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Molecular Imaging

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Biodistribution of Protein Drugs Origin of Peptide Pharmaceuticals Therapy using protein hormones dates back to the 1920s Due to the Genomics Revolution cir. 1980 ... – PowerPoint PPT presentation

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Title: Molecular Imaging


1
Biodistribution of Protein Drugs
2
Origin of Peptide Pharmaceuticals
  • Therapy using protein hormones dates back to the
    1920s
  • Due to the Genomics Revolution cir.
    1980-199015-17 other proteins became serious
    candidates for therapy14
  • Specificity

3
Cetuximab (Erbitux) bound to EGFR
Trastuzumab (Herceptin) bound to HER-2
pertuzumab
SR Hubbard Cell 2005
4
Pharmacokinetics Biodistribution
  • Biodistribution is a term favored by researchers
  • Pharmacokinetics is a term favored by clinicians
  • Distribution,
  • Metabolism,
  • Elimination

5
Monitoring Biodistribution
  • Radioactivity (99Tc, 123/131I, 161Tb, 88/90Y,
    111In)
  • Immunohistochemistry
  • Magnetic Resonance Imaging
  • Fluorescence
  • Radiation toxicity can occur months or years
    after administration
  • The action of pharmaceuticals is drastically
    reduced by unfavorable pharmacokinetics
  • Many peptide imaging molecules are directed at
    specific structures

6
Factors Influencing Biodistribution
  • Specific interactions
  • Nonspecific interactions
  • Tissue Perfusion

7
Tissue Perfusion
Organ O2 Delivery ml/min/100 g tissue Blood Flow Rate ml/min/100 g O2 Consumption ml/min/100 g O2 Consumption/O2 Delivery ()
Brain 10.8 54 3.7 34
Heart 16.8 87 11.0 65
Skel. Musc. 0.5 2.7 0.18 34
Liver 11.6 58 2.2 18
Kidney 84 420 6.8 8
GM Coritsidis, MD State U of NY, Stony Brook
University Hospital and Medical Center Department
of Medicine Division of Nephrology
8
Blood Brain barrier
  • 0.5 kDa molecular mass cutoff

http//www.satori-5.co.uk/word_articles/mcs/engagi
ng_with_mcs.html
9
Circulating Proteases
10
Reticuloendothelial System
11
Immunogenicity can be reduced by humanization
  • Utilizing human sequences for all CH and the CL
    results in a chimeric antibody
  • Humanization Utilizing a completely human
    antibody with only the CDR of a mouse antibody
    results

12
The Liver
Racanelli V and Rehermann B, Hepatology 2006
13
  • The only way to lower the liver uptake of
    radiolabled peptides is to co-administer the same
    peptide that lacks the radiometal to cause
    competition.
  • Beatty BG, O'Conner-Tressel M, Do T, Paxton RJ,
    Beatty JD Cancer Res. 1990 Feb 150(3
    Suppl)846s-851s

14
The Kidney
  • 1-5 total bodyweight24
  • 25 total Cardiac Output24
  • Filtration, Reabsorption Secretion

15
Bohrer, et al in Journal of Chemical
Investigation (1978)
  • The kidney is more efficient at eliminating
    positively charged solutes than negatively
    charged solutes.
  • When the glomerular filtration barrier is
    disrupted, this difference is abolished

http//www.uhmc.sunysb.edu/internalmed/nephro/webp
ages/Part_A.htm
16
Albumin distribution gives insight to renal
processing of proteins
  • Less than 100 mg/ dL Albumin is in the urine 20
  • albumin is 220-320mg/dL in ultrafiltrate20
  • Albumin binds to the apical membrane of proximal
    tubule cells with Kd app 100-300 nM (97-20mg/L)
    20

http//www.uhmc.sunysb.edu/internalmed/nephro/webp
ages/Part_A.htm
17
Albumin Destruction in the Kidney
M Abbate G Remuzzi Am J of Kidney Diseases
(2001)
18
A Closer Look at Megalin and Cubulin
  • Megalin (517 kDa)
  • Necessary for peptide scavenging in the kidney
    22
  • Cubilin (460 kDa glycoprotein)
  • 0.63 ?M Kd for albumin 19
  • In cubulin deficient dogs the albumin excretion
    rate increases by a factor of ten or more 20
  • Can be purified using albumin columns 19
  • 27 ligand bindin domains!26
  • Christensen, et al Pediat Nephrol 2003

