Oligodendrocyte-specific expression and autoantigenicity of transaldolase in multiple sclerosis.

Bánki, Katalin; Colombo, Emanuela; Sia, Frederick; Halladay, David L.; Mattson, David H.; Tatum, Arthur H.; Massa, Paul T.; Phillips, Paul E. M.; Perl, András

doi:10.1084/jem.180.5.1649

Cited by 127 publications

(83 citation statements)

References 53 publications

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“…Catalytic activity of wild-type rTAL-H (50 ng) was also inhibited in the presence of 300/lg/ml purified immunoglobulins from MS patients ALV and LAK, by 37% and 26%, respectively (not shown). These data demonstrated that autoantibodies from patients with MS recognized not only the immunoblotted full-length TAL-H protein and its N-terminal fragment [13] but functionally relevant C-terminal epitopes as well. The pathological significance of inhibition of transaldolase activity by autoantibodies is unknown at this time, but capture of TAL-H by immunoglobulins on the surface of B lymphocytes may play an important role in presenting TAL-H to T cells.…”

Section: Lysine 142 Mediates Catalytic Activity Of Tal-hmentioning

confidence: 78%

“…In fact, activated B cells, by virtue of antigen capture on their surface immunoglobulins, are particularly efficient presenters of low abundance antigens [27]. Proliferation of T cells was stimulated by TAL-H in both patients (LAK, stimulation index, SI = 3.1 [13]; ALV, SI = 4.6, not shown). The identification of enzyme inhibitory autoantibodies capable of binding to native TAL-H may provide an example of how specific autoantibodies can influence autoimmune T cell responses in patients with MS.…”

Section: Lysine 142 Mediates Catalytic Activity Of Tal-hmentioning

confidence: 90%

“…No difference was noted between the wildtype or mutant TAL-H in reactivity with Ab 12484, suggesting that multiple epitopes outside the catalytic domain of the molecule are recognized by these antibodies. High-affinity antibodies to TAL-H are present in patients with MS [13]. Catalytic activity of wild-type rTAL-H (50 ng) was also inhibited in the presence of 300/lg/ml purified immunoglobulins from MS patients ALV and LAK, by 37% and 26%, respectively (not shown).…”

Section: Lysine 142 Mediates Catalytic Activity Of Tal-hmentioning

confidence: 95%

“…Importance of PPP has been documented in host defense mechanisms in all tissues against oxidative stress [1], in embryogenesis [2], neurulation [3], myelination [4], inflammation [5][6][7][8], lymphocyte activation [9,10], phagocytosis [6,8], cardiac arrhythmias [11], resistance to radiation of malignant tumors [12]. We recently demonstrated that transaldolase is expressed selectively in oligodendrocytes at high levels, possibly linked to production of large amounts of lipids as a major component of myelin and to the protection of myelin sheaths from oxygen radicals and that high-affinity autoantibodies to human transaldolase (TAL-H) are present in serum and cerebrospinal fluid of patients with multiple sclerosis (MS) [13].…”

Section: Introductionmentioning

confidence: 99%

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Inhibition of the catalytic activity of human transaldolase by antibodies and site‐directed mutagenesis

Bánki

Perl

1996

FEBS Letters

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Transaldolase is a key enzyme of the pentose phosphate pathway. While antibody (Ab) 169, directed against the N-terminal 139 residues of human transaldolase (TAL-H), had no effect on enzyme activity, Ab 12484 raised against full length and functional recombinant TAL-H inhibited catalytic activity. This tentatively mapped the catalytic site to the C-terminal 140-336 amino acid portion of TAL-H. Dihydroxyacetone transfer reactions catalyzed by transaldolase depend on Schiff base formation by a iysine residue. Replacement of lysine-142 by glutamine using site-directed mutagenesis resulted in a complete loss of enzyme activity, suggesting that lysine-142 is essential for the catalytic activity of TAL-H.

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Section: Lysine 142 Mediates Catalytic Activity Of Tal-hmentioning

confidence: 78%

Section: Lysine 142 Mediates Catalytic Activity Of Tal-hmentioning

confidence: 90%

Section: Lysine 142 Mediates Catalytic Activity Of Tal-hmentioning

confidence: 95%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Inhibition of the catalytic activity of human transaldolase by antibodies and site‐directed mutagenesis

Bánki

Perl

1996

FEBS Letters

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“…17 T cell responses and antibodies are also directed against all the major myelin proteins in MS including myelin basic protein (MBP), proteolipid protein (PLP)], myelin oligodendroglial glycoprotein (MOG), myelin associated glycoprotein (MAG), and MOBP. 17,19 Other protein components in the myelin sheath such as transaldolase and CNPase are targets of the immune response in MS. 19,20 Lipids and carbohydrates of the myelin sheath are also targeted in MS. 21 The immune response to one region of myelin basic protein has been studied the most intensively. The peptide between residues 82 and 99 on myelin basic protein is a major target of both T and B cell responses to MBP.…”

Section: The Antigenic Targets Of T Cells and Antibodies In Msmentioning

confidence: 99%

Antigen-Specific Therapy of Multiple Sclerosis: The Long-Sought Magic Bullet

Steinman

2007

Neurotherapeutics

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Summary:The adaptive immune response in multiple sclerosis (MS) targets various myelin proteins and even some inducible heat shock proteins. A few attempts have been made to tolerize relapsing-remitting patients with MS to either fulllength myelin basic protein or to a key peptide epitope between residues 83-99. These trials have demonstrated that this approach may potentially provide benefit to patients with relapsing-remitting MS. However, manipulation of responses to myelin proteins can have deleterious effects. The immune response to myelin components is positioned at a key tipping point in the pathophysiology of the disease. Clarification of the key target antigens in MS, and better understanding of practical methods to attain tolerance to a wide variety of myelin and neuronal molecules will provide the basis for the ultimately successful antigen specific therapy.

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Identification of known and novel genes in activated monocytes from patients with rheumatoid arthritis

Stuhlmüller

Ungethüm

Scholze

et al. 2000

Arthritis & Rheumatism

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Objective. To define gene activation patterns of monocytes (MO) in patients with rheumatoid arthritis (RA).Methods. A complementary DNA (cDNA) library was constructed from first-leukapheresis MO obtained from an RA patient with active disease; 32 P-labeled cDNA from first-leukapheresis MO (activated pool) and third-leukapheresis MO (nonactivated pool) were used as probes for differential hybridization. Reverse transcriptase-polymerase chain reaction (RT-PCR) was used to assess gene activation in MO from an additional 26 RA patients and 6 normal controls.

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Oligodendrocyte-specific expression and autoantigenicity of transaldolase in multiple sclerosis.

Cited by 127 publications

References 53 publications

Inhibition of the catalytic activity of human transaldolase by antibodies and site‐directed mutagenesis

Inhibition of the catalytic activity of human transaldolase by antibodies and site‐directed mutagenesis

Antigen-Specific Therapy of Multiple Sclerosis: The Long-Sought Magic Bullet

Identification of known and novel genes in activated monocytes from patients with rheumatoid arthritis

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