Identification of a specific APOE transcript and functional elements associated with Alzheimer’s disease

Qiang Chen; Luis Aguirre; Guoming Liang; Huanhuan Zhao; Tao Dong; Felix Borrego; Itziar de Rojas; Qichan Hu; Christopher Reyes; Ling Yan Su; Bao Zhang; James D. Lechleiter; Harald H.H. Göring; Philip L. De Jager; Joel E. Kleinman; Thomas M. Hyde; Pan P. Li; Agustín Ruiz; Daniel R. Weinberger; Sudha Seshadri; Liang Ma

doi:10.1186/s13024-024-00751-7

Identification of a specific APOE transcript and functional elements associated with Alzheimer’s disease

Qiang Chen, Luis Aguirre, Guoming Liang, Huanhuan Zhao, Tao Dong, Felix Borrego, Itziar de Rojas, Qichan Hu, Christopher Reyes, Ling Yan Su, Bao Zhang, James D. Lechleiter, Harald H.H. Göring, Philip L. De Jager, Joel E. Kleinman, Thomas M. Hyde, Pan P. Li, Agustín Ruiz, Daniel R. Weinberger, Sudha SeshadriLiang Ma

Producción científica: Article › revisión exhaustiva

Resumen

Background: The APOE gene is the strongest genetic risk factor for late-onset Alzheimer’s Disease (LOAD). However, the gene regulatory mechanisms at this locus remain incompletely characterized. Methods: To identify novel AD-linked functional elements within the APOE locus, we integrated SNP variants with multi-omics data from human postmortem brains including 2,179 RNA-seq samples from 3 brain regions and two ancestries (European and African), 667 DNA methylation samples, and ChIP-seq samples. Additionally, we plotted the expression trajectory of APOE transcripts in human brains during development. Results: We identified an AD-linked APOE transcript (jxn1.2.2) particularly observed in the dorsolateral prefrontal cortex (DLPFC). The APOE jxn1.2.2 transcript is associated with brain neuropathological features, cognitive impairment, and the presence of the APOE4 allele in DLPFC. We prioritized two independent functional SNPs (rs157580 and rs439401) significantly associated with jxn1.2.2 transcript abundance and DNA methylation levels. These SNPs are located within active chromatin regions and affect brain-related transcription factor-binding affinities. The two SNPs shared effects on the jxn1.2.2 transcript between European and African ethnic groups. Conclusion: The novel APOE functional elements provide potential therapeutic targets with mechanistic insight into the disease etiology.

Idioma original	English (US)
Número de artículo	63
Publicación	Molecular Neurodegeneration
Volumen	19
N.º	1
DOI	https://doi.org/10.1186/s13024-024-00751-7
Estado	Published - dic 2024

ASJC Scopus subject areas

Molecular Biology
Clinical Neurology
Cellular and Molecular Neuroscience

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10.1186/s13024-024-00751-7

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Chen, Q., Aguirre, L., Liang, G., Zhao, H., Dong, T., Borrego, F., de Rojas, I., Hu, Q., Reyes, C., Su, L. Y., Zhang, B., Lechleiter, J. D., Göring, H. H. H., De Jager, P. L., Kleinman, J. E., Hyde, T. M., Li, P. P., Ruiz, A., Weinberger, D. R., ... Ma, L. (2024). Identification of a specific APOE transcript and functional elements associated with Alzheimer’s disease. Molecular Neurodegeneration, 19(1), Artículo 63. https://doi.org/10.1186/s13024-024-00751-7

Chen, Q, Aguirre, L, Liang, G, Zhao, H, Dong, T, Borrego, F, de Rojas, I, Hu, Q, Reyes, C, Su, LY, Zhang, B, Lechleiter, JD, Göring, HHH, De Jager, PL, Kleinman, JE, Hyde, TM, Li, PP, Ruiz, A, Weinberger, DR, Seshadri, S & Ma, L 2024, 'Identification of a specific APOE transcript and functional elements associated with Alzheimer’s disease', Molecular Neurodegeneration, vol. 19, n.º 1, 63. https://doi.org/10.1186/s13024-024-00751-7

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title = "Identification of a specific APOE transcript and functional elements associated with Alzheimer{\textquoteright}s disease",

abstract = "Background: The APOE gene is the strongest genetic risk factor for late-onset Alzheimer{\textquoteright}s Disease (LOAD). However, the gene regulatory mechanisms at this locus remain incompletely characterized. Methods: To identify novel AD-linked functional elements within the APOE locus, we integrated SNP variants with multi-omics data from human postmortem brains including 2,179 RNA-seq samples from 3 brain regions and two ancestries (European and African), 667 DNA methylation samples, and ChIP-seq samples. Additionally, we plotted the expression trajectory of APOE transcripts in human brains during development. Results: We identified an AD-linked APOE transcript (jxn1.2.2) particularly observed in the dorsolateral prefrontal cortex (DLPFC). The APOE jxn1.2.2 transcript is associated with brain neuropathological features, cognitive impairment, and the presence of the APOE4 allele in DLPFC. We prioritized two independent functional SNPs (rs157580 and rs439401) significantly associated with jxn1.2.2 transcript abundance and DNA methylation levels. These SNPs are located within active chromatin regions and affect brain-related transcription factor-binding affinities. The two SNPs shared effects on the jxn1.2.2 transcript between European and African ethnic groups. Conclusion: The novel APOE functional elements provide potential therapeutic targets with mechanistic insight into the disease etiology.",

