription factors. Among 20, the two amino acids can be regulated these are proline and lysine.
  • 15.
  • 16. Protein Degradation: Proteins that are defective for example, misfolded or destined for rapid turnover are often marked for destruction by ubi ubiquitination-the attachment of chains of a small, highly conserved protein, called ubiquitin. Proteins marked in this way are rapidly degraded by a cellular component known as the proteasome, which is a macromolecular, ATP-dependent, proteolytic system located in the cytosol.
  • 17. Protein Folding: Proteins must fold to assume their functional state. Folding can be spontaneous or facilitated by proteins known as Chaperones.