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2 research outputs found

Color-Octet $J/\psi$ Production in the $\Upsilon$ Decay

Author: A. Bizzeti
D. P. Roy
E. Braaten
E. Braaten
E. Braaten
E. Braaten
E. Braaten
E. Braaten
E.J. Eichten
F. Abe
F. Abe
F. Abe
F. Abe
G.T. Bodwin
H. Albrecht
H. Fritzsch
H. Fritzsch
H. Trottier
I.I.Y. Bigi
J. P. Ma
J.P. Leveille
K. Byrum
K. Cheung
Kingman Cheung
L. Montanet
M. Cacciari
M. Cacciari
P. Cho
P. Cho
P. Ko
R. Fulton
R.D. Field
T. Daniels
Tzu Chiang Yuan
W. K. Tang
W. Maschmann
W.Y. Keung
Wai-Yee Keung
Publication venue: 'American Physical Society (APS)'
Publication date: 01/01/1996
Field of study

The direct production rate of

\psi

in the

\Upsilon

decay is shown to be dominated by the process

\Upsilon \to ggg^*

followed by

g^* \to \psi

via the color-octet mechanism proposed recently to explain the anomalous prompt charmonium production at the Tevatron. We show that this plausibly dominant process has a branching ratio compatible with the experimental data. Further experimental study in this channel is important to test the significance of the color-octet component of

c\bar c

pair inside the

\psi

system.Comment: 20 pages, Standard LaTeX, 2 figures; a couple of new processes added, but conclusion unchange

arXiv.org e-Print Archive

Crossref

CERN Document Server

Unexpected finding of uniparental disomy mosaicism in term placentas: Is it a common feature in trisomic placentas?

Author: Boter M. (Marjan)
Cheung W.Y. (Wai Yee)
Diderich K.E.M. (Karin)
Dijkman A.
Galjaard R-J.H. (Robert-Jan)
Go A.T.J.I. (Attie)
Govaerts L.C. (Lutgarde)
Hoefsloot E.H. (Lies)
Joosten A-M.S (Marieke)
Knapen M.F.C.M. (Maarten)
Papatsonis D.N.M. (Dimitri)
Polak J. (Joke)
Saris J.J. (Jasper J.)
Srebniak M.I. (Malgorzata)
van de Helm R. (Robert)
Van Opstal A.R.M. (Diane)
van Veen S. (Stefanie)
Vries F.A.T. (Femke) de
Publication venue: 'Wiley'
Publication date: 01/01/2018
Field of study

Objective: Non-invasive prenatal testing (NIPT) detects placental chromosome aberrations. When amniocentesis reveals a normal karyotype, confined placental mosaicism (CPM) may be assumed. In order to confirm this, placental cytogenetic studies were performed. Method: NIPT was conducted in the course of the Dutch TRIDENT study. Placentas of 10 cases with NIPT results indicating an autosomal trisomy and showing a normal (N = 9) or low mosaic karyotype (N = 1) in amniotic fluid (AF) were investigated. The cytotrophoblast as well as the mesenchymal core of two to four placental chorionic villi biopsies were studied with single nucleotide polymorphism (SNP) array. Clinical outcome data were collected. Results: In 10/10 cases, CPM was proven. In 3/10 cases trisomy/uniparental disomy (UPD)/biparental disomy (BPD) mosaicism was discovered. In 2/3 cases, all three cell lines were present in the placenta, whereas BPD was found in AF. In 1/3 cases trisomy 22/UPD22 was present in AF while trisomy 22/BPD22 mosaicism was found in the placenta. Five of 10 pregnancies were affected with pre-eclampsia, low birth weight, preterm delivery, and/or congenital malformations. Conclusion: The presence of trisomy/UPD/BPD mosaicism in 3/10 cases that we investigated proves that trisomic zygote rescue may involve multiple rescue events during early embryogenesis. UPD mosaicism, when present in crucial fetal tissues, may explain the abnormal phenotype in undiagnosed cases

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