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Integrating i and
in vitro data to identify
putative thyrotropin-
releasing hormone
receptor ligands
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ACS 2020 Fall Meeting
Mahmoud Shobair, PhD Post Doctoral Fellow
L I. S. Environmental
Research Triangle Park, NC
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Disclaimer: The views expressed in this presentation are those of the authors and do not necessarily reflect the views or policies of the U.S. EPA. presentation does not represent EPA policy.
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High-throughput screening (HTS) in risk assessment
K-4K cmpds
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ToxCast WIWW
Tox21
Data
Models
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How many environmentally-relevant chemicals interact
with the thyrotropin-releasing hormone receptor (TRHR)?
Molecular If a chemical interacts with TRHR, it Experimental approach
initiating may disrupt thyroid
event (MIE) production.
A*
Are all hits reliable?
Are we missing important hits?
How can we increase confidence in results?
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Tox21_TRHR Assay Design
Thyrotropin-releasing
BEB1
Hypothesis: Tox21 TRHR assay m
the receptor (TRHR) response to its specific ligand (TRH).
Steps l-IV can influence hit interpretation
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Tox21_TRHR Agonist & Antagonist Actives
Tox21_TRHR
(~ 8000 total
screened)
160
antagonist
388 Total
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Problem Statement & Approach
Tox21_TRHR assay provides an indirect measure of potential TRHR
activity
Large number of diverse environmental chemicals screened, yet
false negatives and positives are expected
Goal is to identify subset of likeliest true actives from the full set of
assay results
Approach is to prioritize subset of actives (true hits) and inactives
(potential false negatives) for follow-up testing using:
> domain knowledge
> chemotype enrichments
> in silico computational chemistry
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Examples of most active Tox21_TRHR actives
Maximum AUC by
chemical is the area
under the curve-fit
from the ToxCast
Pipeline, and
compresses potency
and efficacy into a
single metric.
TRH
Allyl alcohol
Proflavin hydrochloride
Digitonin
Rhodamine 6G
2-Chloro-1,4-diaminobenzene sulfate
Fluorescein 5(6)-isothiocyanate
Riboflavin
Eosin
2,,4',5',7,-Tetrabromofluorescein
4',5'-Dibromofluorescein
Fluorescein sodium
Fluorescein
]+ Ctrl
Some active substances may be due
to assay interference from auto-
fluorescence.
Fluorescent
0 100 200 300 400
max(AUC)
500 600 700
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Privileged scaffolds from chemotype enrichment analysis
chain:alkaneLinear_stearyl_C18
group:carbohydrate_hexopyranose_generic
atom:element_metal_transistion_metal
r i n g: f u sed_ste ro i d_g e n e r i c_[5_6_6_6]
group:ligand_path_5_bidentate_propandiamine
bond:CS_sulfide_dialkyl
bond:CN amine ter-N aromatic
o
10 15 20 25
# antagonists
30
^7""'
I" Hg2+1"
h3c
35 40 45 phenothiazines
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Filtering potential sources of false positive hits
structure-based Detection technology
chemotype enrichment interference
heuristic, Non-specific
literature support Ca2+ response
domain knowledge
derived from 2D filters
reference db
4
??
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Binding reference dataset and modeling
Data cur
10 Journal articles
Patents
BindingDB
Reference dat
binding data to:
- Eliminate
binders wit
- Train models
3D pharmacop
features
r 115 unique ~
structures
Data mining
r i
association rules
& activity
l values R
3D mode
\
pharmacophore
models
L J
(76) Binders rings with > 3 rings
(16) Non-binders with > 3 rings
(23) Non-binders with < 3 rings
(0) Binders with < 3 rings)
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Binding reference dataset: structural diversity
Ki or IC50
0.01 -300 uM
1. Analogs to the natural TRHR ligand
bond:C(=0)N_carboxamide_generic (75)
2. Heterocyclic compound
ring:hetero_[6]_Z_generic (31) .
