Scientific Communications and the General Public


There is a phrase that Albert Einstein used – “You don’t really understand something unless you can explain it to your grandmother.” In my opinion, this quote is imperative to the training of current and future scientists.

When I tell people what a do for a living (biomedical research, in case you were wondering), I typically get a wide-eyed glance of confusion and fascination. After explaining my research at the most basic level, I get a general “Oh, that is cool/great/interesting (insert whatever compliment here)”. Why is it so hard to communicate science to the public?

Not to toot my own horn, but I think that I am pretty good at communicating scientific information to the general public. Unfortunately, this ability is due to teaching as an adjunct professor at a small City of University of New York (CUNY) school and NOT being trained as a biomedical scientist. To be perfectly, honest did not get into tutoring & teaching (starting in graduate school) because I loved scientific communications. I got into it because I needed extra income to live and enjoy New York City, which one really cannot do on a graduate student’s stipend. Extra income aside, I really grew into loving scientific communications, via education. Not to be sentimental, it makes me feel so accomplished, as an effective communicator, when a student asks me if I will teach another science class that he or she is going to take in the following semester.

Incorporating scientific communication training in science

For most U.S. scientists, we all go through same training regimen – a bachelor’s, a master’s, and a doctorate in a specific area of science. During that training, the communications aspect of science is generally overlooked. Yes, at the graduate and postgraduate levels, we publish manuscripts in various biomedical journals, so we know how to write for other scientists. Our type of publishing is great for a specific audience; but, the writing is very dry and complex to most of the general population. Most journal articles follow the sequential formula of: explaining the background of the research, providing specific details about the techniques used, then reporting the significant conclusions. For effective scientific communication we have to flip that concept into something like this: articulating the bottom line, then providing basic details in plain English.

A component of scientific communications needs to be added to the training of up and coming scientists because there are few training opportunities for this skill set.  Although communicating scientific information to the general public is very important, it is necessary for as scientist to market him/herself for a career outside of wet science. In the traditional career path, biomedical doctorate holders work to achieve a position in Academia (or Industry). However, latest trends show that 1 out of 11 Ph.D. holders will obtain a faculty position (that’s less than 10%!!!!). Essentially, the research market is becoming too saturated, so Ph.D. holders need an exit strategy from this traditional career path. Often job descriptions of careers in scientific/medical communications require some training in “non-academic” writing, which many doctorates do not possess. Of course, a person can gain skills in scientific communications, but he/she will have to seek opportunities outside of their formal training. Basically, when Ph.D. holders attempt to enter into the realm of communications, they are often passed over for these positions because we are “overeducated” but “underqualified”. Then, if you are lucky enough to get a position in scientific communications, you often have to start at an entry level with other candidates straight out of college, even though you have 5+ years of scientific expertise over them. It is a bit of a depressing situation – spending years of training only to get “crumbs” once you finish. Although depressing, there are medical/scientific communications agencies that are beginning to understand the value of Ph.D. holders in this field.

Keeping science alive

As we know, governmental funding for many scientific programs are being cut or completely eliminated in this new administration (another topic for another post). For biomedical research, governmental funding is the bread and butter for getting your work out there. Being able to effectively communicate science outside of the ivory towers can build extra support for science, especially from people who are responsible for these funding decisions. It is easier to gain support for embryonic stem cell research, if a politician and his/her constituents understand, in basic terms, what embryonic stem cell research is and how it will directly affect them in a positive manner. Plus, effective scientific communication encourages more participation from the population in process of biomedical research (i.e. increased enrollment in clinical trials).

Concluding remarks

As scientists, we have to understand that we are responsible for going to the public, because the public is not going to come to us. Often scientists are seen as impersonal and standoffish; we already have to fight against the “mad scientist” stereotype. The best way to get to the public is to break down barriers and stereotypes that characterize science as being complex for one to understand unless you have an advanced degree. Let’s make science more accessible to various audiences, thus making it more inclusive and diverse.


Immunotherapy Approvals by the FDA

I wanted to repost this list of FDA approvals of immunotherapeutics that blogger, Brad Loncar has published (***). I made a word cloud of his results and, as expected, Keytruda (pembrolizumab) and Opivid (nivolumab) had the greatest hits for therapies. In recent years the PD-1 inhibitor, Keytruda, has galvanized the immunotherapy field. Keytruda has been found to show indications in advanced non-small cell lung cancer, advanced melanoma, head and neck squamous cell carcinoma, Hodgkin lymphoma, and advanced urothelia bladder cancer. Hopefully, more malignancies can be targeted by Keytruda, along with other drugs.

