Serum levels of P-selectin in men with high-functioning autism

Immune dysfunction has been proposed as a mechanism for thepathophysiology of autistic-spectrum disorders. The selectinfamily of adhesion molecules plays a prominent role in immune/inflammatoryresponses. We determined the serum levels of three types ofsoluble-form selectin (sP, sL and sE) in 15 men with high-functioningautism and 22 age-matched healthy controls by enzyme-linkedimmunosorbent assay. Levels of sP-selectin and sL-selectin were significantly lower in patients than in controls. Furthermore,sP-selectin levels were negatively correlated with impairedsocial development during early childhood.

INTRODUCTION

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INTRODUCTION

Immune dysfunction a potential pathophysiological mechanismof autistic-spectrum disorders.^1,2 Selectins P-selectin,L-selectin and E-selectin are involved in the capture and rollingof lymphocytes along the endothelial cell surface at the first step of lymphocyte migration.³ We found abnormal serum levelsof selectin in schizophrenia,³ but no studies have investigatedany alterations in the serum levels of selectins in autistic-spectrumdisorders. We examined whether men with high-functioning autismhave altered serum levels of soluble (s) forms of selectins(sP-, sL- and sE-), and studied the relationship between theserum selectin levels and clinical features in these men.

Method

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Method

Fifteen men with high-functioning autism and no other comorbid neuropsychiatric disorder were recruited from the Associationfor Asperger Syndrome and Learning Disorders, Nagoya, Japan.All were assessed using the Japanese version of the AutismDiagnostic Interview–Revised (ADI–R).⁴ Resultsof the ADI–R and other cognitive instruments used to assessthe men are given in the online supplement to this paper. Allpatients were unmedicated. A control group of 22 healthy volunteerswas recruited from university students and community volunteers.Control participants had no developmental delay or historyof psychiatric disorder or treatment. Controls were excludedif they had a first- or second-degree family history of psychiatricillness. All patients and controls were Japanese, unrelated,and free of both chronic and acute physical illnesses suchas infectious or immune diseases. The mean age did not differsignificantly between the two groups; 22.8 years (s.d.=2.5)for patients and 23.2 years (s.d.=2.4) for controls (P=0.64).

Serum samples were obtained from peripheral venous blood between11:00 and 12:00 am after fasting for at least 3 h, and werekept at room temperature for 30 min. They were centrifuged,divided into portions and stored at –80°C. Levelsof sP-, sL- and sE-selectin were determined using sandwichenzyme-linked immunosorbent assay kits (R&D Systems Inc. Minneapolis, USA). The samples of all patients were measuredtogether in one assay with a set of control samples. Each samplewas analysed and duplicated, and the mean value of the twomeasures was used for the analyses. A P<0.05 was consideredstatistically significant.

This study was approved by the ethics committee of the HamamatsuUniversity School of Medicine and all participants gave writteninformed consent before voluntary enrolment.

Results

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Results

The serum level of sP-selectin in the patients was significantlyand substantially lower than that of controls, with a medianof 71.7 ng/mL (mean=67.1 ng/ml, s.d.=14.4) and of 122.0 ng/ml(mean= 121.8 ng/ml, s.d.=33.0) respectively (Mann–WhitneyU=27, P<0.001) (online Fig. DS1(a)). The patient group alsohad a significantly decreased level of sL-selectin comparedwith the control group: 942.1 ng/ml v. 1043.9 ng/ml; Mann–WhitneyU=76, P=0.005. Regarding sE-selectin, there was no significantdifference between the two groups: 45.4 ng/ml for patientsv. 39.2 ng/ml for controls (Mann–Whitney U=133, P=0.33).

We first examined the correlations between serum sP-selectinlevels and clinical variables among patients. There was a negativecorrelation between sP-selectin levels and ADI–R scoresfor domain A (Spearman's rank correlation r=–0.589, P=0.021)(Fig. DS1(b)); the lower the level of sP-selectin, the worsethe social development in childhood. There were no marked orsignificant correlations between serum sP-selectin levels andother clinical variables. We then examined the correlationsbetween serum sL-selectin levels and clinical variables, andfound no correlations.

Discussion

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Discussion

The serum levels of sP-selectin and sL-selectin were significantlylower in the patients than in the controls. As patients wereunmedicated and free of physical illness, it is unlikely thatthe altered levels were ascribable to systemic inflammatoryconditions or drug effects. Furthermore, there was little overlapin the distribution of the sP-selectin levels between the patientand control groups; in effect, all patients had lower valuesthan the 25th percentile of the control group (Fig. DS1(a)).