19
Megalin and Cubulin are nonspecific
  • In concious rats, lysozyme, cytochrome c, and
    ß2-macroglobulin compete for uptake in proximal
    tubules 25
  • Cubulin binds to light chains 26, megalin does
    so with a higher affinity 28
  • Tamm-Horsfall protein may be involved in protein
    re-absorption and destruction 27

20
Increasing the negative charge density of an
octreotide reduces renal accumulation
  • RH
  • RCOOH

21
Isoelectric Point and Pharmacokinetics
H Kobayashi et al 1999 Cancer Research
22
Fab and F(ab)2
MT micromet/MedimmuneTM MT-103
pim.medicine.dal.ca/images/atb-2.jpg
23
Isoelectric Point and Pharmacokinetics
Biodistribution of an sa-glyco-Fab (black), an
ma-glyco-Fab (checkered), an mc-glyco-Fab
(dotted), and a non-glyco-Fab (striped) at 15
(A), 45 (B), and 180 (C) minutes after injection
H Kobayashi et al 1999 Cancer Research
24
Isoelectric Point and Pharmacokinetics
H Kobayashi et al 1999 Cancer Research
25
Isoelectric Point and Pharmacokinetics
  • The decreased negative charge probably causes an
    unfavorable interaction with the filtration
    barrier in the glomerulus.

26
Effects of Isoelectric Point and
Co-administration of Lysine
The more negative Fab did not accumulate in the
kidney as well The administration of Lysine can
allow for easier elimination
H Kobayashi et al 1999 Cancer Research
27
Co-administration of Basic Amino Acids
28
Co-administration of Basic Amino Acids
  • Cationic amino acids diminish kidney uptake of
    Fab and F(ab)2 fragments 30
  • Lysine ethyl ester was more potent than lysine
    30
  • D-Lysine and L-lysine are equally effective ip or
    orally
  • D-glucosamine was also effective

Corroborated by PJ Hammond et al Br J Cancer
1993 MV Pim Eur J Nucl Med 1994 TM Behr Cancer
Res 1995
29
PEGylation
FM Veronese G Pasut, Drug Discovery Today 2005
30
Pharmacokinetics of PEGylated IFN a-2a
  • 1 out of 10 animals tested produced an anti
    PEG2-IFN antibody
  • 10 out of 10 animals tested produced and anti IFN
    a-2a
  • PEGylation drastically prolonged serum activity

P Bailon et al, Bioconjugate Chem 2001
31
Biodistribution and Pharmacokinetics of PEGylated
proteins
  • Pegfilgrastim - selectively PEGylated at the
    N-terminal 31
  • Cysteine, Lysine, and N-terminal PEGylating
    moieties available 31
  • PEGylation may extend circulation time to a full
    week

32
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33
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34
N-acetylation and Modification of Basic Residues
  • This method risks enhancing the immunogenicity of
    humanised peptides

JP Tarburton J Biol Response Mod 1990
35
Summary
  • By far, the major point of difficulty for protein
    pharmaceuticals is the kidney.
  • Renal accumulation is almost certainly a result
    of megalin and cubulin activity.
  • In addition to size/effective radius, the
    isoelectric point of a protein influences its
    circulation time, with more positive proteins
    filtered easier.
  • Accumulation in the proximal convoluted tubule
    seems to be hindered by co-administration of
    lysine or other aminated molecules
  • The liver, spleen, and lymphatic tissues are apt
    to metabolize circulating proteins, even those
    that are not immunogenic.
  • PEGylation, and pI adjustments are valid means of
    altering filtration at the glomerulus.

36
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37
Biodistribution of Protein Drugs
38
The Danger of Her-2 Overexpression
  • The HER-2 is locked in the dimerization-competent
    conformation, making it the preferred
    homodimerization partner for all other HERs.

39
Limitations
SGMIB pI 8.1-8.5 SIPC pI 7.4-7.8 SIPMB pI
5.8-6.5
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