Tocilizumab reverses cerebral vasculopathy in a patient with homozygous SAMHD1 mutation


CASE BASED REVIEW

Tocilizumab reverses cerebral vasculopathy in a patient
with homozygous SAMHD1 mutation

Michael Henrickson1 & Heng Wang2

Received: 20 February 2017 /Revised: 28 February 2017 /Accepted: 5 March 2017 /Published online: 13 March 2017
# The Author(s) 2017. This article is published with open access at Springerlink.com

Abstract An auto-inflammatory syndrome consequent to
SAMHD1 mutations involves cerebral vasculopathy char-
acterized by multifocal stenosis and aneurysms within
large arteries, moyamoya, chronic ischemia, and early-
onset strokes (SAMS). While this condition involves the
innate immune system, additional clinical features mimic
systemic lupus erythematosus. Mutations in this gene can
also cause a subset of the rare genetic condition Aicardi-
Goutières syndrome. To date, no established therapy suc-
cessfully prevents disease progression. We report a
corticosteroid-dependent SAMS patient, a 19-year-old
male of Old Order Amish ancestry, with diffuse cerebral
arteriopathy identified through contrast brain magnetic res-
onance arteriography (MRA) and MRI. He received sub-
cutaneous adalimumab every 2 weeks for 9 months with
minimal response. Then, he started intravenous tocilizumab
(6 mg/kg/dose) every 4 weeks. He sustained steadily normal-
izing cerebral vasculopathy and lab abnormalities resolved,
allowing prednisone reduction. We conclude that the cerebral
vasculopathy of the homozygous SAMHD1 mutation-
mediated auto-inflammatory disease SAMS responded favor-
ably to tocilizumab infusion therapy.

Keywords Aicardi-Goutières syndrome . Cerebral
vasculopathy .Moyomoya .SAMHD1mutation .Tocilizumab

Introduction

Cerebral vasculopathy associated with mutations in the
SAMHD1 gene can invoke early-onset stroke [1]. Mutations
in this gene can also cause the rare genetic condition, Aicardi-
Goutières syndrome (AGS, MIM225750), which bears a phe-
notypic resemblance to this cerebral vasculopathy occurring
in the Amish population. AGS involves increased production
of interferon (IFN)-α2 [2]. Loss-of-function mutations in any
of six IFN-stimulated genes (TREX1, RNASEH2A,
RNASEH2B, RNASEH2C, SAMHD1, and ADAR) are the
identified cause of AGS [3]. These mutations involve the in-
nate rather than the adaptive immune system. AGS presents
with a phenotypic overlap of early-onset encephalopathy,
mimicking congenital viral infection (cerebrospinal fluid lym-
phocytosis and elevated IFN-α levels, loss of white matter,
and basal ganglia calcifications), and features of systemic lu-
pus erythematosus (SLE), including cytopenias, oral ulcers,
arthritis, perniosis with cutaneous erythematous lesions, and
autoantibodies [4, 5]. AGS can involve a subset of children
that develop early-onset SLE [5]. Intracerebral large artery
disease and chronic progressive arthropathy with distal joint
contractures have been reported in AGS associated with mu-
tation of AGS5 SAMHD1 protein [6, 7]. Further, AGS associ-
ated with heterozygous TREX1 mutations involves ulcerating
acral skin lesions suggestive of chilblain lupus (lupus pernio)
[8]. Heterozygous SAMHD1 mutation can also be associated
with progressive arthropathy, distal joint contractures, painful
oral ulcers, and chilblains [9].

We describe a patient with a similar clinical spectrum who
does not have AGS, rather homozygous SAMHD1 mutation
which led to cerebral vasculopathy. Affected patients within
described pedigrees carrying this mutation develop multifocal
cerebral stenosis and aneurysms within large arteries, chronic
ischemic changes and moyamoya morphology, leading to

* Michael Henrickson
michael.henrickson@cchmc.org

1 Division of Rheumatology, Cincinnati Children’s Hospital Medical
Center, 3333 Burnet Ave., Cincinnati, OH 45229-3029, USA

2 DDC Clinic for Special Needs Children, Middlefield, OH, USA

Clin Rheumatol (2017) 36:1445–1451
DOI 10.1007/s10067-017-3600-2

http://orcid.org/0000-0002-3038-3482
http://crossmark.crossref.org/dialog/?doi=10.1007/s10067-017-3600-2&domain=pdf


early-onset strokes [1]. We report the first successful reversal
of this cerebral vasculopathy with tocilizumab infusion
therapy.

