Alternative Splicing And Global Transcriptome Changes Associated With LPS Stimulation In Human Peripheral Blood Mononuclear Cells

Esther Chavez-Iglesias
Anatol Sucher
Nidhi Thati
Julia Trudeau
Sue Yom
Marina Sirota
Adam Olshen
Nam Woo Cho
Kord M. Kober

Read the full article

Discuss this preprint

Start a discussion What are Sciety discussions?

Listed in

This article is not in any list yet, why not save it to one of your lists.

Abstract

Introduction

Lipopolysaccharide (LPS), a major component of gram-negative bacterial cell walls, elicits strong innate immune activation and is a widely used model for studying inflammatory responses. While the transcriptional response to LPS stimulation has been characterized, the role of alternative splicing (AS) in modulating this response remains largely unexplored.

Methods

Using deep RNA sequencing of Peripheral Blood Mononuclear Cells from three healthy female donors, we evaluated transcriptome-wide differential gene expression and alternative splicing in response to LPS stimulation.

Results

Our global differential gene expression and pathway impact analyses identified 490 differentially expressed genes and 46 significantly perturbed KEGG pathways, recapitulating known LPS-induced inflammatory responses and identifying two novel signaling pathways, (e.g., SNARE interactions in vesicular transport and the mRNA surveillance pathways). Differential alternative splicing analysis revealed critical impacts on immune-related pathways, including Toll-like receptor signaling, PI3K/AKT signaling, and pro-inflammatory macrophage polarization. Notably, we identified alternative splicing events in genes such as MyD88 and TLR4 , which play key roles in terminating inflammatory signaling, as well as splicing of long non-coding RNAs (e.g., MALAT1 , PVT1 ) with potential regulatory functions in immune responses.

Discussion

This study is the first transcriptome-wide characterization of alternative splicing in response to LPS stimulation in PBMCs. Our findings suggest that alternative splicing is a fundamental regulatory mechanism in the inflammatory response and provides potential targets for therapeutic intervention in immune-related conditions.

Version published to 10.1101/2025.11.09.687437 on bioRxiv
Nov 10, 2025

Neutrophil Transcriptomics in SLE: Exploring Intrinsic, Ex Vivo Adaptation, and CAR T-Cell Therapy-Induced Changes

This article has 9 authors:
1. Ehsan Dehdashtian
2. Guangnan Hu
3. Leah Whiteman
4. Md Tanimul Islam
5. Stefania Gallucci
6. Manuel Garber
7. Dominic Borie
8. Georg Schett
9. Roberto Caricchio
This article has no evaluationsLatest version Nov 5, 2025
Exploring the mechanism of bacterial lipopolysaccharide-related genes involved in polycystic ovary syndrome and its significance in diagnosis

This article has 7 authors:
1. Yang Li
2. Chunmei Bai
3. Xumin Zhang
4. Haixia Song
5. Caixia Yuan
6. Ziwei Huang
7. Jianrong Liu
This article has no evaluationsLatest version Oct 30, 2025
Integrative Multi-Omics Identifies CDK1 as a Key Signaling Regulator of CD4 ⁺ T Cell Effector Function

This article has 11 authors:
1. Nila H. Servaas
2. Hanke Gwendolyn Bauersachs
3. Luisa Abreu
4. Annique Claringbould
5. Ivan Berest
6. Jennifer J. Schwarz
7. Frank Stein
8. Maria Fälth-Savitski
9. Lena Eismann
10. James P. Reddington
11. Judith B. Zaugg
This article has no evaluationsLatest version Oct 31, 2025

Discuss this preprint

Listed in

Abstract

Introduction

Methods

Results

Discussion

Article activity feed

Related articles

Neutrophil Transcriptomics in SLE: Exploring Intrinsic, Ex Vivo Adaptation, and CAR T-Cell Therapy-Induced Changes

Exploring the mechanism of bacterial lipopolysaccharide-related genes involved in polycystic ovary syndrome and its significance in diagnosis

Integrative Multi-Omics Identifies CDK1 as a Key Signaling Regulator of CD4 + T Cell Effector Function

Integrative Multi-Omics Identifies CDK1 as a Key Signaling Regulator of CD4 ⁺ T Cell Effector Function