Kit expression in small cell carcinomas of the lung: effects of chemotherapy.

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Kit Expression in Small Cell Carcinomas of the Lung:
Effects of Chemotherapy
Giulio Rossi, M.D., Alberto Cavazza, M.D., Alessandro Marchioni, M.D., Mario Migaldi, M.D., Ph.D.,
Mario Bavieri, M.D., Nicola Facciolongo, M.D., Stefano Petruzzelli, M.D., Lucia Longo, M.D.,
Stefano Tamberi, M.D., Lucio Crinò, M.D.
Department of Pathologic Anatomy and Forensic Medicine, Section of Pathology (GR, MM), and
Department of Respiratory Diseases (AM, MB, SP), University of Modena and Reggio Emilia; Operative
Units of Pathology (AC) and Pneumology (NF), Ospedale S. Maria Nuova, AUSL Reggio Emilia; and
Operative Unit of Oncology (LL, ST), Ospedale degli Infermi, Faenza, AUSL Ravenna; and Medical
Oncology Division (LC), Ospedale Bellaria, Bologna, Italy
A significant number of small cell lung carcinomas
shows overexpression of the proto-oncogene c-kit
product, a tyrosine kinase known as Kit or CD117.
This molecular pathway seems somewhat impli-
cated in promoting the neoplastic growth of small
cell lung carcinoma. The current pharmacological
availability of its selective inhibitor, together with
the promising clinical results in the management of
CD117-positive neoplasms such as advanced gas-
trointestinal stromal tumors, aroused great interest
among oncologists in also adopting this therapeutic
strategy in other CD117-positive tumors. We evalu-
ated a series of 27 small cell lung carcinomas, com-
paringtheexpressionofCD117oftheprimarynaïve
tumor (before first-line chemotherapy) with the ex-
pression of the same neoplasm after postchemo-
therapy relapse. All the patients underwent similar
chemotherapeutic regimens (cisplatin/carboplatin
plus etoposide). At diagnosis, 21 of 27 cases (78%)
showedstrongimmunoreactivity
Among these 21 originally positive tumors, CD117
remained overexpressed in 10 after relapse (48%),
whereas the other 11 cases became negative. No
originally CD117-negative small cell carcinomas
displayed immunoreactivity after chemotherapy.
CD117 expression was not statistically correlated
with overall survival, occurrence of chemoresis-
tance, or clinical response to chemotherapy. We
also evaluated CD117 expression in a series of 46
forCD117.
surgically resected non–small cell lung carcinomas
(8 squamous cell carcinomas, 10 adenocarcinomas,
5 pleomorphic carcinomas, 10 typical and 3 atypical
carcinoids, and 10 large cell neuroendocrine carci-
nomas). Apart from small cell carcinomas, CD117
overexpression was observed in 6 of 10 large cell
neuroendocrine carcinomas, whereas all the other
histotypes resulted unstained. We speculate that
loss of CD117 expression after chemotherapy in a
high proportion of SCLC indicates that in this tu-
mor, Kit unlikely represents the product of a con-
stitutive mutation, as instead shown in gastrointes-
tinal stromal tumors. Keeping this finding in mind,
oncologists could re-test CD117 expression in re-
lapsing small cell lung carcinomas in order to es-
tablish the best candidates for enrollment in ongo-
ing clinical trials with Kit inhibitors. Practically
speaking, CD117 may be helpful in discriminating
between pulmonary high-grade neuroendocrine tu-
mors and other histotypes, but pathologists should
be aware that treated small cell lung carcinomas
may remain unstained in a not insignificant num-
ber of cases.
KEY WORDS: CD117, c-kit, Immunohistochemistry,
Lung, Small cell carcinoma, STI571.
Mod Pathol 2003;16(10):1041–1047
Small cell lung carcinoma accounts for 15 to 20% of
all primary lung tumors (1). It is considered a sys-
temic disease tending to disseminate early in the
course of its natural history, and it is associated
with the lowest 5-year survival rate among all lung
cancers (2–4). Despite modifications of drug com-
positions and doses in chemotherapeutic protocols
and combinations of chemotherapy with chest and
panencephalic preventive radiotherapy, little im-
provement has been achieved in patients’ survival
(2–4). Until now, combined chemotherapy has re-
Copyright © 2003 by The United States and Canadian Academy of
Pathology, Inc.
