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Featured researches published by Patrice Pere.


Clinical Pharmacokinectics | 1987

Clinical pharmacokinetics of D-penicillamine.

Patrick Netter; Bernard Bannwarth; Patrice Pere; Alain Nicolas

SummaryPenicillamine exists as 2 stereoisomers, but only the D-isomer is used therapeutically. Its chemical reactivity derives from its functional groups, of which the thiol group seems the most important.It is difficult to determine penicillamine in biological fluids because of its instability, the presence of endogenous compounds with a thiol function, and the various chemical forms in which it occurs, namely reduced free penicillamine, penicillamine bound to proteins, and internal (P-S-S-P) and mixed (P-S-S-C) disulphides. The earliest assay methods (colourimetry, isotopic methods, gas-phase chromatography) were neither sensitive nor specific. High performance liquid chromatography with electrochemical detection has led to a more specific assay for D-penkillamine, with detection based on either derivatisation reactions or on electro-oxidisation of the thiol function. With dual-electrode detectors (Au/Hg) disulphides can be assayed directly.D-penicillamine is absorbed rapidly but incompletely (40 to 70%) in the intestine, with wide interindividual variations. Food, antacids and, in particular, iron reduce absorption of the drug. Its bioavailability is also dramatically decreased in patients with malabsorption states. The peak plasma concentration occurs at 1 to 3 hours after ingestion, regardless of dose, and is of the order of 1 to 2 mg/L after an oral dose of 250mg; some investigators have reported a double peak in plasma, which is probably not due to an enterohepatic cycle. The concentration in plasma then decreases rapidly, generally following a biphasic curve. When long term treatment is discontinued, there is a slow elimination phase lasting 4 to 6 days, which suggests that there is a ‘deep compartment’ or ‘slow pool of the drug reversibly bound to tissues’, particularly the skin. This may explain the persistence of its therapeutic effect and the occurrence of undesirable side effects after treatment has been stopped.During long term treatment plasma concentrations are highly variable between individuals. They do not seem to be correlated with the activity or the toxicity of D-penicillamine in patients with rheumatoid arthritis. More than 80% of plasma D-penicillamine is bound to proteins, particularly albumin. The rest is mainly in the free reduced form or as disulphides. Only a small portion of the dose is metabolised in the liver to S-methyl-D-penicillamine. The route of elimination is mainly renal; disulphides represent the main compounds found in the urine. Faecal excretion corresponds mainly to the non-absorbed fraction of the drug.


Skeletal Radiology | 1991

Case report 656

Alain Gaucher; Denis Regent; Pierre Gillet; Patrice Pere; B. Aymard; Véronique Clement

: A case is presented of a 55-year-old man with a MFH in a previous BI. The poor prognosis of such secondary MFH is related in part to the difficulty of its early diagnosis, its aggressive behavior, and its tendency to metastasize (mainly to bone sites and lungs). Nevertheless, although biopsy of asymptomatic bone marrow infarction is not indicated, MRI seems consistent in detecting sarcomatous transformation of symptomatic BIs and plays an important role in the patients preoperative evaluation.


Joint Bone Spine | 2014

Hypertrigyceridemia during infliximab therapy.

Lucie Javot; Patrice Pere; Isabelle Got; Nadine Petitpain; Laurent Peyrin-Biroulet; Pierre Gillet

Joint Bone Spine - In Press.Proof corrected by the author Available online since vendredi 21 juin 2013


British Journal of Clinical Pharmacology | 1992

Plasma and cerebrospinal fluid concentrations of paracetamol after a single intravenous dose of propacetamol.

B. Bannwarth; Patrick Netter; Françoise Lapicque; Pierre Gillet; Patrice Pere; E Boccard; Rj Royer; Alain Gaucher


Rheumatology | 1992

DIALYSIS-ASSOCIATED ARTHROPATHY: A MULTICENTRE SURVEY OF 171 PATIENTS RECEIVING HAEMODIALYSIS FOR OVER 10 YEARS

M. Kessler; Patrick Netter; E. Azoulay; D. Mayeux; Patrice Pere; Alain Gaucher


Journal of Bone and Joint Surgery-british Volume | 1996

THE ‘SMALL-PATELLA’ SYNDROME: HEREDITARY OSTEODYSPLASIA OF THE KNEE, PELVIS AND FOOT

F. Dellestable; Patrice Pere; A. Blum; D. Régent; Alain Gaucher


Arthritis & Rheumatism | 1993

Ossification of the posterior longitudinal ligament in the cervical spine

Alain Gaucher; François Dellestable; Alain Blum; Patrice Pere; Denis Regent


Rheumatology | 2011

Methotrexate-induced hiccups

Lucie Javot; Julien Scala-Bertola; Nadine Petitpain; Philippe Trechot; Patrice Pere; Pierre Gillet


Arthritis & Rheumatism | 1992

Clinical significance of hyaluronan in rheumatic diseases: Comment on the articles by Goldberg et al and Woessner

Jean-Yves Jouzeau; E. Payan; Pierre Gillet; Patrice Pere; Patrick Netter; Alain Gaucher


Arthritis & Rheumatism | 1991

Autosomal dominant arthropathy in a French family.

Alain Gaucher; Georges Weryha; Pascale Perrier; Paul Moreau; Patrice Pere; Pierre Gillet; Vincent Dang Vu

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Alain Gaucher

Centre national de la recherche scientifique

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Alain Gaucher

Centre national de la recherche scientifique

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Denis Regent

Centre national de la recherche scientifique

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Alain Blum

Centre national de la recherche scientifique

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B. Aymard

Centre national de la recherche scientifique

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B. Bannwarth

Centre national de la recherche scientifique

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E Boccard

Centre national de la recherche scientifique

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