LAPATINIB AND TRASTUZUMAB COMBINATION

J Clin Oncol. 2010 Feb 1. [Epub ahead of print]

Randomized Study of Lapatinib Alone or in Combination With Trastuzumab in Women With ErbB2-Positive, Trastuzumab-Refractory Metastatic Breast Cancer.

Blackwell KL, Burstein HJ, Storniolo AM, Rugo H, Sledge G, Koehler M, Ellis C, Casey M, Vukelja S, Bischoff J, Baselga J, O'Shaughnessy J.

Duke University Medical Center, Durham, NC; Dana-Farber Cancer Institute, Boston, MA; Indiana University Melvin and Bren Simon Cancer Center, Indianapolis, IN; University of California, San Francisco Helen Diller Family Comprehensive Cancer Center, San Francisco, CA; Medicine Development Center Oncology, GlaxoSmithKline, Collegeville, PA; Texas Oncology, PA, US Oncology, Tyler; Baylor Sammons Cancer Center, Texas Oncology, PA, US Oncology, Dallas, TX; Otto von Guericke Univeristäte, Madgeburg, Germany; and Vall d'Hebron University Hospital, Barcelona, Spain.

PURPOSE: Preclinical studies in ErbB2-positive cell lines demonstrated a synergistic interaction between lapatinib and trastuzumab, suggesting that dual blockade is more effective than a single agent alone. EGF104900 compared the activity of lapatinib alone or in combination with trastuzumab in patients with ErbB2-positive, trastuzumab-refractory metastatic breast cancer (MBC). PATIENTS AND METHODS: Patients with ErbB2-positive MBC who experienced progression on prior trastuzumab-containing regimens were randomly assigned to receive either lapatinib alone or in combination with trastuzumab. The primary end point was progression-free survival (PFS). Secondary efficacy end points included overall response rate (ORR), clinical benefit rate (CBR; complete response, partial response, and stable disease for >/= 24 weeks), and overall survival (OS). RESULTS: In the intent-to-treat population (N = 296) who received a median of three prior trastuzumab-containing regimens, the combination of lapatinib with trastuzumab was superior to lapatinib alone for PFS (hazard ratio [HR] = 0.73; 95% CI, 0.57 to 0.93; P = .008) and CBR (24.7% in the combination arm v 12.4% in the monotherapy arm; P = .01). A trend for improved OS in the combination arm was observed (HR = 0.75; 95% CI, 0.53 to 1.07; P = .106). There was no difference in ORR (10.3% in the combination arm v 6.9% in the monotherapy arm; P = .46). The most frequent adverse events were diarrhea, rash, nausea, and fatigue; diarrhea was higher in the combination arm (P = .03). The incidence of symptomatic and asymptomatic cardiac events was low (combination therapy = 2% and 3.4%; monotherapy = 0.7% and 1.4%, respectively). CONCLUSION: Despite disease progression on prior trastuzumab-based therapy, lapatinib in combination with trastuzumab significantly improved PFS and CBR versus lapatinib alone, thus offering a chemotherapy-free option with an acceptable safety profile to patients with ErbB2-positive MBC.

BORTEZOMIB FOR FOLLICULAR LYMPHOMA

NEW YORK (Reuters Health) Feb 02 - The proteasome inhibitor bortezomib (Velcade) is effective in patients with follicular lymphoma and other indolent non-Hodgkin's lymphomas, according to a report in the January 12th issue of Clinical Cancer Research.

Approved for managing mantle cell lymphoma, bortezomib has shown an inconsistent pattern of activity across many subtypes of lymphoma, the authors explain, and its activity in follicular lymphoma has been a subject of controversy.

Dr. Owen A. O'Connor from the College of Physicians and Surgeons, Columbia University, New York, and colleagues investigated the activity of bortezomib monotherapy in 77 patients (69 assessable for response) with mantle cell lymphoma, follicular lymphoma, chronic lymphocytic leukemia (CLL), small lymphocytic lymphoma (SLL), marginal zone lymphoma, or Waldenstrom's macroglobulinemia.

The overall response rate was 45% (40% on an intention-to-treat basis).

Nine of 18 patients with follicular lymphoma achieved a major response, including 4 with complete remission. Three of 8 patients with marginal zone lymphoma attained a partial remission; 1 of 9 patients with Waldenstrom's macroglobulinemia had stable disease; and 1 of 6 patients with SLL/CLL responded to treatment.