Case report

The 19-year-old male patient MM, of Old Order Amish an-
cestry, was previously reported with autosomal recessive ho-
mozygous SAMHD1 mutation (X-28 in the original study) [1].
Briefly, he developed symmetric Bdry^ polyarthritis at age
9 years, hoarseness at age 12 years requiring vocal nodule
resection, bilateral hand and foot pernio at age 13 years, and
a clinical course characterized by familial short stature, pho-
tosensitivity, and persistent acral vasculopathy presenting as
episodic Raynaud’s disease and progressive, bilateral hand
and foot sclerodactyly. Peripheral vascular examination re-
vealed diminished bilateral carotid Korotkoff sounds, without
bruits of his bilateral carotid or subclavian arteries, or abdom-
inal aorta. Table 1 summarizes salient data from his disease
and treatment course.

MM underwent contrast brain magnetic resonance arteri-
ography (MRA) and contrast brain MR imaging (MRI) based
upon familial risk associated with his sister’s encephalopathy
and the desire to identify potential vasculopathy prior to sim-
ilarly devastating functional consequences. MM’s initial stud-
ies performed at age 16 years were abnormal. On MRA, he
had diffuse narrowing of his bilateral internal carotid arteries

and irregular, narrowed segments of his bilateral anterior ce-
rebral arteries’ A1 and M1 segments (Fig. 1, 1A–C). His bi-
lateral thalamostriate vessels had increased flow, with mild
asymmetry in the early arterial phase of the perfusion study,
consistent with a compensated perfusion pattern despite ex-
tensive fibromuscular changes of arteriopathy. His brain MRI
had no evidence of cerebrovascular occlusive disease; howev-
er, he had bilateral, diffuse arteriopathic changes of his distal
internal carotid, anterior, and middle cerebral arteries. Figure 1
depicts the serial contrast cerebral MRA findings during his
treatment course. Figure 2 depicts the temporal sequence of
MM’s medication interventions.

Based upon adalimumab’s capacity to penetrate the central
nervous system’s blood brain barrier and the putatively pro-
tective role of functional SAMDH1 in mediating the pro-
inflammatory tumor necrosis factor (TNF)-α response [1],
MM started 40 mg SC adalimumab every other week just
prior to obtaining an interval brain MRI/MRA. MM
underwent serial, biannual, contrast brain imaging (MRI and
MRA) including 3D time-of-flight MRA of the circle of
Willis, to assess therapeutic efficacy, and accompanying lab-
oratory biomarkers of inflammation: erythrocyte sedimenta-
tion rate (ESR), Immunoglobulin G (IgG) and total protein.
Throughout his pre-biologic or biologic therapy clinical
course, the C-reactive protein never increased, nor did he
manifest anemia of chronic disease.

Compared to his baseline study (month 0), contrast brain
MRI and MRA obtained at onset of adalimumab therapy

Table 1 Data summary

Elapsed time 6/10/09 8/15/11 1/6/12 5/18/12 7/13/12 8/9/12 11/1/12 1/24/13 5/23/13

Years 0 2.2 0.4 0.3 0.2 0.1 0.2 0.2 0.3

Months 0 26 4.8 4.1 1.9 0.9 2.8 2.8 4

Cumulative (months) 0 26 30.8 34.9 36.8 37.7 40.5 43.3 47.3

Medication (mg/dose)

Methotrexate (oral, weekly) 20 0 0 0 0 0 0 0 0

Prednisone (oral, daily) 5 10 10 10 60 30 20 10 0

Adalimumab (SC every 2 weeks) 0 40 40 40 0 0 0 0 0

Tocilizumab (monthly infusion number) 0 0 0 0 400 (2nd) 400 (3rd) 400 (6th) 400 (8th) 400 (12th)

Lab results (range)

Hemoglobin (130–160 g/L) 14.2 159 158 153 140 155 150 144 146

ESR (0–15 mm/h) 27 10 18 47 14 10 10 10 7

Immunoglobulin G (7.24–16.11 g/L) 19.30 18.70 ND 17.20 ND ND ND 13.90 ND

Total protein (63–82 g/L) ND 85 90 91 78 85a 84 76 78

Platelets (135–466 × 109/L) 308 248 248 313 232 250 257 253 226

Interleukin-6 (0–0.238 pmol/L) 0.571 1.14

Joint count

Active joints 17 0 0 0 0 0 0

Limited joints 29 22 20 20 20 20 17

ND no data

a 7/20/12 total protein

1446 Clin Rheumatol (2017) 36:1445–1451



(month 26) indicated a mixed picture. Vasculopathy
progressed with mild narrowing of his vertebral arteries’ distal
segments and bilateral globus pallidus early collateralization
consistent with moyamoya. Cerebrovascular disease remained
unchanged with persistent bilateral distal internal carotid ar-
tery narrowing and indicated mild improvement of the anterior
cerebral A1 segments and proximal middle cerebral arteries

