How can I publish a research paper for free?

On Researchia, you can publish research papers, preprints, and science projects instantly and for free — no paywall and no submission fee. Create a free account, go to Explorer, and click "Publish Instantly" to share your work with a global audience.

Where can I find trending research papers?

Researchia Explorer aggregates the latest and most-discussed research papers across AI, Biology, Physics, Engineering, and more. New papers are added daily and ranked by community engagement.

What is a good free alternative to ResearchGate for publishing papers?

Researchia is a free, modern alternative to ResearchGate. You can publish papers instantly, connect with researchers, collaborate on projects, and access an open library of 200M+ scientific records — all without paywalls.

Research PaperResearchia:202604.21021

Geometric coherence of single-cell CRISPR perturbations reveals regulatory architecture and predicts cellular stress

Prashant C. Raju

Abstract

Genome engineering has achieved remarkable sequence-level precision, yet predicting the transcriptomic state that a cell will occupy after perturbation remains an open problem. Single-cell CRISPR screens measure how far cells move from their unperturbed state, but this effect magnitude ignores a fundamental question: do the cells move together? Two perturbations with identical magnitude can produce qualitatively different outcomes if one drives cells coherently along a shared trajectory while th...

Submitted: April 21, 2026Subjects: Biology; Biotechnology

Description / Details

Genome engineering has achieved remarkable sequence-level precision, yet predicting the transcriptomic state that a cell will occupy after perturbation remains an open problem. Single-cell CRISPR screens measure how far cells move from their unperturbed state, but this effect magnitude ignores a fundamental question: do the cells move together? Two perturbations with identical magnitude can produce qualitatively different outcomes if one drives cells coherently along a shared trajectory while the other scatters them across expression space. We introduce a geometric stability metric, Shesha, that quantifies the directional coherence of single-cell perturbation responses as the mean cosine similarity between individual cell shift vectors and the mean perturbation direction. Across five CRISPR datasets (2,200+ perturbations spanning CRISPRa, CRISPRi, and pooled screens), stability correlates strongly with effect magnitude (Spearman $ρ=0.75-0.97$ ), with a calibrated cross-dataset correlation of 0.97. Crucially, discordant cases where the two metrics decouple expose regulatory architecture: pleiotropic master regulators such as CEBPA and GATA1 pay a "geometric tax," producing large but incoherent shifts, while lineage-specific factors such as KLF1 produce tightly coordinated responses. After controlling for magnitude, geometric instability is independently associated with elevated chaperone activation (HSPA5/BiP; $ρ_{partial}=-0.34$ and $-0.21$ across datasets), and the high-stability/high-stress quadrant is systematically depleted. The magnitude-stability relationship persists in scGPT foundation model embeddings, confirming it is a property of biological state space rather than linear projection. Perturbation stability provides a complementary axis for hit prioritization in screens, phenotypic quality control in cell manufacturing, and evaluation of in silico perturbation predictions.

Source: arXiv:2604.16642v1 - http://arxiv.org/abs/2604.16642v1 PDF: https://arxiv.org/pdf/2604.16642v1 Original Link: http://arxiv.org/abs/2604.16642v1

Please sign in to join the discussion.

No comments yet. Be the first to share your thoughts!