The median time to response was 11 to 12 weeks for patients with follicular lymphoma, compared with 4 weeks for patients with mantle cell lymphoma and all other subtypes of non-Hodgkin's lymphoma.

The overall progression-free survival was 4.75 months, the researchers note, compared with 9.8 months for the line of prior chemotherapy just before entry into this study.

Patients entering the study with refractory disease did worse than patients with relapsed disease, but the difference was of only borderline significance (p = 0.06).

There were no major hematologic toxicities besides lymphopenia and thrombocytopenia, and there were no opportunistic infections, but electrolyte abnormalities were common.

"These data suggest bortezomib has significant single-agent activity in patients with follicular lymphoma, and that longer durations of treatment may improve overall response," the authors say.

They add that theirs is the first report to suggest "that the time to treatment response may be one of the most important determinants of activity" for bortezomib in these patients.

The delayed response may be due to "the immunomodulatory effects of bortezomib on the lymphoma node microenvironment," they speculate.

"Future directions focused on understanding the merits of bortezomib in the indolent lymphomas will continue to explore how best to combine the agent with other known drugs used for these diseases," the investigators add.

Millennium Pharmaceutical, which manufactures bortezomib, provided commercial research grant support and an honorarium to Dr. O'Connor.

Clin Cancer Res 2010;16:719-726.

PERTUZUMAB REVERSES TRASTUZUMAB RESISTANCE?

NEW YORK (Reuters Health) Feb 01 - When given with trastuzumab, pertuzumab, a HER2-targeted monoclonal antibody, can be an effective treatment for HER2-positive breast cancer that progressed during prior trastuzumab therapy, new research suggests.

By contrast, pertuzumab (rhuMAb 2C4) is probably not useful for HER2-negative disease, according to a separate study conducted by many of the same researchers.

Both papers appear in the February 1 Journal of Clinical Oncology.

The first study -- an open-label phase II trial led by Dr. Jose Baselga, from Vall d'Hebron University Hospital in Barcelona - involved 66 patients who received pertuzumab plus trastuzumab after disease progression with trastuzumab-based therapy. Along with trastuzumab, patients received pertuzumab in an 840-mg loading dose, followed by 420 mg every 3 weeks until disease progression or excessive toxicity.

Roughly 24% of patients had an objective response, defined as confirmed complete or partial responses. Fifty percent of patients had a clinical benefit, defined as the total number of objective responses plus stable disease >6 months. Complete response, partial response, and stable disease rates were roughly 8%, 17%, and 26%, respectively.

The median progression-free survival period was 5.5 months, the researchers note.

The drug combination was generally well tolerated, and side effects were mild to moderate. Cardiac toxicity was minimal and no patients discontinued therapy for cardiac-related reasons.

The authors note that single-agent pertuzumab is now being evaluated in the same patient population.

The second study, headed by Dr. Luca Gianni from Istituto Nazionale Tumori in Milan, assessed stable disease rates in 78 patients with HER2-negative metastatic breast cancer, all of whom received an 840-mg loading dose of pertuzumab. The patients were then randomized to continue with either 420 mg or 1050 mg given every 3 weeks.

Eighteen patients (44%) given 420 mg of pertuzumab and 14 (38%) given 1050 mg had stable disease lasting 12 weeks or longer. However, only 6 patients had a treatment response or stable disease lasting 6 months or more.

As in the first study, pertuzumab was generally well tolerated with minimal side effects. Eight patients had a potentially clinically relevant drop in cardiac function, including one with congestive heart failure.

"The limited efficacy observed in this study" and the "generally stable disease of relatively short duration" suggests there is little point to further studies of monotherapy with pertuzumab in unselected patients with HER2-negative breast cancer, the authors conclude.

Both studies were supported by F. Hoffmann-La Roche, which manufactures pertuzumab.

J Clin Oncol 2010.

SIMPLE OVARIAN CYSTS IN POSTMENOPAUSAL WOMEN

NEW YORK (Reuters Health) Feb 02 - In women over 55, simple ovarian cysts are common, usually resolving or persisting without progression, according to data from the prospective Prostate, Lung, Colorectal, and Ovarian Cancer Screening Trial (PLCO).

The presence of simple cysts, often found incidentally during transvaginal ultrasound (TVU) exams, did not affect the risk of ovarian cancer, according to lead author Dr. Robert T. Greenlee and colleagues -- bolstering recent recommendations that unilocular simple cysts in postmenopausal women be followed without intervention.