(M1 segments). There were equivocal changes of mild basilar
artery narrowing and subtle abnormalities of the internal cap-
sules’ posterior limb (arising from the anterior cerebral A1 and
M1 segments). There was also increased signal intensity of the
corticospinal tracts, extending into his cerebral peduncles and
pons. The second study obtained during adalimumab therapy at
month 31 indicated stable vasculopathy without progressive
change in these previously identified abnormalities (Fig. 1, 2A–C).

During a 9-month course of adalimumab therapy, there was
mild evidence of disease advancement (including evolving
moyomoya) but predominant stability while he remained on
a daily 10-mg prednisone dose. However, the therapeutic goal
was amelioration of identified extra- and intracranial medium-
and small-vessel vasculitis with elimination of corticosteroid
dependence. Failure to meet these goals compelled the deci-
sion to change biologic therapy. Serum interleukin-6 (IL-6)
was elevated (0.571 pmol/L) [normal 0–0.238] after 9 months
of adalimumab therapy. With this evidence, he discontinued
adalimumab at month 35 and started tocilizumab 400 mg IV
every 4 weeks at month 36 (6.2 mg/kg/dose).

Although MM did not appreciate a clinical change in
his perniosis or articular disease after his first two month-
ly tocilizumab infusions, he had appreciable improvement

Fig. 1 Serial contrast magnetic resonance cerebral arteriography

Fig. 2 Treatment course

Clin Rheumatol (2017) 36:1445–1451 1447



in his cerebral vasculopathy. This coincided with temporal
deterioration in unilateral hand perniosis requiring escala-
tion in his prednisone dose to 1 mg/kg/day during his
second month of tocilizumab therapy. He tapered predni-
sone successfully to 0.5 mg/kg/day by his third monthly
infusion, when he obtained repeat brain imaging.
Following two tocilizumab infusions, the MRA at month
38 indicated similarly stable findings with the exception
of normalization of his A1 and M1 cerebral artery seg-
ments (Fig. 1, 3A–C). At month 43, the second MRA
obtained during tocilizumab therapy indicated stable in-
creased signal intensity within the bilateral internal cap-
sules’ posterior limbs; other previous abnormalities
remained stable, and the A1 and M1 cerebral artery seg-
ments stayed normal (Fig. 1, 4A–C). At month 47, repeat
MRA following 11 consecutive tocilizumab infusions re-
vealed stable, bilateral distal internal carotid artery
narrowing, continued A1 and M1 segment improvement,
resolution of globus pallidus communicating artery
collateralization (moyamoya), and normalization of the
previously increased bilateral cortical spinal tract signal
intensity (Fig. 1, 5A–C).

Discussion

The auto-inflammatory disease SAMS, an acronym for
cerebral stenosis, aneurysm, moyomoya, and stroke, pro-
duces a heterogeneous phenotype of diverse clinical pre-
sentations, including cerebral palsy, stroke, developmental
delay, failure to thrive, chilblains, and arthritis. Early fea-
tures include mild intrauterine growth restriction, infantile
hypotonia, and irritability, followed by failure to thrive
and short stature. During cold weather months, affected
patients experience a spectrum of vascular abnormalities
of their acral regions including Raynaud’s disease and
chilblain lesions (lupus pernio). They may also have a
low-pitch hoarse voice, glaucoma, migraine headache,
and arthritis characterized by joint tenderness and restrict-
ed motion. Patients do not have hypertension; their car-
diopulmonary, hepatic, and renal function is normal. The
elevated ESR, IgG, neopterin, and tumor necrosis factor-α
(TNF-α) found in these patients are consistent with in-
flammatory disease. Cerebral vasculopathy is a major
hallmark found in all affected individuals typified by ste-
noses and aneurysms. Distinctive neuroimaging findings
include chronic ischemic changes, multifocal stenoses of
the large intracranial arteries, including some with
moyamoya morphology and evidence of prior acute in-
farction and hemorrhage [1]. Clinical outcomes in affected
patients are largely dependent on cerebral vasculopathic pro-
gression. Indeed, the early-onset or recurrence of cerebral

vasculopathy-associated strokes always predicts severe func-
tional impairment and poor cognitive outcomes.

