Download Document

Survey
yes no Was this document useful for you?
   Thank you for your participation!

* Your assessment is very important for improving the work of artificial intelligence, which forms the content of this project

page
1
page
2
page
3
page
4
page
5
page
6
page
7
page
8
page
9
page
10
page
11
page
12
page
13
page
14
page
15
page
16
page
17
page
18
page
19
page
20
page
21
page
22
page
23
page
24
page
25
page
26
page
27
page
28
page
29
Document related concepts
no text concepts found
Transcript 
Protein Folding of
A Biopharmaceutical — hCD83
Lin Zhang
Chemical Engineering
Department
Biopharmaceuticals
Proteins
In use:
Insulin
Potential use:
tPA
Human CD83
Outlines

Backgrounds of hCD83

Preliminary Results and Discussion
Human CD83 (hCD83)

Human CD83 is expressed predominantly on
the surface of dendritic cells (DCs)

DCs are the most potent antigen presenting
cells of the immune system

Glycoprotein CD83 is one of the best-known
maturation markers for human DCs
Backgrounds
hCD83
Argos
DC Bio
Preclinical Trial
Production
Backgrounds
Insulin
Backgrounds
What we are interested in:



Dynamic process of protein folding
Protein Aggregation
3D Structure
Backgrounds
FDA Approval
3D Structure
Crystallography
3D Structure Prediction Flowchart
Target Sequence
Conserved Domain
Ⅰ
Yes
No
Homologous
in PDB
Secondary
Structure
Comparative
Modeling
Comparison
Tertiary
Structure
Ⅱ
Preliminary Results
Descriptions
Database Searching
Protein-Protein Blast
Preliminary Results
Preliminary Results
1MCP_H


Class: All beta proteins
Fold: Immunoglobulin-like
beta-sandwich
sandwich; 7 strands in 2 sheets;
greek-key
some members of the fold have
additional strands
1GL4_B


Class: All beta proteins
Fold: Immunoglobulin-like
beta-sandwich
sandwich; 7 strands in 2 sheets;
greek-key
some members of the fold have
additional strands

Superfamily: Immunoglobulin
(IG)

Superfamily: Immunoglobulin
(IG)

Family: V set domains
(antibody variable domain-like)

Family: I set domains
Preliminary Results
Protein fold recognition
1nez_g
Phyre
Preliminary Results
Ⅰ Comparative Modeling
Swiss-Model
RAPTOR
Preliminary Results
Swiss-Model
1MCP_H
(7~121)
Preliminary Results
Swiss-Model
1a6w_L
Discussion
Common
Discussion
Differences
1MCP_H
1α-helix
e
f
Discussion
Differences
1a6w_L
b
c
e
f
2α-helices
Preliminary Results
RAPTOR
1a49_a
Preliminary Results
1a49_a
1 α-helix:
e
f : Thr(83)~Ser(87)
Preliminary Results
Ⅱ Secondary Structure and Tertiary Structure
Secondary Structure: PHD and Jnet
Tertiary Structure :
HMMSTR
Preliminary Results
PHD
Preliminary Results
Jnet
Discussion
Secondary Structure
PHD: 6 β-strands, no α-helix, not to be globular protein
V(8)~V(10), D(17)~C(20), V(32)~K(36), S(76)~N(81),
T(89)~L(94), V(107)~T(112)
Jnet: 8 β-strands, no α-helix
V(8)~C(12), D(15)~T(21), T(31)~K(36), E(43)~T(47)
N(64)~D(68), Y(75)~N(81), T(89)~Q(95), G(104)~T(112)
Preliminary Results
HMMSTR
Discussion
HMMSTR
3 α- helices:
Asp(98)~Asn(102)
Pro(115)~Arg (118)
Lys(119)~Ile(130)
Discussion
Comparison
A. Fold Pattern
Comparative Modeling: distinguished hydrophobic
core and hydrophilic side,
regular, tight
HMMSTR: irregular, loose pattern, no related motif
Discussion
Comparison
B. Composition
Comparative Modeling: more beta-strands and loops
as well as hydrogen bonds
HMMSTR: less beta-strands, loops and hydrogen bonds
Related documents