Dr. Greenlee, from the Marshfield Clinic Research Foundation, Wisconsin, and associates followed 15,735 postmenopausal women through 4 years of annual TVU screening. All were between 55 and 74 years old at enrollment, and all had CA-125 measurements and TVU studies at baseline. Both tests were repeated annually. In addition, for a woman to be included in the study, both ovaries had to be visualized at least once by TVU.

Simple cysts were defined as having a volume <>

In a paper published online January 25 in the American Journal of Obstetrics and Gynecology, the investigators report that the prevalence of at least 1 simple cyst detected during the first fully visualized TVU screening was 14.1%. Potential correlates of prevalent simple cysts were younger age (55 to 59), education past high school, and early menopause. The odds were also higher in women with a history of benign ovarian cysts, menopause before age 40, and a first pregnancy at or beyond age 30.

Among women without a cyst of any kind on their first fully visualized TVU screening, the incidence of simple cysts was approximately 8% per year, remained fairly constant, and did not vary by age.

One-third of ovaries with simple cysts were cyst-free the following year. Even when 2 or more cysts were present, all resolved a quarter of the time. Only 6% progressed in complexity from 1 year to the next.

Women with and without simple cysts were at similar risk of invasive ovarian cancer after nearly 8 years of follow-up evaluation, the authors write. Furthermore, traditional ovarian cancer risk factors, such as increasing age, family history of breast or ovarian cancer, nulliparity, and infertility, were not associated with simple cysts. Finally, changes in average CA-125 were not correlated with increases in the number or progression of simple cysts.

Thus, Dr. Greenlee and his group conclude, "Simple cysts are not likely cancer precursors or markers of increased risk and can be followed conservatively."

Am J Obstet Gynecol 2010.

ASCO FOR GENETIC TESTING

February 4, 2010 — The American Society of Clinical Oncology (ASCO) has issued an updated policy statement on genetic and genomic testing for cancer susceptibility. The new document, an update of a statement issued in 2003, was published online January 11 in the Journal of Clinical Oncology.

The update was prompted by an increase in the number of such tests, and it raises 2 main concerns — the fact that some tests are of unproven clinical benefit, and the fact that some are now being marketed directly to consumers.

More than 900 genetic tests are now available, although only 5% to 10% of all cancers are considered to be hereditary, according to ASCO.

"The awareness of individual genetic differences within the population has sparked a number of significant developments and an unprecedented level of raw information being made available, not only to health professionals, but also to the public in the form of direct-to-consumer [DTC] tests," said senior author Kenneth Offit, MD, MPH, chief of the Clinical Genetics Service at Memorial Sloan-Kettering Cancer Center in New York City, and a member of ASCO's Ethics Committee.

These updated recommendations "attempt to get back to the basics — patient safety and clinical utility — for the individuals considering genetic testing and the doctors who offer testing or may be asked by patients to interpret direct-to-consumer test results," Dr. Offit said in a statement.

Oncologists and other healthcare providers who offer genetic tests should continue to be guided by a recommendation made in 2003, which states that testing should be offered only when the following criteria are met:

• the individual being tested has a personal or family history suggestive of genetic cancer susceptibility
• the genetic test can be adequately interpreted
• the test results have accepted clinical utility.

The updated statement acknowledges that emerging technologies, like genomic profiling for low-penetrance genetic variants (markers of very low disease risk), might be appropriate for patients who do not have a personal or family history suggestive of cancer risk, provided that clinical utility is established and results can be easily interpreted. However, it also points out that the genomic tests for low-penetrance variants currently do not have proven clinical utility.

"None of us in this field is trying to block or delay the transmissions of useful genetic information to the broadest possible constituency," Dr. Offit emphasized in an interview with Medscape Oncology. "But we want to do this in a responsible way," he added, and there is concern that "the premature dissemination of some of these technologies can lead to problems of false reassurances and false alarms."

There are 2 separate issues, Dr. Offit explained.

There is a clear demarcation between genetic tests for high-prevalence mutations, which have proven clinical utility, and genomic tests for low-prevalence variants, which currently have no proven clinical utility, he said.

He explained that there is also a big difference between using these tests in a traditional medical model, where the test is ordered by and discussed with a healthcare provider who is responsible for the patient's health, and the new situation, where these tests are marketed by commercial companies over the internet and where results are issued in a computer printout without any human interaction.

Tests With Accepted Clinical Utility

Examples of genetic tests for which clinical utility is accepted are testing for high-penetration mutations, such as BRCA1/2 for breast cancer and MLH1/MSH2 for colorectal cancer. These tests inform clinical decision-making and facilitate the prevention or amelioration of adverse health outcomes, the authors explain.