VOL. 16, NO. 10, P. 1041, 2003 Printed in the U.S.A.
Date of acceptance: June 20, 2003.
Presented in part at the 39th Annual Meeting of the American Society of
Clinical Oncology (ASCO), Chicago, Illinois, May 31–June 3, 2003.
Address reprint requests to: Giulio Rossi, M.D., Department of Pathologic
Anatomy and Forensic Medicine, Section of Pathology, University of
Modena and Reggio Emilia, via del Pozzo, 71-41100, Modena, Italy; fax:
?39.059.4224820; e-mail: rossi.giulio@unimo.it.
DOI: 10.1097/01.MP.0000089780.30006.DE
1041

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mained the mainstay in treating such tumors, but
new approaches are clearly needed, especially in
chemoresistant cases. In this regard, great expecta-
tions aroused by the observation that the auto-
crine/paracrine growth regulation pathway medi-
ated by Kit/CD117, the proto-oncogene c-kit–
derived product, is strongly expressed in ?70% of
small cell carcinomas of the lung, both on cell lines
and paraffin-embedded tissues (5–12). Kit is a Type
III transmembrane tyrosine kinase receptor of 145
kDa that is structurally and functionally related to
platelet-derived growth factor receptor (PDGFR) (5,
6, 12, 13). This membrane-bound protein is essen-
tial for the regulation of cell development and
growth of some hematopoietic cell lines, mast cells,
melanocytes, germ cells, and interstitial gastroin-
testinal cells of Cajal (8, 11–13). Its phosphorylation
and dimerization, as a result of binding with steel
factor or stem cell factor (SCF), provokes a cascade
of intracytoplasmic signals that are deeply impli-
cated in promoting and keeping neoplastic prolif-
eration in malignancies of different histogenesis,
especially in gastrointestinal stromal tumors, mast
cell disorders, and acute myeloproliferative disor-
ders and in a restricted subset of other solid malig-
nancies, including seminomas and small cell lung
carcinomas (11–20). The important therapeutic re-
sults using imatinib mesylate (formerly STI571,
Gleevec; Novartis Pharmaceuticals Corp., East
Hanover, NJ), a selective inhibitor of different ty-
rosine kinases that has been implicated in patho-
genesis of chronic myeloid leukemia (Bcr-Abl) (21),
gastrointestinal stromal tumors (Kit) (22–25), and
dermatofibrosarcoma protuberans (PDGFR) (26),
seem to provide an attractive base for the develop-
ment of this biologic therapy in other Kit-positive
neoplasms also. Although it is yet unanswered
whether Kit expression in small cell lung carcinoma
might be related to an activating (gain-of-function)
mutational event, as instead demonstrated in the
above pathologic conditions (22–26), preclinical in
vitro studies reported that imatinib mesylate effi-
ciently blocked neoplastic growth of small cell lung
carcinoma cell lines (27–29). In light of these obser-
vations, we investigate by immunohistochemistry
whether CD117 expression was modified by che-
motherapy in a series of 27 patients with small cell
carcinoma of the lung who underwent tumor bi-
opsy before first-line chemotherapy and after re-
lapse. Immunohistochemical results were then
combined with clinical findings to analyze the value
of CD117 immunostaining in predicting chemore-
sistance, clinical response, and overall survival in
this specific setting. Moreover, a series of 46 surgi-
cally resected non–small cell lung tumors of various
histotypes were tested for CD117 immunoreactivity
to evaluate the possible diagnostic role of this
marker in lung neoplasms.
MATERIALS AND METHODS
Patient Selection and Immunohistochemistry
From the files of the Section of Pathology of the
University of Modena and Reggio Emilia and from
the Operative Unit of Pathology of the Hospital S.