4
N*
O.
o
"NH
3. Benzodiazepine-like structures
ring:hetero_[6_7]_N_benzodiazepine_(1_4-) (7)
h2n^
o o
Mil'
11
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Filtering potential sources of false positive hits
structure-based
chemotype enrichment
heuristic,
literature support
388 hits
Detection technology
interference
Non-specific
Ca2+ response
domain kno
derived
reference
2D filters
4
140 filtered hits
~ -8
Hg
2+
~ -26
HO Y 0H
~ -208
sOH
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Pharmacophore modeling
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Generation of 3D
conformations
Molecular alignment of
binders
MOE
J
r ^
Generation & validation
of pharmacophore
models
l. j
C3
O
.to
D
U
Qj
v -Cl
u
o
Q. Qj
^ to
Qj
Querying structure
database
Analysis of model
results
mol
~F
A
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&
$¦
A
i
ti
%
rmsd
0.4799
0.2784
0.2636
0.5092
0.2334
0.3147
0.4857
0.2842
0.3047
0.3550
0.2474
0.3806
0.3041
0.2422
0.2404
0.2885
0.4383
0.5112
0.2485
0-13482
F5:Hyd
F3:Aro|Hyd
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Prioritizing active hits
388 hits
140 filtered hits
MODERATE
HIGH
[TRH model, benzo model 1, benzo model 2, mixed model 1 , mixed model 2
[0, 1, 0, 1, 0, 1, 1, 0, 1, 0, 0, 0, 0, 0, 1]
Concordance:
Models
Assay &
Expert
MODERATE:
at least one +
model
quality check
14
Flurazepam
F3:Aro|Hyd
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Predicted TRHR inhibitor: PK-11195 (Moderate binder)
3D Modeling yields plausible
results in the dru
DTXSID7041097
isoquinoline carboxamide binds selectively to
the peripheral benzodiazepine receptor (PBR)
Midazolam, known TRHR binder
PK-11195 aligned
to Midazolam
DTXSID8047846
15
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Moderate-plausibility assay active: Chlorophacinone
Chlorophacinone has structural features
associated with Benzodiazepine inhibition
ofTRHR [ hit in 5 models]
TRHR antagonist
DTXSID1023071
DTXSID2032348
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High-plausibility assay active
TRH
F5:Hyd
F3:Aro|Hyd
Saquinavir mesylate
Saquinavir mesylate
DTXSID9023835
17
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Newly identified TRHR candidate modulators from actives
Benzodiazepine
Known TRHR
competitive
(midazolam),
assay active
/^New atypical Benzodiazepine Opioid antagonist
Does not bind GABA receptor,
inhibits peptide receptor (CCK)
Unclear,
further inqu
18
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Identifying false negatives
7872 chemicals
2D filter
> 2 rings
<0
1553 structures
for 3D modeling
Diverse
structures
(27) benzodiazepines
(3) peptides
19
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Prioritized peptide-like structures
F5:Hyd
F3:Aro|Hyd
DTXSID8023551
Assay
active
DTXSID4047252
DTXSID8046456
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Predicted Moderate Binders
Structurally diverse
Multi-ring structures
Primarily drugs
O-T^K
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Summary & Conclusions
>50% assay false positive; enriched features associated with artifacts
Multistep prioritization workflow combines
> existing domain knowledge
> in vitro results
> in silico computational chemistry
Integrated approach points to small number of true active candidates in both the
hits and negatives, including a novel benzodiazepine-type structure
A limitation of this work is that the 3D modeling assumes the TRHR binding
pocket in the native conformation.
3D models predict larger set of structurally diverse moderate binders among hits
that are of potential environmental significance, warranting follow-up evaluation
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Summary & Conclusions
Multistep workflow is generalizable and can be applied to other high-throughput
assay results to improve ability to filter out false positives and identify potential
true actives for follow-up screening.
Data
Molecular initiating even
^ Adverse
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Acknowledgements
> Chris Grulke
> Katie Paul Friedman
> Ann Richard
> Daniel Chang
> Ryan Lougee
> Tox21 & ToxCast assay
collaborative group
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