EEIG2

EEIG family member 2 · UniProt Q5T8I3

Length: 360 aa
Mass: 39.3 kDa
Annotated: 2026-06-09

4 papers in source corpus 2 papers cited in narrative 2 extracted findings

Cross-family judge faithfulness: 2/2 claims corpus-supported (100%)

Mechanistic narrative

Synthesis pass · prose summary of the discoveries below

EEIG2 (FAM102B) functions as an adaptor protein at ER–plasma membrane contact sites, where it mediates recruitment of the bridge-like lipid transfer protein BLTP2 to the plasma membrane alongside phosphoinositides and N-BAR domain proteins (PMID:40899996). Through this interaction, EEIG2 contributes to ER tethering to the plasma membrane, supporting membrane contact at sites of bulk lipid transport (PMID:40899996). Beyond its role as a BLTP2 adaptor at these contact sites, no further mechanistic detail for EEIG2 has been characterized in the available corpus.

Mechanistic history

Synthesis pass · year-by-year structured walk · 2 steps

2025 Medium
Whether FAM102B/EEIG2 had a defined molecular role was unknown; identifying it as a BLTP2 binding partner at ER-PM contacts established it as an adaptor coupling a bridge-like lipid transfer protein to the plasma membrane.

Evidence Interaction mapping and localization in cell-based systems, with loss-of-function showing PM-connected intracellular vacuole accumulation (peer-reviewed)

PMID:40899996
Open questions at the time
- No orthogonal validation (mutagenesis or reconstitution) for the FAM102B-BLTP2 interaction specifically
- Vacuole accumulation phenotype attributed to BLTP2 loss, not directly to FAM102B loss
- Mechanism by which FAM102B engages the PM (lipid vs protein determinants) not defined
2025 Medium
The preprint extended the adaptor model by placing FAM102B-mediated BLTP2 tethering at tubular endosomes continuous with the PM and at macropinosomes fusing with the PM, broadening the membrane contexts where it operates.

Evidence Interaction mapping and localization in cell-based systems (preprint)

PMID:39974967
Open questions at the time
- Preprint without detailed orthogonal validation for FAM102B
- Direct demonstration of lipid transport dependence on FAM102B not shown
- Stoichiometry and structural basis of the BLTP2 interaction unresolved

Open questions

Synthesis pass · forward-looking unresolved questions

How FAM102B selects and stabilizes specific contact-site geometries, and whether its adaptor function is required for bulk lipid transport itself, remains open.
No direct loss-of-function phenotype attributed specifically to FAM102B
No structural or biochemical reconstitution of the FAM102B-BLTP2-PM assembly
Physiological consequences of FAM102B loss at the organism level uncharacterized

Mechanism profile

Synthesis pass · controlled-vocabulary classification · explore literature graph →

Molecular activity

GO:0060090 molecular adaptor activity 1

Localization

GO:0005783 endoplasmic reticulum 1 GO:0005886 plasma membrane 1

Pathway

R-HSA-1430728 Metabolism 1

Partners

BLTP2

Evidence

Reading pass · 2 per-paper findings extracted from the source corpus

Year	Finding	Method	Journal	Conf	PMIDs
2025	FAM102B (EEIG2) acts as an adaptor protein that mediates binding of the bridge-like lipid transfer protein BLTP2 to the plasma membrane at ER-PM contact sites, alongside phosphoinositides and N-BAR domain proteins.	Interaction mapping / localization studies identifying FAM102B as a binding partner of BLTP2 at ER-PM contacts; loss-of-function showing accumulation of intracellular vacuoles connected to the PM.	The Journal of cell biology	Medium	40899996
2025	FAM102B (EEIG2) acts as an adaptor protein that mediates binding of BLTP2 to the plasma membrane at ER-PM contact sites, contributing to ER tethering at tubular endosomes that become continuous with the PM and at macropinosomes fusing with the PM.	Interaction mapping and localization studies in cell-based systems identifying FAM102B as a BLTP2 binding partner at membrane contact sites (preprint version of the peer-reviewed paper).	bioRxivpreprint	Medium	39974967

Source papers

Stage 0 corpus · 4 papers · ranked by NIH iCite citations

Year	Title	Journal	Citations	PMID
2019	Predicting drug-free remission in rheumatoid arthritis: A prospective interventional cohort study.	Journal of autoimmunity	45	31280933
2025	Multiple interactions recruit BLTP2 to ER-PM contacts to control plasma membrane dynamics.	The Journal of cell biology	6	40899996
2025	Multiple interactions mediate the localization of BLTP2 at ER-PM contacts to control plasma membrane dynamics.	bioRxiv : the preprint server for biology	1	39974967
2025	Population Cohort-Validated PM2.5-Induced Gene Signatures: A Machine Learning Approach to Individual Exposure Prediction.	Toxics	1	40711007

DepMap portal ↗

Not essential

Human Protein Atlas profile ↗

Subcell. Nucleoli Cytosol

RNA spec. Low tissue specificity

AlphaFold structure ↗

pLDDT 70

Domains 2.60.40.150 -

Sources data + JSON

JSON record ↗ UniProt ↗ PubMed ↗

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