Maria Nuova of Reggio Emilia, we collected 27 pa-
tients with small cell carcinoma of the lung who
had biopsies obtained before and after postchemo-
therapy relapse between 1991 and 2001. At diagno-
sis, tissue specimens consisted of 20 bronchial bi-
opsies, 2 transthoracic biopsies, and 5 pulmonary
wedge resections, whereas relapsed tumors con-
sisted of 20 bronchial biopsies, 1 transthoracic bi-
opsy, and 6 lobectomies. All the patients underwent
a similar first-line chemotherapeutic regimen (cis-
platin/carboplatin plus etoposide). The second bi-
opsy was obtained after at least three courses of
chemotherapy. Extent of disease at diagnosis was
assessed by fiberscopic bronchoscopy, chest radio-
graph, total-body CT scan, and bone scintigraphy.
Tumor stage was assessed according to the two-
stage Veterans Administration Lung Study Group
system (30). Response to treatment was assessed by
total-body CT scan, and patients were stratified as
nonresponders, partial responders, or complete re-
sponders, in agreement with the protocol of Ther-
asse et al. (31).
The tumor samples were routinely fixed in 10%
buffered formalin and then paraffin embedded. All
the slides were reviewed at a multiheaded micro-
scope by two pathologists (GR, AC). The cases were
included in the study if they fulfilled the accepted
histologic criteria for small cell lung carcinoma (32).
For a better comprehension of the possible diag-
nostic role of CD117 expression in these tumors, 46
surgically resected non–small cell lung tumors (in-
cluding 8 squamous cell carcinomas, 10 adenocar-
cinomas, 5 pleomorphic carcinomas, 10 typical and
3 atypical carcinoids, and 10 large cell neuroendo-
crine carcinomas) were randomly retrieved from
the files of a single institution (the section of pa-
thology of the University of Modena and Reggio
Emilia)andsubsequently
immunostaining.
In each case, 4-?m-thick sections were obtained
from a representative block. Sections were air-dried
overnight at 37° C, then deparaffinized in xylene
and rehydrated through a decreasing concentration
of alcohol to water. Endogenous peroxidase activity
was blocked by immersion for 10 minutes with 3%
hydrogen peroxide (H2O2) in methanol. Immuno-
histochemical staining was performed using a 1:200
dilution of the polyclonal antibody A4502 (DAKO,
Glostrup, Denmark), without antigen retrieval. In-
cubation with the primary antibodies was accom-
plished with a modified avidin-biotin peroxidase
technique using a commercial immunohistochem-
tested forCD117
1042Modern Pathology

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ical autostainer (Ventana, Strasbourg, France); 3'-
3diaminobenzidine was used as the chromogen,
and Harris hematoxylin, as the counterstain. Mast
cells and fibroblasts served as positive internal con-
trols for CD117, whereas appropriate sections of a
gastrointestinal stromal tumor known to be strongly
positive for CD117 were used as external positive con-
trol. Negative controls were included in each test by
substituting the primary antibodies with nonimmune
mouse IgG.
The percentage of positive cells (0: negative, 1?:
1 to 25%, 2?: 26 to 50%, and 3?: ?50%) and the
intensity of staining (0: negative, 1: weak, 2: mod-
erate, 3: strong) were recorded in each case. A tu-
mor was considered positive if ?50% of the neo-
plastic cells reacted with an intensity of ?2? on the
relevant subcellular localization (cytoplasmic and
membranous distribution with or without dotlike
accentuation). Clinical data were collected from
pathological reports, clinical charts, and referring
physicians or directly from the patient’s families.
Statistical Analysis
The comparison between clinicopathologic pa-
rameters and immunohistochemical results was
performed using contingency table methods. Re-
sults were tested for significance using the Pear-
son’s ?2test and Student’s t test and by means of
one-way ANOVA analysis. Estimation of the cumu-
lative distribution of the overall survival was calcu-
lated using the Kaplan-Meier method, and the log-
rank test was used for analysis. All calculations were
performed with Statistical Package for Social Sci-
ences (SPSS) release 8.00, and differences were con-
sidered significant at P values of ?.05.
