TY - JOUR
T1 - A randomized double-lind trial on perioperative administration of probiotics in colorectal cancer patients
AU - Gianotti, Luca
AU - Morelli, Lorenzo
AU - Galbiati, Francesca
AU - Rocchetti, Simona
AU - Coppola, Sara
AU - Beneduce, Aldo
AU - Gilardini, Cristina
AU - Zonenschain, Daniela
AU - Nespoli, Angelo
AU - Braga, Marco
PY - 2010
Y1 - 2010
N2 - AIM: To investigate whether probiotic bacteria, given
perioperatively, might adhere to the colonic mucosa,
reduce concentration of pathogens in stools, and modulate
the local immune function.
METHODS: A randomized, double-blind clinical trial
was carried out in 31 subjects undergoing elective
colorectal resection for cancer. Patients were allocated
to receive either a placebo (group A, n = 10), or a dose
of 107 of a mixture of Bifidobacterium longum (BB536 )
and Lactobacillus johnsonii (La1 ) (group B, n = 11), or the same mixture at a concentration of 109 (group
C, n = 10). Probiotics, or a placebo, were given orally
2 doses/d for 3 d before operation. The same treatment
continued postoperatively from day two to day four.
Stools were collected before treatment, during surgery
(day 0) and 5 d after operation. During the operation,
colonic mucosa samples were harvested to evaluate
bacterial adherence and to assess the phenotype of
dendritic cells (DCs) and lymphocyte subsets by surface
antigen expression (flow cytometry). The presence of
BB536 and La1 was evaluated by the random amplified
polymorphism DNA method with specific PCR probes.
RESULTS: The three groups were balanced for baseline
and surgical parameters. BB536 was never found
at any time-points studied. At day 0, La1 was present
in 6/10 (60%) patients in either stools or by biopsy in
group C, in 3/11 (27.2%) in group B, and none in the
placebo group (P = 0.02 C vs A). There was a linear
correlation between dose given and number of adherent
La1 (P = 0.01). The rate of mucosal colonization by
enterobacteriacae was 30% (3/10) in C, 81.8% (9/11)
in B and 70% (7/10) in A (P = 0.03 C vs B). The Enterobacteriacae
count in stools was 2.4 (log10 scale) in
C, 4.6 in B, and 4.5 in A (P = 0.07 C vs A and B). The
same trend was observed for colonizing enterococchi.
La1 was not found at day +5. We observed greater
expression of CD3, CD4, CD8, and naive and memory
lymphocyte subsets in group C than in group A with a
dose response trend (C > B > A). Treatment did not
affect DC phenotype or activation, but after ex vivo
stimulation with lipopolysaccharides, groups C and B
had a lower proliferation rate compared to group A
(P = 0.04). Moreover, dendritic phenotypes CD83-123,
CD83-HLADR, and CD83-11c (markers of activation)
were significantly less expressed in patients colonized
with La1 (P = 0.03 vs not colonized).
CONCLUSION: La1 , but not BB536 , adheres to the
colonic mucosa, and affects intestinal microbiota by reducing the concentration of pathogens and modulates
local immunity.
AB - AIM: To investigate whether probiotic bacteria, given
perioperatively, might adhere to the colonic mucosa,
reduce concentration of pathogens in stools, and modulate
the local immune function.
METHODS: A randomized, double-blind clinical trial
was carried out in 31 subjects undergoing elective
colorectal resection for cancer. Patients were allocated
to receive either a placebo (group A, n = 10), or a dose
of 107 of a mixture of Bifidobacterium longum (BB536 )
and Lactobacillus johnsonii (La1 ) (group B, n = 11), or the same mixture at a concentration of 109 (group
C, n = 10). Probiotics, or a placebo, were given orally
2 doses/d for 3 d before operation. The same treatment
continued postoperatively from day two to day four.
Stools were collected before treatment, during surgery
(day 0) and 5 d after operation. During the operation,
colonic mucosa samples were harvested to evaluate
bacterial adherence and to assess the phenotype of
dendritic cells (DCs) and lymphocyte subsets by surface
antigen expression (flow cytometry). The presence of
BB536 and La1 was evaluated by the random amplified
polymorphism DNA method with specific PCR probes.
RESULTS: The three groups were balanced for baseline
and surgical parameters. BB536 was never found
at any time-points studied. At day 0, La1 was present
in 6/10 (60%) patients in either stools or by biopsy in
group C, in 3/11 (27.2%) in group B, and none in the
placebo group (P = 0.02 C vs A). There was a linear
correlation between dose given and number of adherent
La1 (P = 0.01). The rate of mucosal colonization by
enterobacteriacae was 30% (3/10) in C, 81.8% (9/11)
in B and 70% (7/10) in A (P = 0.03 C vs B). The Enterobacteriacae
count in stools was 2.4 (log10 scale) in
C, 4.6 in B, and 4.5 in A (P = 0.07 C vs A and B). The
same trend was observed for colonizing enterococchi.
La1 was not found at day +5. We observed greater
expression of CD3, CD4, CD8, and naive and memory
lymphocyte subsets in group C than in group A with a
dose response trend (C > B > A). Treatment did not
affect DC phenotype or activation, but after ex vivo
stimulation with lipopolysaccharides, groups C and B
had a lower proliferation rate compared to group A
(P = 0.04). Moreover, dendritic phenotypes CD83-123,
CD83-HLADR, and CD83-11c (markers of activation)
were significantly less expressed in patients colonized
with La1 (P = 0.03 vs not colonized).
CONCLUSION: La1 , but not BB536 , adheres to the
colonic mucosa, and affects intestinal microbiota by reducing the concentration of pathogens and modulates
local immunity.
KW - colon cancer
KW - dentritic cell
KW - intestinal immunity
KW - lymphocyte
KW - microbiota
KW - probiotic
KW - surgery
KW - colon cancer
KW - dentritic cell
KW - intestinal immunity
KW - lymphocyte
KW - microbiota
KW - probiotic
KW - surgery
UR - http://hdl.handle.net/10807/28104
M3 - Article
SN - 1007-9327
SP - 152
EP - 160
JO - World Journal of Gastroenterology
JF - World Journal of Gastroenterology
ER -