While the specific pathophysiology is uncertain, aberrant
processes involving the innate immune system may support
one or several potential mechanisms. Defective metabolism of
intracellular nucleic acids can activate a cell-intrinsic autoim-
mune response, pivotal to host capacity to discriminate be-
tween self and non-self (e.g., viral) nucleic acids. Nucleic acid
recognition is an essential innate immune strategy for detect-
ing viral infection. Functional regulation involves prevention
of self-activated innate immunity, including negative regula-
tion of the IFN-stimulatory DNA (ISD) response. Virtually all
IFN-mediated antiviral immunity occurs via two types of
nucleic acid detection systems: toll-like receptors (TLRs)
and cytosolic sensors [10]. Because flawed distinction of viral
from self nucleic acids can occur, defective clearance of self-
derived nucleic acids may lead to severe, IFN-associated au-
toimmunity [11]. Activation of TLRs on autoreactive B cell
lymphocytes is a major contributing mechanism. Specific
TLRs predispose to autoantibody production in murine
models of lupus and autoimmunity. Such activation of TLR-
dependent IFN production also occurs in human autoimmuni-
ty (e.g., psoriasis) [12]. In each circumstance, accumulated
nucleic acids are detected by non-cell autonomous mecha-
nisms rather than cell-dependent detection [11].

Cytosolic nucleic acid sensors can initiate autoimmunity if
flawed control mechanisms exist. Negative regulators of the
ISD response play a major role in preventing self-activation of
innate immunity via cell-intrinsic components. One important
negative regulatory mechanism in part involves 3′ repair exo-
nuclease 1 (TREX1) induction. TREX1 is a cytosolic toll-like
receptor-independent, antiviral pathway that detects DNA and
triggers immune activation through transcription factor IFN
regulatory factor 3 [11]. Cell-intrinsic initiation of autoimmu-
nity has distinct requirements for regulation and unique mech-
anisms that precipitate lymphocyte-dependent autoimmunity.
Autoimmunity may be triggered by cell-intrinsic initiation of
the ISD pathway in TREX1-deficient mice, preceding a TLR-
dependent contribution to autoantibody production [11].

Disease pathogenesis may reflect SAMHD1 protein loss of
function instead of partially functional protein expression [1].
The SAMHD1 gene mutation localizes to chromosome
20q11.22-q12 involving a pathogenic, homozygous splice-
acceptor site mutation (c.1411–2A > G) in intron 12. The
SAMHD1 gene consists of 16 coding exons and encodes a
protein of 626 amino acids. This identified mutation results
in exon 13 mRNA transcription skipping, leading to formation
of an aberrant protein. There are two functional domains in the
SAMHD1 protein: a sterile alpha motif (SAM) (residuals 42–
110) and an HD domain (residuals 160–325) [1]. The SAM
domain has the ability to bind RNA [13]. The HD domain
recurs in an enzyme superfamily with phosphohydrolase ac-
tivity which is involved in nucleic acid metabolism [14].

1448 Clin Rheumatol (2017) 36:1445–1451



SAMHD1 is a dGTP-stimulated triphosphohydrolase; it con-
verts deoxynucleoside triphosphates (dNTP) to
deoxynucleoside and inorganic triphosphate. This gene de-
creases dNTP to minimal levels that do not support reverse
transcription, preventing viral infection [15, 16]. SAMHD1
also plays a significant role in clearance of cellular waste
and maintaining IFN homeostasis [2]. While this suggests
SAMHD1 may function as a nuclease, SAMHD1, like
TREX1, is also another potential negative regulator of the
ISD response. Both genes may have a similarly protective,
immunomodulatory role in preventing self-activation of in-
nate immunity. Finally, SAMHD1 may further provide a
protective role in mediating TNF-α pro-inflammatory
responses [2].

In a case-control study of AGS, a phenotypically similar
inflammatory disorder caused by mutations in any of six IFN-
stimulating genes (SAMHD1, TREX1, RNASEH2A,
RNASEH2B, RNASEH2C and ADAR), 90% (74/82) of affect-
ed patients vs. 7% (2/29) of controls had a positive IFN score,
reflecting increased expression of these genes [3]. Clinically,
AGS presents as an infantile encephalopathy, manifesting as
progressive microcephaly and psychomotor retardation; 25%
of patients die in early childhood consequent to its leukodys-
trophy and microangiopathy. A leading hypothesis regarding
AGS is that the accumulation of intracellular nucleic acids
triggers an auto-inflammatory response and consequent in-
creased astrocytic IFN-α production [17]. In AGS, chronic
IFN-α exposure results in altered gene expression for proteins
involved in the stability of brain white matter (ATF4, eIF2Bα,
cathepsin D, cystatin F), an increase of antigen-presenting
genes (human leukocyte antigen class I) and downregulation
of pro-angiogenic factors and other cytokines, i.e., vascular
endothelial growth factor and interleukin-1 (IL-1). These ef-
fects on therapeutic targets for AGS and other IFN-α-
mediated encephalopathies, may primarily involve down-
stream IFN-α signaling cascade effectors rather than only
IFN-α [17].