RESULTS
The relevant clinical data and the immunohisto-
chemical results are summarized in Table 1. Briefly,
case series consisted of 27 patients (17 males and 10
females) with small cell carcinoma of the lung who
underwent tumor biopsy both at diagnosis (on na-
ive untreated cancer) and at the onset of chemore-
sistance after first-line chemotherapy (cisplatin
plus etoposide in 18 cases and carboplatin plus
etoposide in 9). All the patients but two were smok-
ers. Age ranged from 29 to 82 years (mean, 66 y;
median, 66 y). At diagnosis, 10 patients were clini-
cally staged as having limited disease, whereas the
other 17 had extensive disease. Follow-up was ob-
tained in all the cases, ranging from 6 to 92 months
(median, 22 mo). Twenty-four patients died of tu-
mor progression, whereas three are alive with dis-
ease. Immunohistochemically, bronchial and bron-
chiolar epithelium and alveolar pneumocytes in
Table 1. Summary of the Clinical Data and Immunohistochemical Results for CD117 Expression in Small Cell Lung
Carcinomas
Case Age (years)Sex Stage
CD117-preCT
(intensity/%)
First Line
Chemotherapy
Clinical Response
CD117-PostCT
(intensity/%)
Follow-Up
(months)
1
2
3
4
5
6
7
8
9
62
63
66
29
75
56
61
59
65
82
73
59
54
73
74
71
71
75
63
57
65
73
73
60
75
71
72
M
F
M
F
F
F
F
M
M
M
F
M
F
M
M
M
M
M
M
M
M
M
F
F
F
M
M
LD
ED
LD
ED
LD
LD
LD
ED
ED
ED
ED
ED
LD
ED
ED
ED
ED
ED
ED
ED
ED
LD
LD
LD
LD
ED
ED
3?/80 %
?/?
3?/100%
3?/100%
3?/80 %
?/?
1?/10 %
2?/60 %
3?/70 %
3?/75 %
3?/100%
3?/100%
?/?
3?/100%
2?/90 %
2?/80 %
3?/100%
3?/100%
3?/100%
3?/100%
3?/100%
3?/100%
3?/80 %
3?/100%
?/?
3?/90 %
?/?
Cis ? Eto
Carbo ? Eto
Carbo ? Eto
Cis ? Eto
Carbo ? Eto
Cis ? Eto
Carbo ? Eto
Cis ? Eto
Cis ? Eto
Cis ? Eto
Cis ? Eto
Carbo ? Eto
Cis ? Eto
Carbo ? Eto
Cis ? Eto
Carbo ? Eto
Cis ? Eto
Cis ? Eto
Cis ? Eto
Cis ? Eto
Cis ? Eto
Cis ? Eto
Cis ? Eto
Carbo ? Eto
Carbo ? Eto
Cis ? Eto
Cis ? Eto
PR
NR
PR
CR
CR
PR
CR
PR
PR
CR
NR
NR
PR
PR
PR
NR
PR
PR
PR
PR
CR
CR
NR
CR
CR
PR
RC
?/?
?/?
3?/80 %
1?/10 %
?/?
?/?
?/?
1?/3
2?/80 %
1?/10 %
3?/70 %
1?/15 %
?/?
3?/100%
?/?
1?/10 %
3?/90 %
3?/100%
3?/80 %
3?/100%
3?/100%
2?/80 %
1?/2
1?/3
?/?
?/?
?/?
14, DOD
6, DOD
11, DOD
45, DOD
42, DOD
20, DOD
55, DOD
22, DOD
30, DOD
32, DOD
10, DOD
19, DOD
11, DOD
34, DOD
30, DOD
10, DOD
20, DOD
22, DOD
19, DOD
11, DOD
33, DOD
92, AWD
8, DOD
23, AWD
46, AWD
11, DOD
51, DOD
%
10
11
12
13
14
15
16
17
18
19
20
21
22
23
24
25
26
27
%
%
F, female; M, Male; LD, limited disease; ED, extensive disease; Cis, cisplatin; Carbo, carboplatin; Eto, etoposid; CR, complete response; PR, partial
response; NR, no response; DOD, dead of disease; AWD, alive with disease; CD117-preCT, CD117 expression before first line chemotherapy; CD117-
postCT, CD117 expression after first line chemotherapy.