Future of Cancer Research

Anyone who works in the realm of biomedical research at one point or another has been asked this question, “When will we have a cure for cancer?” Sometimes this question can be annoying, because many people believe that cancer will be cured with one silver bullet. However, one cannot be too annoyed with the question, because it is a fairly honest question. We have been researching, reporting about, and experiencing the ups and downs of cancer for ages. After President Nixon declared war on cancer in 1971, many politicians have promised a cure for this deadly malady.  Since a large portion of biomedical research is funded through various governmental funding agencies, the people, as taxpayers, have a right to ask this question.

This blog update based on an article published by Eva Kiesler and Meredith Begley (***), which lists five reasons for continued optimism in cancer research.  Here, I will touch on three of these reasons that I find very interesting and exciting.

Precision Medicine: In 2015, President Obama announced a $215 million genetic research plan to genetically map one million people, to research the genetic causes of various cancers, and to gauge new drugs and treatments. Of course many of these ideas set forth this initiative may change under the current administration, which has not been very friendly towards science in general.  Of course there is some good mixed with the bad in the field of Precision Medicine. Some of the good can be realized in: understanding the genetic background of new diagnoses, detecting diseases at earlier stages, and developing personalized treatments. However, there are several drawbacks to this field of study that resonate with critics. The biggest criticism is what happens if all of this genetic information falls into the wrong hands. Would someone be denied insurance coverage or a job based on his/her genetic background? Time will only tell how Precision Medicine will help or hinder cancer research, especially under this new administration.

Immunotherapy: Over the past couple of years, immunotherapy has become a very “sexy” field in cancer research. Generally put, immunotherapy uses a patient’s own immune system to fight his/her cancer. It has been long believed that the “cure” for cancer lies in immunology, because cancer basically evades the surveillance mechanism of the immune system. PD-1 inhibitors represent the first class of immunotherapies, but plenty of others inhibitors are quickly catching up to PD-1 inhibitors. Recently, epacdodostat [Indoleamine 2, 3-odioxygenase (IDO) inhibitor], produced by Incyte Corporation, has had great success in combination with PD-1 inhibitors for treating non-small cell lung cancer and kidney cancer.  Many people inside and outside of the laboratory have high hopes for immunotherapy, especially through combination treatment.

Cell-based Therapies: A few years ago, chimeric antigen receptor (CAR) T cells jumped on the scene as an intriguing way to attack cancer cells. This technology makes “killer” T-cells from a patient’s own blood cells. A patient’s T cells are collected; the cells are genetically modified to attack a specific types of proteins expressed on cancer cells; and then these genetically-modified cells are re-introduced into the patient. A major concern with this technology is that one has to modify the T-cells for targets that are expressed on cancer cells and not on healthy cells. In many cases, similar proteins can be expressed on both cancer and normal cells. Since this technology is very personalized, it will take very specialized laboratories to manufacture these cells. Typically, when you get into this extreme level of specialized medicine, the price tag is not cheap. Currently, Novartis and Kite Pharma are two companies that are in the lead for getting this therapy approved by the FDA for treating acute lymphoblastic leukemia and B-cell non-Hodgkin lymphoma, respectively.

Although we have not eliminated various types of cancer, I think that we are well on our way. Here, I touched on three exciting areas of cancer research that may provide some answers in the field of oncology. I think that we are in a very exciting moment of cancer research but time will tell how effective these new therapies will be.

Immuno-oncology . . . the New Frontier

Immuno-oncology . . . the new frontier

As we have learned throughout many successes (and failures) in preclinical, translational, and clinical research, there always has been a very intriguing interface between immunology and oncology, especially with regards to the development of immunotherapeutic drugs. According to GlobalData, a research and consulting firm, the immune-oncology (I/O) market will be worth $14 billion by 2019 and this amount will increase to $34 billion by 2024.

Why is this market so promising?

