Transcriptomics informed discovery of developmentally essential transcription factors

Gillian Forbes; Pauline Schaap

doi:10.1242/bio.062354

Transcriptomics informed discovery of developmentally essential transcription factors

Gillian Forbes
, Pauline Schaap (Lead / Corresponding author)

Research output: Contribution to journal › Article › peer-review

Abstract

Transcription factors (TFs) regulate cell differentiation in multicellular organisms and were mostly identified by forward genetics in model organisms. However, genomes contain several-fold more TFs without known roles. To classify these orphans, we investigated conservation, cell-type specificity and temporal expression of the ∼290 TFs of Dictyostelia amoebas, which aggregate when starved to form migrating slugs and fruiting bodies consisting of spores and three somatic cell types. Here we deleted seven somatically expressed TF genes and found that four knock-outs were developmentally defective. ariA− lost slug migration and robust fruiting body formation. gtaJ− skipped slug migration and directly developed aggregates into robust fruiting bodies. mybAA− formed multi-tipped aggregates, defective slugs and fruiting bodies with few spores. Hierarchical clustering of the expression profiles of mybAA and 45 other multi-tip suppressing genes grouped mybAA with seven autophagy genes, with similar developmental defects as mybAA−, suggesting that mybAA induces autophagy gene expression. mybM− slugs poorly migrated and fruiting bodies had kinked, rough stalks, but normally expressed cell-type marker genes, indicating defective morphogenesis. Overall, transcriptomics informed TF selection proved useful for gene function discovery.

Original language	English
Article number	bio062354
Number of pages	9
Journal	Biology Open
Volume	14
Issue number	11
DOIs	https://doi.org/10.1242/bio.062354
Publication status	Published - 2 Dec 2025

Keywords

Evolution of soma
ariA
gtaJ
mybAA
mybM
Life cycle choice
Autophagy
Morphogenetic movement
Social amoebas

Access to Document

10.1242/bio.062354Licence: CC BY

Final Published VersionFinal published version, 10.3 MBLicence: CC BY

Evolution of Multicellularity and Somatic Cell Specialisation (EVOSOM)
Schaap, P. (Investigator)
COMMISSION OF THE EUROPEAN COMMUNITIES
1/05/17 → 30/04/23
Project: Research

Cite this

@article{39772b53d41a43738a0190e4bb32ae95,

title = "Transcriptomics informed discovery of developmentally essential transcription factors",

abstract = "Transcription factors (TFs) regulate cell differentiation in multicellular organisms and were mostly identified by forward genetics in model organisms. However, genomes contain several-fold more TFs without known roles. To classify these orphans, we investigated conservation, cell-type specificity and temporal expression of the ∼290 TFs of Dictyostelia amoebas, which aggregate when starved to form migrating slugs and fruiting bodies consisting of spores and three somatic cell types. Here we deleted seven somatically expressed TF genes and found that four knock-outs were developmentally defective. ariA− lost slug migration and robust fruiting body formation. gtaJ− skipped slug migration and directly developed aggregates into robust fruiting bodies. mybAA− formed multi-tipped aggregates, defective slugs and fruiting bodies with few spores. Hierarchical clustering of the expression profiles of mybAA and 45 other multi-tip suppressing genes grouped mybAA with seven autophagy genes, with similar developmental defects as mybAA−, suggesting that mybAA induces autophagy gene expression. mybM− slugs poorly migrated and fruiting bodies had kinked, rough stalks, but normally expressed cell-type marker genes, indicating defective morphogenesis. Overall, transcriptomics informed TF selection proved useful for gene function discovery.",

keywords = "Evolution of soma, ariA, gtaJ, mybAA, mybM, Life cycle choice, Autophagy, Morphogenetic movement, Social amoebas",

author = "Gillian Forbes and Pauline Schaap",

note = "Copyright: {\textcopyright} 2025. Published by The Company of Biologists.",

year = "2025",

month = dec,

day = "2",

doi = "10.1242/bio.062354",

language = "English",

volume = "14",

journal = "Biology Open",

issn = "2046-6390",

publisher = "Company of Biologists",

number = "11",

}

TY - JOUR

T1 - Transcriptomics informed discovery of developmentally essential transcription factors

AU - Forbes, Gillian

AU - Schaap, Pauline

PY - 2025/12/2

Y1 - 2025/12/2

N2 - Transcription factors (TFs) regulate cell differentiation in multicellular organisms and were mostly identified by forward genetics in model organisms. However, genomes contain several-fold more TFs without known roles. To classify these orphans, we investigated conservation, cell-type specificity and temporal expression of the ∼290 TFs of Dictyostelia amoebas, which aggregate when starved to form migrating slugs and fruiting bodies consisting of spores and three somatic cell types. Here we deleted seven somatically expressed TF genes and found that four knock-outs were developmentally defective. ariA− lost slug migration and robust fruiting body formation. gtaJ− skipped slug migration and directly developed aggregates into robust fruiting bodies. mybAA− formed multi-tipped aggregates, defective slugs and fruiting bodies with few spores. Hierarchical clustering of the expression profiles of mybAA and 45 other multi-tip suppressing genes grouped mybAA with seven autophagy genes, with similar developmental defects as mybAA−, suggesting that mybAA induces autophagy gene expression. mybM− slugs poorly migrated and fruiting bodies had kinked, rough stalks, but normally expressed cell-type marker genes, indicating defective morphogenesis. Overall, transcriptomics informed TF selection proved useful for gene function discovery.

AB - Transcription factors (TFs) regulate cell differentiation in multicellular organisms and were mostly identified by forward genetics in model organisms. However, genomes contain several-fold more TFs without known roles. To classify these orphans, we investigated conservation, cell-type specificity and temporal expression of the ∼290 TFs of Dictyostelia amoebas, which aggregate when starved to form migrating slugs and fruiting bodies consisting of spores and three somatic cell types. Here we deleted seven somatically expressed TF genes and found that four knock-outs were developmentally defective. ariA− lost slug migration and robust fruiting body formation. gtaJ− skipped slug migration and directly developed aggregates into robust fruiting bodies. mybAA− formed multi-tipped aggregates, defective slugs and fruiting bodies with few spores. Hierarchical clustering of the expression profiles of mybAA and 45 other multi-tip suppressing genes grouped mybAA with seven autophagy genes, with similar developmental defects as mybAA−, suggesting that mybAA induces autophagy gene expression. mybM− slugs poorly migrated and fruiting bodies had kinked, rough stalks, but normally expressed cell-type marker genes, indicating defective morphogenesis. Overall, transcriptomics informed TF selection proved useful for gene function discovery.

KW - Evolution of soma

KW - ariA

KW - gtaJ

KW - mybAA

KW - mybM

KW - Life cycle choice

KW - Autophagy

KW - Morphogenetic movement

KW - Social amoebas

U2 - 10.1242/bio.062354

DO - 10.1242/bio.062354

M3 - Article

C2 - 41328750

SN - 2046-6390

VL - 14

JO - Biology Open

JF - Biology Open

IS - 11

M1 - bio062354

ER -

Transcriptomics informed discovery of developmentally essential transcription factors

Abstract

Keywords

Access to Document

Fingerprint

Projects

Evolution of Multicellularity and Somatic Cell Specialisation (EVOSOM)

Cite this