Small Cell Lung Carcinoma and CD117 (G. Rossi et al.) 1043

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normal lung parenchyma adjacent to tumor re-
mained completely unstained for CD117, whereas
scattered positive mast cells and fibroblasts were
noted in the interstitial stroma and in mesenchy-
mal tissue around bronchi and bronchioles and
served as positive internal controls. Among non–
small cell lung neoplasms, including squamous cell
carcinomas (8 cases), adenocarcinomas (10 cases),
pleomorphic carcinomas (5 cases), and carcinoid
tumors (10 typical and 3 atypical), no immuno-
staining was observed except in rare and scattered
tumor cells in 2 of 10 adenocarcinomas. By con-
trast, strong and diffuse Kit overexpression was ob-
served in 21 of 27 naive small cell lung carcinomas
(78%; Fig. 1) and in 6 of 10 large cell neuroendo-
crine carcinomas (60%). In comparison with other
non–small cell lung tumors, high-grade neuroendo-
crine carcinomas (small cell carcinomas and large
cell neuroendocrine carcinomas) showed a statisti-
cally significant difference for Kit expression (P ?
.001; ?2test). Of the 21 positive small cell carcino-
mas,immunoreactivity
postchemotherapyrelapse
whereas no staining was observed in the remaining
11 (52%; Fig. 2). The six patients who were negative
at diagnosis remained negative also after postche-
motherapy relapse. A statistically significant de-
crease of CD117 immunoreactivity after chemo-
therapy was found in regard to intensity staining (P
? .006; ?2test) and percentage of positive tumor
cells (P ? .003; t test). Anecdotally, just one of the
patients with large cell neuroendocrine carcinoma
underwent surgical resection of the lung before and
after chemotherapy, even if performing a different
regimen (cisplatin plus gemcitabine), but both tu-
mors strongly stained with CD117.
No significant difference in overall survival and
response to chemotherapy was observed between
CD117-positive and CD117-negative small cell lung
wasmaintained
only
after
(48%),in10
carcinomas. As expected, stage (limited disease)
and positive clinical response (partial or complete)
correlated significantly with patient survival (P ?
.045 and P ? .034, respectively; log-rank test). Pa-
tients with CD117-positive tumors had more fre-
quently extensive disease (15 of 17) in comparison
to CD117-negative cases (6 of 10), although the
difference did not reach statistical significance (P ?
.153; ?2test).
DISCUSSION
In a recent editorial, Carney (33) stated that “che-
motherapy in advanced lung cancer has reached a
plateau” and thus alternative therapeutic ap-
proaches are clearly required, especially in che-
moresistant cases. In this view, understanding of
lung cancer biology focused particular interest on
several autocrine/paracrine growth loops that were
FIGURE 1. In this case (Case 24), a pulmonary wedge resection showed a small cell lung carcinoma (on the left; hematoxylin and eosin, 200?
magnification). At diagnosis, the tumor overexpressed Kit protein (on the right; CD117, immunoperoxidase, 200? magnification).
FIGURE 2. After first-line chemotherapy, the same patient underwent
a transthoracic biopsy of the relapsed small cell lung carcinoma, but
the tumor was essentially unstained for Kit protein (CD117,
immunoperoxidase, 200? magnification).
1044 Modern Pathology

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thought to be somewhat implicated in their patho-
genesis (34–38). Several works (6–17) demonstrated
that ?70% of small cell carcinomas of the lung
coexpress Kit/CD117, the c-kit proto-oncogene–de-
rived product, and its ligand stem cell factor (SCF).
It is thus suggested that the Kit/SCF pathway pro-
motes and keeps tumor cell proliferation in in vitro
small cell lung carcinoma cell lines. Moreover,
Krystal et al. (27), Wang et al. (28), and, more re-
cently, Kijima et al. (29) elegantly demonstrated
that small cell lung carcinoma cell line growth is
significantly blocked by STI571/imatinib mesylate,
a 2-phenylaminopyrimidine derivative inhibiting
some tyrosine kinases in different neoplastic con-
ditions, such as Bcr-Abl in chronic myeloid leuke-
mia (21), Kit in gastrointestinal stromal tumors (22–
25), andPDGFR in
protuberans (26). Nevertheless, Krystal et al. (27)
reported that STI571 failed to enhance the cytotox-
icity of either carboplatin or etoposide when coad-
ministered in small cell lung carcinoma cell lines. In
the present study, we evaluated the immunohisto-
chemical expression of Kit in a group of small cell
carcinomas of the lung that underwent biopsy be-
fore and after chemotherapy. We had two main
intentions: (1) to analyze whether chemotherapy
effects might give rise to changes on Kit immuno-
staining in these tumors; and (2) to investigate
whether CD117 expression in small cell lung carci-
noma may be a valuable prognostic marker. More-
over, we compared the CD117 immunohistochem-
ical expression in a series of lung tumors of
different histotypes to evaluate the possible diag-
nostic role of this marker in the field of neoplastic
lung pathology.
