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go vs pralsetinib

Mechanistic comparison of go 6976 and pralsetinib based on molecular target overlap from BindingDB and ChEMBL binding affinity data.

2
Shared Targets
15%
Jaccard Similarity
13%
IDF-Weighted Similarity
Jaccard measures raw target overlap. IDF-weighted downweights promiscuous hub targets (e.g. CYP enzymes) that bind many compounds non-specifically.

Evidence Comparison

go 6976
โ€”
Evidence Score
0
PubMed Studies
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pralsetinib
โ€”
Evidence Score
0
PubMed Studies
View full profile โ†’

Target Overlap

go and pralsetinib share 2 molecular targets based on binding affinity data from BindingDB (Kd/IC50 โ‰ค 10 ยตM) and ChEMBL. A Jaccard index of 0.154 means 15% of the combined target set is bound by both compounds. The IDF-weighted score of 0.126 accounts for non-specific binding to metabolic enzymes.

Note: High target overlap does not imply identical mechanism or therapeutic equivalence. Binding affinity, tissue distribution, bioavailability, and downstream signaling differ significantly between compounds even when they bind the same protein.

Frequently Asked Questions

What do go and pralsetinib have in common?
go and pralsetinib share 2 molecular targets with a Jaccard similarity of 15%. Both bind overlapping sets of proteins based on BindingDB and ChEMBL binding affinity data.
Can go and pralsetinib be combined?
go and pralsetinib share 2 molecular targets, suggesting potential pathway overlap. Combination use should be evaluated with a qualified healthcare professional. BiohacksAI does not provide medical advice.
Which has more research: go or pralsetinib?
In the BiohacksAI corpus: go has 0 PubMed-indexed studies, pralsetinib has 0 studies.

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