For example, women found to carry the BRCA1 mutation, which increases the relative risk of developing breast cancer 32-fold by the age of 40 to 49 years, can be offered increased screening with mammography or magnetic resonance imaging, or risk-reducing surgery. Individuals found to carry the MSH2 mutation, which increases the risk for colon cancer 13.1-fold by the age of 30 years and 9.3-fold by the age of 50 years, can be offered earlier and more frequent endoscopy and a prophylactic colectomy after a diagnosis of malignancy.

Similar interventions can be offered to individuals found to carry another high-penetrance mutation, APC, which increases the risk for colorectal cancer 19-fold over a lifetime. Another high-penetrance mutation is RET, which increases the risk for medullary thyroid cancer 125-fold over a lifetime; people found to carry this mutation are offered prophylactic thyroidectomy.

However, although these high-penetrance mutations are clinically relevant, they are uncommon, the authors point out.

Most inherited cancer susceptibility arises from a number of DNA sequence variants, each of which, in isolation, confers a limited increase in risk. Genetic tests for intermediate-penetrance mutations and low-penetrance variants (single-nucleotide polymorphisms [SNPs]) are of uncertain clinical utility because the cancer risk associated with the mutation or SNP is too small to form an appropriate basis for clinical decision-making. For all of these intermediate- and low-penetrance variants, there is no proven intervention.

ASCO recommends that genetic tests with uncertain clinical utility, including genomic risk assessment, be administered in the context of clinical trials. However, some of these tests are being directly marketed to the public.

One example of a low-penetrance variant (SNP) is rs10505477 at 8q24, which increases the relative risk for colon cancer 1.27-fold and the relative risk for prostate cancer 1.43-fold.

There are also 2 low-penetrance variants, rs13281615 at 8q24 and rs1219648 at FGFR2, which increase the relative risk for breast cancer 1.21-fold and 1.23-fold, respectively. The authors note that this increase in the relative risk of developing breast cancer is equivalent to that of delaying childbearing from age 30 to age 35. "This level of risk does not warrant changes in recommendations for screening or prevention," they add.

Considerable Concern Over DTC Genetic Testing

Genetic testing for cancer susceptibility has become an accepted part of oncologic care, Dr. Offit and colleagues write. To date, most of this testing is professionally mediated and is of accepted clinical utility, they explain.

However, there is "considerable concern within the medical community about various aspects of direct-to-consumer genetic testing," the authors note. With marketing over the internet, there are concerns about informed consent and inadequate counseling, both before and after testing.

"Not all DTC testing companies offer counseling, and they may only offer counseling to consumers who pay additional fees," the team points out. "Where counseling is provided, there is some concern that the advice offered by testing companies may be biased in favor of testing."

It makes for a tricky situation when individuals who obtain DTC tests then turn to a healthcare professional for help interpreting test results. Such requests can "pose significant challenges," the authors write.

"While most of us look forward to a time when all doctors will offer genome scans to guide preventive care of their patients," Dr. Offit said, he is not as sure that the DTC delivery of these services by for-profit companies is the model to aim for.

Some of these points were raised recently by researchers from the University of Michigan Comprehensive Cancer Center in Ann Arbor.

"While the test is a very easy thing to do — it's a simple blood test — the interpretation of the results can sometimes be very complicated," said Mark Pearlman, MD, professor of obstetrics and gynecology at the University of Michigan Medical School.

"It's important to understand that getting the genetic test result is only a piece of the puzzle," he continued. "It really takes a professional who understands genetics to work with individual women and men to allow them to understand exactly what the piece of information means to them in terms of their risk, their loved ones' risks, and what can then be done to lower that risk."

These comments appear in a press statement issued by the university in response to a new advertising campaign in the United States that encourages women to be tested for gene mutations related to breast and ovarian cancer (BRCA1/2).

Only 2% of the population should be tested for these mutations, Dr. Pearlman and colleagues point out.

"It's very important that the right women seek out genetic testing for breast and ovarian cancer," said Sofia Merajver, MD, PhD, director of the Breast and Ovarian Risk Evaluation Program at the University of Michigan. "Cancer risk is more complex than a simple yes or no, and the test for genetic mutations is only part of the picture."

Most cases of breast and ovarian cancer are random and are not linked to BRCA gene mutations, the doctors point out. Less than 10% of all women with breast cancer and less than 15% of all women with ovarian cancer carry a BRCA gene mutation.

