Health and National Security Issues for the USA and Is The United States of America Prepared

Lack of vaccine and proven treatment for COVID-19 has had the world scrambling to find treatments. Every pharma company is looking for ways to control the disease. Hydroxychloroquine and other drugs have been suggested and used. They might work on individuals but its efficacy is anecdotal. US had difficulty in acquiring sufficient dosages from overseas. FDA had to let that company it had banned to export to US ship to US. US and Indian governments at its highest levels had get involved. This brings up a point of discussion of having capabilities to acquire or produce critical drugs. There is no financial interest with any entity.

Answer to this question for the developed countries is flat NO. 

Most of the generic drugs which are better than 80% of the total US prescription market are imported from China and India ⁽¹⁾. If the drugs stop coming from these countries, US will have no capability to serve its populations pharma needs ⁽²⁾. 

I am sure US legislators are cognizant of these facts and considering alternate options. Ultimate remedy has to bring pharma manufacturing home. However, there are three bottlenecks. They are:

1. US FDA
2. Pharma lobbies
3. Pharmacy Benefit Managers (PBM)

There is no point in discussing what these have done as everyone is aware of there doings. They can implement plans to remedy the situation and bring pharma manufacturing home. 

Pharma and PBM lobbies have to be contained. In addition US FDA has to fix its broken ANDA approval system and create an environment and incentive to bring manufacturing home. Some of these plans are laid out in eth linked blogs. 

1.     What Is Needed for a Regulatory Approval of NDA/ANDA Filings in 90 Days? http://bit.ly/31ALUcu

2.     Impact of Regulations, Manufacturing and Pharmaceutical Supply Chain (PBMs) on Drug Shortages and Affordability Part 2 https://bit.ly/2TYQeOQ

3.     Drug Shortages, Quality and Prices: Who is Responsible? http://bit.ly/2oVgmAD

4.     ONE PAGE Road Map to Reduce Drug Shortages, Assure Quality and Improve Affordability http://bit.ly/34RYypH  

5.     Strategies to Increase Generic Drug Competition and Bring Manufacturing to The United States of America http://bit.ly/3d0gjaO

6.     How Would US FDA Behave/React if They Were on the Receiving End? https://bit.ly/3bwGiVW

7.     Long Term Drug Quality Supplies for US, FDA and A New Reality https://bit.ly/3aKaxZw

Above are ideas that can be used to fine-tuned to create and implement viable plans.  

Girish Malhotra, PE

EPCOT International

1. https://www.statista.com/statistics/205042/proportion-of-brand-to-generic-prescriptions-dispensed/ Accessed May 8, 2020
2. Gibson, Rosemary, China Rx: Exposing the Risks of America’s Dependence on China for Medicine, https://www.uscc.gov/sites/default/files/RosemaryGibsonTestimonyUSCCJuly152019.pdf, accessed May 8, 2020

How Would US FDA Behave/React if They Were on the Receiving End?

Corona virus COVID-19 has given us all time to think and conjure up things that can upset the established apple cart or improve it. We need and that includes FDA to simplify FDA’s approval processes and method if we want the drug industry to come back to the United States and be able to supply needed essential medicines. We have an opportunity. There is no financial affiliation with any for profit and nonprofit entity. 

The current global epidemic is not the last one. We could have many. We need to be self-sufficient to access the needed drugs. Why I say this? In the current and any future epidemic countries will fend for their needs. Case in point is chloroquine. Many have speculated that chloroquine can help in treatment of COVID-19. It is in short supply in US. US FDA asked ⁽¹⁾ Ipca Lab, India, to supply the drug for the US market when in 2017 Ipca Labs⁽²⁾ was banned to exports to US. Interestingly Indian Government banned chloroquine exports ⁽³⁾. 

If we want pharma manufacturing to come back to US, the FDA current review and approval methods and processes ^{(4, 5)} need to streamlined and simplified. I am sure US has a list of essential drugs. Stockpiles might not help if we cannot manufacture the active ingredients and formulate them in US.  

Should the US population revolt to bring pharma manufacturing home? Besides lip talk our legislator and the regulators would not do anything. In addition to bringing pharma manufacturing home, they have to compete against the best manufacturing technologies outside to produce quality drugs at the lowest cost. Many stars will have to align. 

