Science_-_6_March_2020

and fig. S35), while many astrocyte and microglia
genes are classified as elevated in other tissues. In
fact, several astrocyte signature genes are highly
expressed in liver and/or muscle tissue, whereas
many microglia signature genes are enriched in
lymphoid tissue, bone marrow, and/or blood.
In summary, the global analysis reveals that
most of the putative astrocyte and microglia
signaturegenesarehighlyexpressedinselec-
tive peripheral tissues, often exceeding the ex-
pression levels in the brain.
We superimposed the putative cell type sig-
nature genes on the global tissue expression
landscape using the data from this study (Fig.
7C). Expression of only 180 of the human cere-
bral cortex cell type signature genes (43%) was
classified as brain-elevated with regard to ex-
pression, and 158 genes (38%) were classified

as elevated in expression in nonbrain tissues

and the expression of the remaining genes

(n= 82) classified as low tissue specific. To

further explore this lack of“brain specificity”

of many of the putative brain signature genes,

we analyzed some of these genes further, as

showninFig.7D.Themicrogliasignature

genes arachidonate 5-lipoxygenase (ALOX5)

and integrin subunit beta 2 (ITGB2) both showed

elevated expression in blood (lymphoid tissues),

while other microglia signature genes showed

elevated expression in specific blood cells. For

example, the gene for PYD and CARD domain

containing protein (PYCARD) is expressed by

granulocytes, monocytes, and dendritic cells.

These results confirm the notion of shared

origin and functions between microglia and

immune cells. In contrast, several astrocyte sig-

nature genes are classified as genes with ele-

vated expression in liver or muscle tissue. Out

of the 19 genes with liver-elevated expression,

six are transport-related genes, including solute

carrier family 13 member 5 (SLC13A5), detected

in the membrane of hepatocytes and end feet

of astrocytes in brain, and nine genes code for

metabolic enzymes such as aldehyde dehy-

drogenase 1 family member L1 (ALDH1L1),

detected in cytoplasm of hepatocytes and as-

trocytes. Genes classified as having muscle-

elevated expression include several proteins

with structural function, such as syntrophin

alpha 1 (SNTA1), detected both in astrocytes

andskeletalmuscle.Allthreearethusclassified

as showing elevated expression in tissues other

than brain on the tissue level. These results

highlight the shared function of astrocytes

Sjöstedtet al.,Science 367 , eaay5947 (2020) 6 March 2020 9of16

Basal ganglia Cerebellum

GFAP

ADORA2A

CRYAB

Testis Brain Hippocampus

CACNG3

ALDH6A1

AIF1

RFX2

ACSL4

ATP1A3

520

48356

2296

6835

8097

AKAP17A

2072

Regional specificity

ARHGEF33

ANK1

Heart muscle

Heart muscle

Heart muscle

Lymph node

Lymph node

Lymph node

1776

8027

1059

4395

El

ev

at

ed

in

tis

su

es

ot

he

rth

an

bra

in

Lo

w

tis

su

es

pe

cifi

city

Notdete

cted

Lo

w

re

gi

on

al

sp

ec

fici

tyi

elevated

eleva

ted

Regiona

Brain lly

Tissue specificity

Fig. 6. The regional expression in brain compared with whole-body
expression.Gene classification based on tissue specificity using transcript
expression data in 37 different tissue types enables separation of genes
into brain-elevated, elevated in tissues other than brain, and low tissue
specificity. This is compared to the classification based on regional expression
in the brain. Of 1059 genes, 520 with regionally elevated expression were
also classified as brain-elevated. Genes classified as elevated in tissues other
than the brain are often detected in brain but expressed with low regional
specificity. Rho guanine nucleotide exchange factor 33 (ARHGEF33) is brain-
enriched, including cerebellum-enriched, and here detected in Purkinje cells
(HPA041051). ATPase Na+/K+transporting subunit alpha 3 (ATP1A3) is
group-enriched in brain and heart muscle and detected in all brain regions
with low regional specificity. Immunohistochemistry using HPA056446
displayed the intercalated discs in heart muscle and had a synaptic location
in brain. Crystallin alpha B (CRYAB) is tissue-enhanced in striated muscle,
found in all brain regions with low tissue specificity, and detected in
oligodendrocytes (HPA057100). Regulatory factor X2 (RFX2) is elevated in
testis and detected in all brain regions with low regional specificity, and with a

nuclear localization in testis and neuropil in brain (HPA048969). AIF1 is

enhanced in blood and lymphoid tissues, while also detected in microglia in

all brain regions with low regional specificity (HPA049234). ACSL4 is classified

as low specificity both in tissues as well as brain regions (HPA005552).

ADORA2A is group-enriched in lymphoid tissues and brain, including basal

ganglia–enriched (HPA075997). Calcium voltage-gated channel auxiliary

subunit gamma 3 (CACNG3) is brain-enriched and group-enriched in cerebrum

regions but was not detected in cerebellum, also verified at the protein level

(HPA077238). ANK1 is group-enriched in skeletal muscle and tongue as well as

cerebellum-enhanced in brain, where the protein is selectively associated

with the Purkinje cell membrane (HPA004842). GFAP is brain-enriched and

detected in all brain regions with low regional specificity (HPA056030).

ALDH6A1 is group-enriched in kidney and liver, detected in all brain regions with

low regional specificity, and, as GFAP, localized to astrocytes (HPA029074).

AKAP17A is expressed in all tissue types with low tissue specificity as well as

low regional specificity in the brain; the protein is detected in subsets of

cell nuclei and in brain in glial cells as well as granular cells in cerebellum

(HPA043247). Scale bar, 25mm.

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