Transcriptional advantage influence odorant receptor gene choice

Author:

Mohanty Sanjay Kumar1ORCID,Maryam Sidrah1,Gautam Vishakha1,Mittal Aayushi1,Gupta Krishan2ORCID,Arora Radhika1,Bhadra Wrik1,Mishra Tripti3,Sengupta Debarka12,Ahuja Gaurav1ORCID

Affiliation:

1. Indraprastha Institute of Information Technology-Delhi (IIIT-Delhi) Department of Computational Biology, , Okhla, Phase III, New Delhi 110020, India

2. Indraprastha Institute of Information Technology-Delhi (IIIT-Delhi) Department of Computer Science and Engineering, , Okhla, Phase III, New Delhi 110020, India

3. Pathfinder Research and Training Foundation , Uttar Pradesh 201308, India

Abstract

Abstract Odorant receptors (ORs) obey mutual exclusivity and monoallelic mode of expression. Efforts are ongoing to decipher the molecular mechanism that drives the ‘one-neuron-one-receptor’ rule of olfaction. Recently, single-cell profiling of olfactory sensory neurons (OSNs) revealed the expression of multiple ORs in the immature neurons, suggesting that the OR gene choice mechanism is much more complex than previously described by the silence-all-and-activate-one model. These results also led to the genesis of two possible mechanistic models i.e. winner-takes-all and stochastic selection. We developed Reverse Cell Tracking (RCT), a novel computational framework that facilitates OR-guided cellular backtracking by leveraging Uniform Manifold Approximation and Projection embeddings from RNA Velocity Workflow. RCT-based trajectory backtracking, coupled with statistical analysis, revealed the OR gene choice bias for the transcriptionally advanced (highest expressed) OR during neuronal differentiation. Interestingly, the observed selection bias was uniform for all ORs across different spatial zones or their relative expression within the olfactory organ. We validated these findings on independent datasets and further confirmed that the OR gene selection may be regulated by Upf3b. Lastly, our RNA dynamics-based tracking of the differentiation cascade revealed a transition cell state that harbors mixed molecular identities of immature and mature OSNs, and their relative abundance is regulated by Upf3b.

Funder

INSPIRE faculty grant

IHUB Anubhuti

Start-Up Research Grant

Ramalingaswami Re-entry Fellowship

Publisher

Oxford University Press (OUP)

Subject

Genetics,Molecular Biology,Biochemistry,General Medicine

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