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Examen

PH 310 Exam Questions With Verified Answers

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PH 310 Exam Questions With Verified Answers ...

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Institución
PH 310
Grado
PH 310

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Subido en
17 de enero de 2025
Número de páginas
34
Escrito en
2024/2025
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Examen
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PH 310 Exam Questions With
Verified Answers

4 attributes of adaptive immunity - ANSWER 1) specificity

2) memory: remembers, next response quicker

3) amplification: clonal expansion

4) modulation: switching of ab isotypes

primary and secondary response in adaptive immunity - ANSWER primary: lag phase is
1 week, ab number peaks for a few days, then rapidly decreases (predom IgM)

secondary: no lag phase, bigger response/many ab made, response remains high for a
few days (predom IgG and a lil IgM)

third response even stronger

antibody (BCR) basic structure - ANSWER - 4 polypeptide chains: 2 heavy H (50 kDa), 2
light L (25 kDa)

- linked by disulfide bonds

- variable region at N-terminus

- constant regions has c-terminus

Ig are membrane bound form and antibodies are the secreted form --> when bound by
antigens, B-cells differentiates to antibody-secreting plasma cells - ANSWER

plant protease papain cleaves ab into - ANSWER - 2 Fab fragments [fragment antigen
binding] that can still bind antigen

- 1 Fc fragment [fragment crystallizable] that can still opsonize

gut protease pepsin does____ - ANSWER degrades Fc from F(ab)2 fragment --> learned
that Fc on intact ab is important for opsonization

immunoglobulin isotype aka class of antibody - ANSWER genetic variations in the
CONSTANT REGIONS of heavy and light chains; GAMED; variable regions are the same

heavy chain isotypes - ANSWER alpha (IgA), delta (IgD), epsilon (IgE), gamma (IgG), mu
(IgM)

,light chain isotypes - ANSWER kappa and lambda

paratope - ANSWER ag-binding site on the ab; 4 framework regions (FR) have little
variability, 3 hypervariable regions (HV) aka complementary determining regions (CDR)
provide a binding surface for ag

ab tertiary structure - ANSWER constant domains have few loops, variable domains
have many fingerlike loops that can bind ag at antigen binding site

epitopes - ANSWER antigenic region on ag where ab binds; carbohydrates, proteins, or
both; most ag are multivalent

type of bonding of ag-ab - ANSWER weak non-covalent; lock and key model where there
is a complementarity of shape, charge, polarity, hydrophobicity

epitopes bind to - ANSWER pockets, grooves, surfaces

post-translational events - ANSWER - polypeptide glycosylation influences ab-ag
interactions

- proteins for secretion vs insertion into phospholipid bilayer and then presented cell
membrane

immunoglobulin diversity - ANSWER - Ig genes are fragmented in all cells so that they
cannot be expressed EXCEPT for in the B-cell

- consist of gene loci

- called the germline configuration

Recombination activating genes (RAG) enzymes 1 and 2 - ANSWER found only in
lymphocytes in b and t cells and no other body cells

gene segment recombination - ANSWER - Ig constant region genes are ready to
transcribe and don't need to be spliced (but still consist of introns and exons)

- ig variable region genes are coded by V, J, or D gene loci that require RAG-mediated
rearrangement

- the 3rd HV region is coded by a spliced junction between VJ or VDJ, which increases
variable domain diversity

light chain has one recombo event and heavy chain has two (to join DJ and then VDJ) -
ANSWER

Recombination Signal Sequences (RSS) - ANSWER - directs RAG mediated gene
segment recombination

- two types of RSS: heptamer and nonamer

- 12 or 23 bp separate the 7 and 9

,- gene to be cut is always flanked by 7, RAG binds at 12/23 bp sequences and cuts the
heptamer

- gene segments that will join are always flagged by heptamer (cut site)

from igM and igD to the others - ANSWER - naive B-cells express IgM and IgD

- VDJ rearranging triggers tx of full Ig gene, the mRNA is spliced, then translated

- igM and igD heavy chain C regions are transcribed and expressed first REVERSIBLE
PROCESS

allelic exclusion - ANSWER each B-cell produces Ig of only one specificity: once variable
region is rearranged, it is PERMANENT and cannot longer be altered

- ANSWER 1) gene segment recombination

2) allellic exclusion

how Ig goes to the surface - ANSWER - Ig polypeptides enter ER to assemble into Ig
molecules

- hydrophobic *membrane coding (MC)* region if present inserts into membrane
REVERSIBLE PROCESS

- Ig then associates with IgB and IgA transmembrane proteins linked by disulfide bonds,
and these serve to signal the B-cell that has surface Ig

B cell receptor (BCR) - ANSWER surface Ig on a B cell that binds to a specific antigen.

affinity maturation - ANSWER ag bound to ab causes structural changes in the Ig,
attracts IgA and IgB transmembrane proteins, which signals the b-cell to rapidly divide.
will IRREVERSIBLY hypermutate and increases diversity of rearranged gene segments.
over time, ab becomes more specific for the ag

ab isotype switching - ANSWER 1) IgM and IgD are co-expressed on B-cells. IgM
secreted first as a pentamer bc it is transcribed first

3) isotype switching is IRREVERSIBLE DNA recomb that rearranges the same V-region
with other heavy-chain constant genes (loops out)

4) switch to IgG is common.

5) V region is the same for all isotypes but C-regions determine effector functions

IgM secreted form - ANSWER pentamer linked by a J chain

IgD secreted form - ANSWER monomer

IgG secreted form - ANSWER monomer

, IgE secreted form - ANSWER monomer

IgA secreted form - ANSWER dimer linked by J chain. Most common secreted ab in
mucus membranes (guts, eyes) bc J chain can go through the epithelium

heaviest Ig - ANSWER IgM

most common Ig in serum - ANSWER IgG bc it is small and can distribute better

longest half life Ig - ANSWER IgG

shortest half life Ig - ANSWER IgE and few in serum

fewest Ig in serum - ANSWER IgE bc only for allergies

IgM is good at - ANSWER - neutralization

- activation of complement sys

- transport across epithelium

IgD is good at - ANSWER nothing

IgG is good at - ANSWER - neutralization

- opsonization

- some sensitization for killing by NK cells

- some sensitization of mast cells

- activation of complement system

- transport across placenta

- diffusion into extravascular sites

IgA is good at - ANSWER - neutralization

- opsonization

- activation of complement sys

- transport across epithelium

- diffusion into extravascular sites

IgE is good at - ANSWER - sensitization of mast cells

- diffusion into extravascular sites

immunoassay - ANSWER a sensitive analytical test that utilizes highly specific ab-ag
complexes to produce a signal that can be measured and related to concentration of a
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