The relationship of increased IL-6 production and IFN-α
signaling in the context of SAMHD1 mutation disease is un-
clear. However, the model of viral infection provides context
for indirect evidence of increased IL-6 expression consequent
to IFN-α priming. During viral infection, host cells are alerted
by the presence of circulating class I IFN, preparing them for
response if they become infected. When a cell recognizes
double-stranded RNA (dsRNA), this indicates the cell is likely
already infected with virus. However, when a cell encounters
either IL-1β or TNF-α, the cell receives warning about the
host’s escalating inflammatory response. This warning does
not indicate direct viral infection of the cell. Instead, the class I
IFN priming phenomenon promotes a vigorous response to
direct viral infection more than IL-1β or TNF-α provide.
While IFN-α does not directly induce IL-6 expression, prior
cellular exposure to IFN-α synergistically enhances IL-6

expression in response to the viral dsRNA. The magnitude
and kinetics of IL-6 induction vary in these situations since
class I IFNs selectively enhance response to dsRNA [18].

Systemic vasculitides with increased IL-6 expression in-
clude Takayasu’s arteritis [19–22], acute Henoch-Schönlein
purpura [23], giant cell arteritis [24, 25], acute Kawasaki dis-
ease [26–28], and various large vessel vasculitides [29–33].
Tocilizumab therapy provides a promising role in achieving
disease remission for refractory neuro-Behçet’s disease, re-
lapsing or refractory giant cell arteritis, and large vessel vas-
culitis secondary to Takayasu’s arteritis, Cogan syndrome, and
relapsing polychondritis [29, 33–39].

TNF inhibition (typically infliximab) has circumstantial
evidence suggesting efficacy in open label use for large vessel
vasculitis secondary to refractory Takayasu’s arteritis, relaps-
ing polychondritis, Behçet’s disease (also including
adalimumab), and relapsing polychondritis. However, this ap-
proach has not been effective for large vessel vasculitis due to
giant cell arteritis as demonstrated in randomized controlled
trials or a prospective trial for granulomatosis with polyangi-
itis [31, 40]. Adalimumab stabilized our patient’s cerebral
vasculitis without remarkably reversing progressive
arteriopathy.

Results are mixed regarding the efficacy of TNF inhibitors
for the therapy of lupus pernio. TNF inhibitors can induce this
disease [41]. However, lupus pernio secondary to sarcoidosis
responded swiftly to adalimumab in one case report [42].
Tocilizumab has not been reported for this use. Neither
adalimumab nor tocilizumab were effective for our patient’s
SAMS-associated pernio.

Conclusions

There is no established, uniformly successful treatment strat-
egy for SAMS, an auto-inflammatory disease consequent to
homozygous SAMHD1 mutation. Relapses remain common
with prednisone tapering. Traditional corticosteroid-sparing,
non-biologic immunosuppressive medications used in the
treatment of rheumatic diseases involving adaptive immunity,
e.g., methotrexate, are ineffective in the treatment of SAMS
cerebral vasculopathy, a disease involving the innate immune
system. Based on the effectiveness of tocilizumab in control-
ling a variety of active large vessel vasculitides including
Takayasu’s arteritis and giant cell arteritis, tocilizumab pro-
vides a novel therapeutic option for SAMS. Following its
initiation, MM obtained disease control within 2 months,
followed by substantial reversal of much of his cerebral vas-
culopathy after nearly a year of tocilizumab treatment. With
this apparent efficacy and durability, tocilizumab may offer a
means of controlling cerebral vasculopathy from the auto-
inflammatory disease SAMS.

Clin Rheumatol (2017) 36:1445–1451 1449



Acknowledgements None.

Compliance with ethical standards

Funding source No funding was secured for this study.

Financial disclosure Authors have no financial relationships relevant
to this article to disclose.

Disclosures None.

Open Access This article is distributed under the terms of the Creative
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creativecommons.org/licenses/by/4.0/), which permits unrestricted use,
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	Tocilizumab reverses cerebral vasculopathy in a patient with homozygous SAMHD1 mutation
	Abstract
	Introduction
	Case report
	Discussion
	Conclusions
	References