In my recent post ⁽⁵⁾ I have tried to describe the current approval and application process. I am not a master of the application process, but if the pieces and parts of what I understand are true, we have an opportunity to improve. This will give the industry an incentive to come to US. I call my perspective “nondestructive creation” or an outlier thinking. Some or many could consider all this a farfetched dream and can’t be done. Well most thought man could not go the moon and come back. Well, we did that and some.

US FDA, like any manufacturing organization, where continuous improvement is routine, has to improve and simplify its NDA/ANDA review and approval processes. FDA has to shed its lenient methods (483 citations which I call “medal of honor” and take a tougher stand ^(6,7). Best of the best in pharma have to compete for the largest market. It’s not just the new drugs. FDA has to hold their feet to the fire. In addition, we need to be able to manufacture lifesaving drugs in case we need them for the next pandemic. We are not ready today as we can’t get chloroquine as explained earlier.

Every manufacturer practices QbD from the get go for every product. Industry practices “continuous improvement” in everything they it does. If they did not their products would have a very short shelf life. FDA has been preaching “quality by design (QbD)⁽⁸⁾”. Has it been practicing them for its NDA/ANDA review and approval processes? In addition, what has FDA done with respect to incorporate “continuous improvement” in its review and approval processes. My conjecture is and many others would concur that FDA’s current NDA/ANDA processes are quality by analysis/aggravation processes and could use improvements. 

May be their understanding of QbD is different from what they have been preaching. If regulators believe their current ANDA/NDA application/review/approval process pathway is QbD based then we need to reexamine QbD definition. My conjecture is FDA would not be pleased to see their QbD rating if there was such a scale. As discussed earlier ⁽⁵⁾ no one really knows how much time it takes to get approvals. With that said, I wonder how many companies would want to establish manufacturing plants in the United States. 

We need to be proactive and not reactive in bringing manufacturing home. In that effort we can also improve regulatory practices. If we don’t do it, another epidemic might not be kind to the US population. 

Girish Malhotra, PE

President

EPCOT International

1.     FDA frees India’s Ipca Lab from import ban so it can ship unproven Chloroquine for COVID-19 treatments, FiercePharma, March 23, 2020

2.     FDA bans imports of Ipca Lab drugs, FiercePhama, June 19, 2017 

3.     India bans export of malaria drug Trump touted as coronavirus treatment, Fortune, March 25, 2020

4.     Malhotra, Girish: Strategies to Increase Generic Drug Competition and Bring Manufacturing to The United States of America, Profitability through Simplicity, March 16, 2020

5.     Malhotra, Girish: GDFUA II ANDA (Abbreviated New Drug Application) Review Target of 8-10 Months should be a Cause of Concern, Profitability through Simplicity, March 24, 2020 

6.     Malhotra, Girish: Are US FDA 483 Citations a "Medal of Honor" or “Rite of Passage” to Disgrace for the Pharma companies? Profitability through Simplicity, October 16, 2019

7.     Malhotra, Girish: ONE PAGE Road Map to Reduce Drug Shortages, Assure Quality and Improve Affordability, Profitability through Simplicity, December 6, 2019

8.     Quality by Design for ANDAs, FDA.gov, Accessed March 26, 2020

GDFUA II ANDA (Abbreviated New Drug Application) Review Target of 8-10 Months should be a Cause of Concern

Understanding what it takes to file and get approval of any ANDA from US FDA is a great question and the answers are enlightening.

Practical impact of GDUFA II is that generic drug sponsors can expect to have their ANDAs reviewed and responded to within ten months of submission. If the review does not result in approval, the sponsor will receive a Complete Response Letter (CRL) which compiles a list of major issues the Agency has found with the application. The sponsor must rectify each deficiency before resubmitting the amended ANDA for another review cycle ⁽¹⁾. Word “review” does not mean “approval” and that can mean that the generic drug approval can still be wandering in halls of FDA. Based on this one has to wonder what is the purpose of the exercise. This is frightening and can make us all wonder “can US react to national security challenges posed by drug shortages and affordability”.  

I tried to find out how much real time it takes to get an ANDA approved. I was confident that someone at FDA can give an answer. Unfortunately I did not succeed. That in itself is a sad story. It is probably less painful to walk over bed of hot coals than spend time trying to get answer the subject question. No pun intended. There is no financial relationship with any for profit or non-profit organization.

I tried to find a flow diagram that will tell me/us a simple pathway and time gap between events. Unfortunately, I could not. Using testimony FDA documentation and suggested pathway, I have tried to create a simple schematic Figure 1^{(2,3,4,5, 6)}.  