Our results are consistent with those reported in
previous studies (6–17), confirming that a signifi-
cant number of small cell lung carcinomas (21 of
27: 78%) is positive for Kit, thus representing a
possible target for a novel therapeutic approach
with STI571. However, the current study shows for
the first time that fewer than half of the originally
CD117-positive cases maintain CD117 overexpres-
sion after standard chemotherapy. This phenome-
non is probably secondary to chemotherapy-
induced selection of CD117-negative neoplastic
clones in relapsing small cell lung carcinomas. Kit
activation in neoplastic cells is most commonly
related to the acquisition of activating mutations or
requires the presence of an autocrine or paracrine
stimulation by its ligand (18, 34–38). Although no
studies have explored c-kit locus mutation at 4q11–
12, it is interesting that genetic abnormalities in-
volving chromosome 4q have been found also in
small cell lung carcinoma (39). We suppose that
CD117 overexpression in a significant number of
small cell carcinomas of the lung could be unre-
lated to a true activating (gain-of-function) consti-
dermatofibrosarcoma
tutional mutation, as instead shown in gastrointes-
tinal stromal tumors (40) and more likely represents
the manifestation of one of the main molecular
mechanisms originally implicated in their neoplas-
tic proliferation. Clearly, further studies mainly ex-
ploring c-kit sequence analysis in small cell lung
carcinomas are necessary to better explain the mo-
lecular mechanisms leading to Kit activation. As
also previously noted by Matsuda et al. (10) and
Arber et al. (13), it is noteworthy that normal lung
epithelial structures were completely unstained for
CD117, thus indicating that this aberrant expres-
sion in small cell carcinomas of the lung should
play an important role in promoting their patho-
genesis. Taken together, all the above preclinical
observations provide the scientific rationale for
considering the alternative targeted therapy with
STI571, strongly suggesting that at least a certain
number of naive and chemoresistant small cell lung
carcinomas could receive a potential benefit from
this therapeutic approach. Provided that overex-
pression of CD117 represents the preliminary basis
for using this biologic therapy, our findings may in
part explain the low effectiveness recently reported
by Johnson et al. (41) in their phase II study with
STI571 in a small series of small cell carcinomas of
the lung. Those authors, in fact, treated with STI571
19 patients with extensive stage (both chemother-
apy naive and relapsed), but they tested CD117
overexpression at diagnosis in only 14 cases; more-
over, in no case was the status of CD117 overex-
pression evaluated after tumor relapse. As well ex-
emplified in other oncologic settings adopting
biologic therapy, such as for estrogen and proges-
terone receptor and HER-2 status in patients with
breast cancer or CD20 expression in some non-
Hodgkin lymphomas, immunohistochemical posi-
tivity of the neoplastic cells is one of the main
criteria for a tumor to be treated with targeted
therapy. Although it remains to be seen whether Kit
inhibitor is really effective in this oncologic field,
the frequent loss of CD117 overexpression after
chemotherapy could be considered as a criterion
indicating the need for a rebiopsy of the relapsed
tumors before adopting this kind of treatment. This
will prevent an erroneous selection of patients and
forewarn of possible bias in the evaluation of clin-
ical responses in ongoing clinical trials. By the way,
in patients with refractory small cell lung carci-
noma that maintain CD117 overexpression, the
treatment with STI571 might be considered, espe-
cially in light of its safety and good compliance.
Recently, Naeem et al. (17) reported that CD117-
positive small cell lung carcinomas seem to have a
poorer prognosis than those that are CD117 nega-
tive. We were not able to confirm this observation,
but the unbalanced number of cases in the CD117-
negative (n ? 6) and -positive (n ? 21) groups made
Small Cell Lung Carcinoma and CD117 (G. Rossi et al.)1045