Only 1 of the 5 authors of the ASCO policy statement update reports a relevant financial relationship: Mark Robson, MD, from Memorial Sloan-Kettering Cancer Center, reports receiving research funding from AstraZeneca and Kudos Pharmaceuticals.

J Clin Oncol. Published online January 11, 2010. Abstract

ATYPICAL ENDOMETRIAL HYPERPLASIA AND CANCER

NEW YORK (Reuters Health) Feb 02 - The cumulative 20-year risk of endometrial carcinoma for women with atypical endometrial hyperplasia is 28%, compared with a combined rate of less than 5% for women with simple or complex hyperplasia, according to a new report.

"Before our study there were major questions about how likely each of the types of endometrial hyperplasia -- simple hyperplasia, complex hyperplasia, and atypical hyperplasia -- was to progress," senior author Dr. James V. Lacey, Jr., from City of Hope, Duarte, California, told Reuters Health.

Dr. Lacey and his colleagues conducted a case-control study nested in a cohort of 7947 women with endometrial hyperplasia. Case patients (n = 138) were diagnosed with carcinoma an average of 6 years after their diagnosis of hyperplasia. Control patients (n = 241) were matched to case patients on age at hyperplasia diagnosis, date of diagnosis, duration of follow-up, and hyperplasia severity. Original slides and medical records of cases and controls were reviewed.

In the January 10th online issue of the Journal of Clinical Oncology, the researchers report that in women without atypical endometrial hyperplasia (i.e., women with simple or complex hyperplasia), the cumulative risk of progression to cancer after the index biopsy increased from 1.2% through 4 years, to 1.9% through 9 years, to 4.6% through 19 years. For atypical hyperplasia, the cumulative risk increased from 8.2% through 4 years, to 12.4% through 9 years, to 27.5% through 19 years.

Hormonal treatment for endometrial hyperplasia and follow-up biopsies were similar between case patients and controls. All case patients with atypical hyperplasia who were diagnosed with carcinoma at least 5 years after index biopsy received hormonal treatment, and 89% received at least one follow-up biopsy.

"For women who are diagnosed with endometrial hyperplasia and the health care providers who treat them, our data provide the most accurate estimates to date of how likely those women are to clinically progress to carcinoma in the 5, 10, and 20 years after being diagnosed with endometrial hyperplasia," Dr. Lacey noted.

"Numbers like that, expressed as absolute risks," he added, "can be especially helpful in weighing the pros and cons of whether to pursue a course of definitive treatment, like hysterectomy, or whether to pursue a course of nonsurgical clinical management that includes progestin-based therapy and continued observation."

J Clin Oncol 2010.

CETUXIMAB IN NSCLC

J Clin Oncol. 2010 Jan 25. [Epub ahead of print]

Cetuximab and First-Line Taxane/Carboplatin Chemotherapy in Advanced Non-Small-Cell Lung Cancer: Results of the Randomized Multicenter Phase III Trial BMS099.

Lynch TJ, Patel T, Dreisbach L, McCleod M, Heim WJ, Hermann RC, Paschold E, Iannotti NO, Dakhil S, Gorton S, Pautret V, Weber MR, Woytowitz D.

Yale School of Medicine, New Haven; Bristol-Myers Squibb, Wallingford, CT; Mid Ohio Oncology/Hematology, Columbus, OH; Desert Hematology Oncology Medical Group, Rancho Mirage, CA; Florida Cancer Specialists, Fort Myers; Hematology-Oncology Associates of The Treasure Coast, Port Saint-Lucie, FL; Hematology & Oncology Associates of Northeastern Pennsylvania, Dunmore, PA; Northwest Georgia Oncology Centers, Marietta, GA; Piedmont Hematology Oncology Associates, Winston-Salem, NC; Cancer Center of Kansas, Wichita, KS; Western Washington Oncology, Lacey, WA; and Bristol-Myers Squibb, Braine l'Alleud, Belgium.

PURPOSE: To evaluate the efficacy of cetuximab plus taxane/carboplatin (TC) as first-line treatment of advanced non-small-cell lung cancer (NSCLC). PATIENTS AND METHODS: This multicenter, open-label, phase III study enrolled 676 chemotherapy-naïve patients with stage IIIB (pleural effusion) or IV NSCLC, without restrictions by histology or epidermal growth factor receptor expression. Patients were randomly assigned to cetuximab/TC or TC. TC consisted of paclitaxel (225 mg/m(2)) or docetaxel (75 mg/m(2)), at the investigator's discretion, and carboplatin (area under the curve = 6) on day 1 every 3 weeks for

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