GDUFA related information repeatedly suggest that ANDA would be reviewed in 8-10 months but does not give the total time it takes to get ANDA approved. Not having an example of average time it takes an applicant to get an approval is not very comforting. With this uncertainty I wonder can how bureaucracy of GDUFA instill competition in generic drugs, make drugs affordable and bring manufacturing jobs to US ⁽⁷⁾. Additional question can be “can FDA address US national security issues to alleviate dependence of generic drugs on other countries”. Based on published information, many will have serious doubts. 

Figure 1: ANDA Time Line

Review of following references each reader can draw their own conclusions. Testimony ⁽³⁾ of Directors of CDER, CBER, and CDAH, - Janet Woodcock, M.D., Director, Center for Drug Evaluation and Research; Peter Marks, M.D., Ph.D., Director, Center for Biologics Evaluation and Research; Jeffrey Shuren, M.D., J.D., Director, Center for Devices and Radiological Health, Food and Drug Administration, U.S. Department of Health and Human Services (HHS) Figure 4 highlights first cycle approvals but does not give the actual numbers and the time period, a critical element. Figure 3 ⁽³⁾ shares relative number of meetings held. That clearly suggests that FDA has not clearly stated what it needs to get ANDA approved. 

Figure 8 in reference ⁽³⁾ touts number 835 ANDAs (approvals and tentative approvals) but does not reveal how much total time they took. Number for 2016 approvals is high. Question “were the numbers coincidentally stacked for 2016?”. Proof of the pudding is how many approvals are done in 90 days from the date of ANDA filing. This should the new normal ^{(5, 6, 7, 8)} we should expect. All kinds of numbers have been shared in this testimony ⁽³⁾ but the question is do they have any relevance when it comes getting the products to the patients by reducing time from ANDA application filing to their approval. One could call this busy work or self-appreciation. Essentially FDA has enslaved the pharmaceutical industry to dictate what and how of review and approvals. They even tell industry which methodologies and technologies they should use when they have not produced any product. 

GDUFA documents talk about application review time but no one shares or talks about how much real time (months) it takes from the day application arrives at FDA to get the review completed and application approved. That is a hidden secret and my conjecture is that no one has the real answer. ANDA approval time is most crucial and valuable answer as it influences availability and affordability of generic drugs.

Considerable effort was made trying to find out if there is a simple map (similar to Figure 1) for ANDA filings and approvals which will show ANDA filers do’s and don’ts of filing. Except for a simple road map one finds overwhelming volume of paper work one has to follow for any submission, try to master but still fail. 

The paper work and the shear bureaucracy for filing ANDA and for that matter NDAs also will essentially enslave every company. My conjecture is that as structured presently there is no single reviewer at FDA who knows what makes an application complete and is necessary for ANDA approval. Instead of companies having a template and telling companies what FDA needs to file/approve an ANDA each company’s application is reviewed by multitude and that is like being fitted by many to get a tailormade suit that needs repeated alterations.  

If all the referenced documents ^{(4, 5, 6,11, 12)} are printed and reviewed, it will take an army of chemists, chemical engineers, outside consultants and lawyers to figure out what all is needed for ANDA application approval. Poor chemist and chemical engineer who developed, designed and commercialized a process to produce quality product from the get go has no say in the exercise. They mastered their process and methods to create a quality product all the time is critiqued and subjected to second guesses and torture. They are being told to exercise QbD (quality by design), which they do. However, the regulators who create an approval pathway and should be model of QbD, believe in QbA (quality by analysis/aggravation) thorough pre, middle and post mortem meetings to review/approve every submission. I wonder how much hands-on experience reviewers have in process development, design, commercialization and managing any drug API manufacturing or their formulation.      

If FDA had template/s that can be used by companies, ANDA filing and review process ^(7,8,9,10) could be smoothed out to minimize approval time. They could be used to simplify NDA approval time also. Such simplification is necessary for self-reliance and manufacturing bringing jobs back to the United States to relieve its dependency on others specially with incentive of 30 day approval ⁽⁵⁾.

Let us hope that the ANDA related meetings with FDA are not a fertile ground for data manipulation that rear their ugly head during onsite inspections resulting in 483 citations ⁽¹³⁾ which are worthless as they have no impact on company. 

Prolonged ANDA review and approval processes have to be stopped as such adventures increase generic prices, reduce competition and put The United States strategically in a very vulnerable position and dependent on others ⁽⁷⁾. In addition, delays of months increase cost of drugs which is passed to patients. This is unacceptable. Question to FDA and the US Government is “Is the current vulnerability acceptable?” Most will say NO. What do you think? 