Neither P-selectin nor L-selectin has been reported in the humanbrain; however, P-selectin is expressed on the endotheliumof the blood–central nervous system (CNS) barrier andsoluble L-selectin has been found in cerebrospinal fluid.³Since both P- and L-selectin play important roles in the entryof circulating T-lymphocytes into the CNS,⁵ the decreased serum level of these two types of selectin observed in ourstudy indicates an involvement of hypoactivity of T-lymphocytesin the pathophysiology of high-functioning autistic-spectrumdisorders. It is possible that molecules not expressed in thebrain may alter CNS function. Mice deprived of mature T-cellsmanifest spatial learning/memory impairments that are amelioratedby T-cell restoration.³ Furthermore, it has been reportedthat in children with autistic-spectrum disorders aberrantbehaviour (e.g. irritability, lethargy, hyperactivity, stereotypy,inappropriate speech) improves during fever but returns whenthe child recovers.⁶ These behavioural improvements may involveactivation of T-lymphocyte function.

Aberrant immune activity during brain development might alsoplay a role in the neural basis of high-functioning autism.Diminished expression of P-selectin is associated with delayedneutrophil transmigration in neonatal rats. Therefore, decreasedexpression of P-selectin in individuals early in life may contributeto delayed leukocyte transmigration and increased susceptibilityto infection,⁷ which may in turn damage neural tissues duringCNS development. In fact, there is evidence that maternal viralinfection in the first trimester can increase the risk of offspringdeveloping an autistic-spectrum disorder.⁸

We recently found that the serum level of sL-selectin in patientswith schizophrenia was significantly higher than that in controls,whereas the level of sP-selectin was not altered.³ Schizophreniaand (high-functioning) autistic-spectrum disorders are both viewed as neurodevelopmental disorders, and immune dysfunctionhas been proposed as a potential mechanism for the pathophysiologyof both.^1,2,9 The alterations in serum levels of the selectinsin the two disorders suggest that selectins play a role intheir pathophysiology. However, the existence of distinctivepatterns of alterations (i.e. reduced (for high-functioning autism) v. elevated (for schizophrenia) selectin levels) indicates that the pathological mechanism may differ between the twodisorders, although they share some phenotypic characteristics.The possible distinction may be supported by the differentfindings in brain histopathology and pharmacological sensitivityin these two disorders. Nevertheless, caution is required ininterpretation based merely on one measurement of serum materials.

Low serum levels of platelet-endothelial adhesion molecule-1(PECAM-1) and vascular cell adhesion molecule-1 (VCAM-1) occurin patients with high-functioning autistic-spectrum disorders.¹⁰Since these adhesion molecules, together with selectins, playroles in the migration of leukocytes into inflammatory sites,⁵our observation may reflect an impairment of the adhesion cascade,which in turn is responsible for dysregulation of the immuneresponse in high-functioning autistic-spectrum disorders.

Reduced sP-selectin levels in our patient group were correlatedwith disturbances in social function during early childhoodas assessed with ADI–R (Fig. DS1(b)). However, participantswere over 18 years of age. It would be of interest to measuresP-selectin levels in very young children with high-functioningautistic-spectrum disorders to determine whether such adhesionmolecules serve as a serological marker.

This study has potential limitations. Active or previous exposureto common viral pathogens that may affect immunological markerexpression (e.g. hepatitis and Epstein–Barr viruses)was not tested for. If exposure to these pathogens differedbetween patient and control groups (e.g. if the patients hadbeen hospitalised for long periods, increasing risk of exposure), erroneous conclusions would be drawn. However, none of thepatients was institutionalised, either at the time of the studyor previously. Furthermore, if it were the case, elevated ratherthan reduced levels of selectin would be expected in the patientgroup. Factors such as cigarette smoking and exercise, whichwere not systematically assessed, may have confounded our findings. Studies have suggested that both factors may increase levelsof sP-selectin.^11,12 Although all patients in our study werenon-smokers, some controls may not have been. Individuals withautistic-spectrum disorders are less likely to engage in exercisethan healthy people because of their impaired reciprocal socialinteractions, and restricted behavioural repertoire and interests.The possible bias arising from these potential confoundersmay lead to an overestimation of the results. However, theserum level of sP-selectin was found to correlate with impairedsocial development during early childhood. This implies thatthe current results cannot be ascribed entirely to such confoundersthat pertain to contemporary behaviour.

Soluble P-selectin was implicated in the pathophysiology of high-functioning autism, but studies using larger and youngersamples are required to confirm our findings.

ACKNOWLEDGMENTS

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ACKNOWLEDGMENTS

Partial support from the Ministry of Health, Labour and Welfare,Japan. N.T. is recipient of a Grant-in-Aid for Science Research(B) (2) (14370288) and a grant for the National Center forChild Health and Development (19KOU-3) from the Ministry ofHealth, Labour and Welfare, Japan.

REFERENCES

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