Before answering that question, let’s take a step back to understand the importance of the immune system in relation to oncology. If you can image the human body as a garden, we have some key players: the soil = the immune system; “good” cells = nice pretty flowers; and weeds = cancer cells. Using this analogy, cancer cells (the weeds) will begin to overtake the good cells (the pretty flower) by competing for space and nutrients. Current treatments (surgery, chemotherapy, and radiation) attempt to kill the weeds but often times the good flowers are harmed and the roots for the weeds remain. Targeted therapies block the growth and spread of these weeds by interacting with these weeds. Some examples of FDA approved targeted therapies include: cetuximbab (Erbitux®; colorectal cancer and squamous cell carcinoma of the head and neck), bevacizumab (Avastin®; cervical cancer, colorectal cancer, and renal cell cancer), and sorafenib tosylate (Nexavar®; hepatocellular carcinoma, renal cell carcinoma, and thyroid cancer). Although these therapies attack the weeds, the good plants may still be damaged. I/O therapy activates the immune system in hopes that only the tumor cells/weeds will be destroyed. In our garden analogy, rather than directly attacking the weeds, I/O therapy is like adding weed-control fertilizer to the soil, although a small number of the flowers may be harmed.

Programmed cell death protein (PD-1) inhibitors, a major player in the IO field, have seen exception sales. Bristol-Myers Squibb’s Opdivo® (nivolumab) and Merck’s Keytruda® (pembrolizumab), being the first generation of I/O pharmaceutical to market, are estimated to generate over $7+ billion in sales by 2024.

In 2016, Opdivo®, Keytruda®, and Yervoy® racked up $3.8, $1.4, and $1.1 billion dollars in sales, respectively. While targets against PD-1/PD-L1 and CTLA-4 represent the first generation of I/O therapies, other pharmaceutic agents against other immunotargets (TIM3, LAG3, and OX40) are quickly competing for market share within this field. Also, there will come a point when these therapies will saturate the market; however, as scientists have learned – two therapies combined often times will make one GREAT therapy. It seems now the race is on for not only finding the best I/O therapy but also for finding the best combination of I/O drugs. This combined approach (with other I/O and/or non-I/O treatments) will lead to some interesting alliances in the I/O field.

Additionally, the emergence of I/O therapies has allowed very lucrative partnerships between various pharmaceutical companies. In 2016, GEN reported the top 15 I/O collaborations (***), ranked on dollar value and press announcements/releases. Below, is a quick list of the top 5 collaborations.

  • Merck & Co. and Ablynx – $6.4 billion, July 2015
  • Pfizer and Cellectis – $2.9 billion, June 2014
  • Merck KGaA and Pfizer – $2.9 billion, November 2014
  • Celgene and Jounce Therapeutics – $2.6 billion, July 2016
  • Sanofi and Regeneron – $2.2 billion, July 2015

Time will only tell how well the I/O field with its current and potential Biopharm collaborations will pan out regarding treatment of various cancers. Although we cannot predict the future of this growing field, the general consensus is a positive one.


Minority Participation in Clinical Trials


The other day some friends/acquaintances and I were randomly chatting about clinical trials. I say that the chat was “random,” because many of these people are not scientists and scientific topics rarely come up in these chats. Then, the story took another random twist into the area about minority groups that are involved in these trials. This twist was more comedic in nature, like would women be considered for participation in a clinical trial for prostate cancer. I wrote this entry, because I wanted to throw my thoughts and interpretations about the lack of minority enrollment in various clinical trials.

Jokes aside, why is this topic so important?

Based on statistics from the U.S. Census, the minority population was 38% of the total U.S. population in 2014; however, the minority population is expected to rise to 56% by 2060. Although minorities currently make up more than a third of the U.S. population, minorities make up less than 10% of patients enrolled in clinical trials, according to the National Institutes of Health (NIH) National Institute on Minority Health and Health Disparities. The major concern with these trials is that many illnesses are observed at a disproportionately higher rate in minority communities. Due to lower enrollment and participation, the data from these trials are limited in terms of effectiveness of treatments and may not represent the best approaches for treatment. There are several factors that may be attributed to this issue, which include lack trust of the medical community, lower incomes, less education, and greater hurdles for accessing healthcare.

In my opinion (I know that others would agree), I think distrust of the medical community and reduced access to adequate healthcare are the two most important factors affecting the enrollment of minorities in clinical trials.

Lack of trust

It is no secret that many people (in addition to minorities) has serious trust issues for towards the medical community. We are well familiar with the Tuskegee study, in which African American men with syphilis were left untreated well after it was discovered that syphilis could be cured in early stages. Although that travesty occurred in the mid 1900’s, the negative ramifications of this study (and other stores of minority medical exploitation, e.g. Henrietta Lacks) are still ingrained in the minds of African Americans. med apartheidHarriet Washington’s book “Medical Apartheid: The Dark History of Medical Experimentation on Black Americans from Colonial Times to the Present” articulates the extreme nature of these notorious (and often useless) medical experiments.