keywords = "APOE, Alzheimer{\textquoteright}s disease, Postmortem brain, SNP, Transcript",

author = "Qiang Chen and Luis Aguirre and Guoming Liang and Huanhuan Zhao and Tao Dong and Felix Borrego and {de Rojas}, Itziar and Qichan Hu and Christopher Reyes and Su, {Ling Yan} and Bao Zhang and Lechleiter, {James D.} and G{\"o}ring, {Harald H.H.} and {De Jager}, {Philip L.} and Kleinman, {Joel E.} and Hyde, {Thomas M.} and Li, {Pan P.} and Agust{\'i}n Ruiz and Weinberger, {Daniel R.} and Sudha Seshadri and Liang Ma",

note = "Publisher Copyright: {\textcopyright} The Author(s) 2024.",

year = "2024",

month = dec,

doi = "10.1186/s13024-024-00751-7",

language = "English (US)",

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T1 - Identification of a specific APOE transcript and functional elements associated with Alzheimer’s disease

AU - Chen, Qiang

AU - Aguirre, Luis

AU - Liang, Guoming

AU - Zhao, Huanhuan

AU - Dong, Tao

AU - Borrego, Felix

AU - de Rojas, Itziar

AU - Hu, Qichan

AU - Reyes, Christopher

AU - Su, Ling Yan

AU - Zhang, Bao

AU - Lechleiter, James D.

AU - Göring, Harald H.H.

AU - De Jager, Philip L.

AU - Kleinman, Joel E.

AU - Hyde, Thomas M.

AU - Li, Pan P.

AU - Ruiz, Agustín

AU - Weinberger, Daniel R.

AU - Seshadri, Sudha

AU - Ma, Liang

PY - 2024/12

Y1 - 2024/12

N2 - Background: The APOE gene is the strongest genetic risk factor for late-onset Alzheimer’s Disease (LOAD). However, the gene regulatory mechanisms at this locus remain incompletely characterized. Methods: To identify novel AD-linked functional elements within the APOE locus, we integrated SNP variants with multi-omics data from human postmortem brains including 2,179 RNA-seq samples from 3 brain regions and two ancestries (European and African), 667 DNA methylation samples, and ChIP-seq samples. Additionally, we plotted the expression trajectory of APOE transcripts in human brains during development. Results: We identified an AD-linked APOE transcript (jxn1.2.2) particularly observed in the dorsolateral prefrontal cortex (DLPFC). The APOE jxn1.2.2 transcript is associated with brain neuropathological features, cognitive impairment, and the presence of the APOE4 allele in DLPFC. We prioritized two independent functional SNPs (rs157580 and rs439401) significantly associated with jxn1.2.2 transcript abundance and DNA methylation levels. These SNPs are located within active chromatin regions and affect brain-related transcription factor-binding affinities. The two SNPs shared effects on the jxn1.2.2 transcript between European and African ethnic groups. Conclusion: The novel APOE functional elements provide potential therapeutic targets with mechanistic insight into the disease etiology.

AB - Background: The APOE gene is the strongest genetic risk factor for late-onset Alzheimer’s Disease (LOAD). However, the gene regulatory mechanisms at this locus remain incompletely characterized. Methods: To identify novel AD-linked functional elements within the APOE locus, we integrated SNP variants with multi-omics data from human postmortem brains including 2,179 RNA-seq samples from 3 brain regions and two ancestries (European and African), 667 DNA methylation samples, and ChIP-seq samples. Additionally, we plotted the expression trajectory of APOE transcripts in human brains during development. Results: We identified an AD-linked APOE transcript (jxn1.2.2) particularly observed in the dorsolateral prefrontal cortex (DLPFC). The APOE jxn1.2.2 transcript is associated with brain neuropathological features, cognitive impairment, and the presence of the APOE4 allele in DLPFC. We prioritized two independent functional SNPs (rs157580 and rs439401) significantly associated with jxn1.2.2 transcript abundance and DNA methylation levels. These SNPs are located within active chromatin regions and affect brain-related transcription factor-binding affinities. The two SNPs shared effects on the jxn1.2.2 transcript between European and African ethnic groups. Conclusion: The novel APOE functional elements provide potential therapeutic targets with mechanistic insight into the disease etiology.

KW - APOE

KW - Alzheimer’s disease

KW - Postmortem brain

KW - SNP

KW - Transcript

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SN - 1750-1326

VL - 19

JO - Molecular Neurodegeneration

JF - Molecular Neurodegeneration

IS - 1

M1 - 63

ER -

Identification of a specific APOE transcript and functional elements associated with Alzheimer’s disease

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