Human Anti-Thyroid Peroxidase Single-Chain Fragment Variable of Ig Isolated from a Combinatorial Library Assembled In-Cell: Insights into the In Vivo Situation

Chapal, Nicolas; Péraldi-Roux, Sylvie; Bresson, Damien; Pugnière, Martine; Mani, Jean‐Claude; Granier, Claude; Baldet, L; Guerrier, B.; Pau, Bernard; Bouanani, Majida

doi:10.4049/jimmunol.164.8.4162

Cited by 25 publications

(29 citation statements)

References 57 publications

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“…These regulatory proteins are expressed on NPA cell membrane and probably partially protect them from CDC. Combining the various human recombinants anti-TPO aAbs we selected by phage display and characterised in term of epitopes (Bresson et al, 2003(Bresson et al, , 2004Chapal et al, 2000;Rebuffat et al, 2006), could make it possible to improve complement activation.…”

Section: Discussionmentioning

confidence: 99%

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Human recombinant anti-thyroperoxidase autoantibodies: in vitro cytotoxic activity on papillary thyroid cancer expressing TPO

Rebuffat¹,

Morin²,

Nguyen³

et al. 2010

Br J Cancer

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BACKGROUND: Thyroid cancers are difficult to treat due to their limited responsiveness to chemo-and radiotherapy. There is thus a great interest in and a need for alternative therapeutic approaches. RESULTS: We studied the cytotoxic activity of anti-thyroperoxidase autoantibodies (anti-TPO aAbs, expressed in baculovirus/insect cell (B4) and CHO cells (B4 0 ) or purified from patients' sera) against a papillary thyroid cancer (NPA) cell line. Anti-TPO aAbs from patients' sera led to a partial destruction of NPA cell line by complement-dependent cytotoxicity (CDC) and antibody-dependent cell-mediated cytotoxicity (ADCC) and exhibited an anti-proliferative activity. Comparison of the cytotoxic activity of anti-TPO aAbs shows that B4 0 induced an anti-proliferative effect and a better ADCC than B4, but a lower one than anti-TPO aAbs from patients' sera. Antibody-dependent cell-mediated cytotoxicity was increased when human peripheral blood mononuclear cells were used as effector cells, suggesting that FcgRs, CD64, CD32 and CD16 are involved. Indeed, anti-TPO aAbs from patients' sera, but not B4 and B4 0 , exhibited CDC activity. CONCLUSIONS: These data indicate that anti-TPO aAbs display moderate ADCC and anti-proliferative activities on NPA cells; IgG glycosylation appears to be important for cytotoxic activity and ADCC efficiency depends on FcgR-bearing cells. Finally, recombinant human anti-TPO aAbs cannot yet be considered as an optimal tool for the development of a novel therapeutic approach for thyroid cancer.

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Section: Discussionmentioning

confidence: 99%

“…Using the phage-display technology, we previously selected and characterised human recombinant anti-TPO aAbs (Chapal et al, 2000. These human recombinant anti-TPO aAbs mimic human anti-TPO aAbs present in the sera of patients suffering from AITD and recognise the human TPO (hTPO) immunodominant region (Bresson et al, 2003, 2004, 2005, Rebuffat et al, 2006.…”

mentioning

confidence: 99%

Human recombinant anti-thyroperoxidase autoantibodies: in vitro cytotoxic activity on papillary thyroid cancer expressing TPO

Rebuffat¹,

Morin²,

Nguyen³

et al. 2010

Br J Cancer

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“…This also can explain that unmutated CLL cases and mutated CLL cases express different antibody repertoires and different VH genes (Fais et al 1988;Johnson et al 1997). Current data support that CLL cells are in active (auto) antigen driven receptor editing, presumably by keeping away from autoreactivity associated with preferential autoimmune linked IGHV gene utilization in CLL patients like IGHV3-21, IGHV4-34, IGKV1-17 (Foreman et al 2007;Hadzidimitruiou et al 2009) and also IGHV5-51 and IGHV1-69 in unmutated IgVH genes (Chapal et al 2000;Vanura et al 2008). Interestingly, highly polyreactive antibodies are expressed frequently by unmutated CLL, but only rarely by mutated cases, supporting the view that the receptor editing mechanism is significantly active to try to elude autoimmunity in CLL.…”

Section: Development Of Mutated Cll B Cellsmentioning

confidence: 85%

Is Chronic Lymphocytic Leukemia a Mistake of Tolerance Mechanisms?

García‐Muñoz¹,

Anton-Remirez²,

Feliu³

et al. 2012

Recent Advances in Immunology to Target Cancer, Inflammation and Infections

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“…Addressing this concern, phage display has also been used to mine non-combinatorial antibody libraries, i.e., antibody libraries that retain original heavy and light chain pairings of human antibody repertoires through in-cell RT-PCR. 110 This method is of particular interest for the identification of human antibodies in autoimmune repertoires.…”

Section: Combinatorial Miningmentioning

confidence: 99%