Another potential reason for this distrust is due to the fact that physicians do not look like the people they are serving. Although we have made great racial strides as a country, race and racial bias are still major issues in this country. Typically, many minorities prefer to be examined by people who look like them. Perhaps, a minority patient may feel that the physician will be more empathetic to his/her medical concerns than a non-minority physician. The problem with this rationale is that minorities do not make up a large percentage of practicing physicians serving these communities. In a report from HealthDay Reporter, the percentages of African American and Hispanic practicing physicians are 4 percent and 5 percent, respectively. This statistic shows that there is a large gap between the minority U.S. population and minority physicians.

Access to healthcare

Although distrust is a major issue, I think the lack of access to healthcare is a bigger issue that must be tackled, in regards to clinical trial participation. Since many minorities live within a lower socioeconomic bracket, it is harder for these populations to visit specialists that may inform them of beneficial clinical trials. For example, many minorities have to visit lower quality community health centers where multitude of patients is a great burden for many of the physicians. In a waiting room of 50 patients, I do not think that a physician will have the time and energy to explain every potential treatment that may help one particular patient.

Since many people within these populations also live in lower-income neighborhoods, it is harder for potential clinical trial participants to even visit the health center where the studies are held. If a clinical study requires a long-term commitment with multiple checkups and site visits, this patient may not be able to enroll or complete it, because he/she cannot take time off from work, afford transportation to and from the site, or pay for extra hours of child care.  Since socioeconomic status and education level typically go hand in hand, many members of these populations may not fully understand how participation in the trials would help them and others. This hurdle especially is noticeable if the patient does not speak (or has limited knowledge of) English.

Although I have painted a somewhat grim picture, there are ways to increase the participation of minorities in clinical trials. There have been several outreach programs that will advertise these trials in churches, barbershops, language- or ethnic-specific newspapers and radio stations.  Also, the National Cancer Institute (NCI) recently funded a patient navigator program to assist in the education and enrollment of minorities in clinical trials. Specifically, these patient navigators take the burden off of primary physicians and nurses by meeting with potential trial participants, explaining the trial to the participants, and helping the participants fill out appropriate consent forms. A study in the Journal of Oncology Practice (June 2016) concluded that African American clinical trial participants were twice more like to stay in these trials when assisted with patient navigators. Even though this is a well thought out initiative, there still are issues about initially informing the patient about a potential clinical trial.

Hopefully, the medical community, through various methods of outreach, will continue its efforts in recruiting more minorities for clinical trials. Increased minority participation in these trials potentially will not only help the patient suffering from a particular illness but also provide a better overall public health.

Just Getting Started

In this ever changing climate in pharmaceuticals, life sciences, biotech, regulatory affairs, etc., it can be hard to stay informed. Well, I guess that it can be hard for me but it may be easier for other folks. From my graduate school adventures (back in 2008), I found that it was easier for me to stay abreast of changing aspects in my industry when I actively wrote about them. This previous sentiment is a shout out to my blogging days.  I wonder if Xanga’s portal still exists. This blog space will represent my random thoughts about biomedical research, mostly at within the translational and clinical science “realms”, with a dash of medical regulatory affairs.  Although I do some writing in my current position, it is not as much as I like (compared to writing in an academic setting). For this blog, I will try to add a mix of humor, seriousness, and sarcasm to these updates, because writing about biomedicine does not have to be so dry.

Some quick information about me:

I guess this is the part where I show that I am qualified to speak/blog about science. I have been in the biomedical field, as a scientist, for over 10 years. I pretty much did the traditional career path as many scientists have before me – earned a Ph.D. in a specific field (Molecular Oncology and Immunology, in my case), completed postdoctoral training, and now working as a senior scientist in Immuno-Oncology for a small pharmaceutic company. To slightly differentiate myself, I am an adjunct assistant professor of biology at a couple of CUNY schools in the NYC area. I will say that I really love the teaching aspect of being an adjunct professor, because I can be more creative in the realm of scientific/medical education than in my “wet” scientific roles.  In future post, I will go into more detail about my background.

Here’s to my reentry into the blogosphere.