Girish Malhotra, PE

EPCOT International

1. How GDUFA II Impacts the Timing & Approval Process for Generic Drug Sponsors, Weinberg Group, Accessed March 23, 2020
2. Pre ANDA Program, Accessed March 23, 2020
3. Prescription Drug User Fee Act Reauthorization (PDUFA VI), Medical Device User Fee Act Reauthorization (MDUFA IV), Generic Drug User Fee Act Reauthorization (GDUFA II), Biosimilar User Fee Act Reauthorization (BsUFA II) Accessed November 25, 2018
4. Sherwood, Edward, GDUFA II Training - Goals October 25, 2017
5. Sherwood, Edward, Sansone, Vincent: FDA’s Generic Drug Program Offers Assistance, Resources For ANDA Applicants Pharmaexec.com, November 5, 2019, Accessed March 23, 2020
6. Sansone, Vincent: GDUFA II Performance Goals, FDA.gov, Accessed March 23, 2020
7. Malhotra, Girish: Strategies to Increase Generic Drug Competition and Bring Manufacturing to The United States of America, Profitability through Simplicity, March 16, 2020
8. Malhotra, Girish: Can the Review and Approval Process for ANDA at US FDA be Reduced from Ten Months to Three Months?Profitability through Simplicity, http://bit.ly/33SiqHS  March 25, 2017
9. Malhotra, Girish: http://bit.ly/31ALUcu What Is Needed for a Regulatory Approval of NDA/ANDA Filings in 90 Days? Profitability through Simplicity, October 24, 2018
10. Malhotra, Girish: ONE PAGE Road Map to Reduce Drug Shortages, Assure Quality and Improve Affordability: Profitability through Simplicity, December 6, 2019
11.  Abbreviated New Drug Application (ANDA), Accessed March 23, 2020
12. Filing Review of Abbreviated New Drug Applications, Accessed March 23, 2020
13. Malhotra, Girish: Are US FDA 483 Citations a "Medal of Honor" or “Rite of Passage” to Disgrace for the Pharma companies? Profitability through Simplicity, October 16, 2019

Can the Review and Approval Process for ANDA at USFDA be Reduced from Ten Months to Three Months?

Not having been involved with regulatory filing aspects of pharmaceuticals, reviewing Generic Drug User Fee Act Reauthorization (GDUFA II) ⁽¹⁾ was educational. After review my process simplification instincts kicked in. If the current approval time line can be reduced from TEN months to THREE months, impact of the process will be lower drug costs.

Reading joint testimony of Drs. Woodcock, Marks and Shuren ⁽²⁾ and having had time to review the application process, reinforced my thinking that a time reduction is possible but to get there industry along with USFDA would have to practice what chemical engineers and chemists are taught and asked to practice for every manufacturing process they develop, design and commercialize i.e. produce quality first time and all the time. In terms of FDA’s vocabulary the filling and review processes would have to follow QbD (Quality by Design) practices. FDA will have to follow what it has been asking the industry to practice. Industry will also have to follow suit. I believe industry will also get hands on practice about QbD and it will trickle through the whole organization, a win-win.

Many associated and proficient with regulatory filings would categorically say that filings are not a manufacturing process and such a time reduction is impossible and cannot be done. Currently filing an application is a task that is repeated by many to create quality application. It will generate higher profits for the filer if they can reduce its approval time. It can be continuously improved and deserves our attention. We improve every repetitive task to facilitate our daily lives. So why not improve the FDA ANDA (abbreviated new drug application) application filing and approval process? Improvements here could have far reaching impact for other filings also.

I firmly believe that such a time reduction is possible but many things will have to change to get there. Our thinking and work philosophy has to change. In the current application process following challenges ⁽¹⁾ have been identified. Each challenge is reviewed.

• Submission completeness: It takes about four review cycles to approve ANDA.
• Volume of applications
• Other factors. Several factors delay timely consumer access.



a) Risk Evaluation and Mitigation Strategies are used by Brand companies to delay generic entry



b) Delaying or denying generic companies’ access to reference listed drug products, thereby preventing companies from conducting studies required for approval



c) Misuse of FDA’s citizen petition process as a means to block generic approvals. 


d) FDA generally cannot approve generics until patent and exclusivity on the innovator product expire. Patent litigation and other legal challenges can frustrate timely approval. 

Submission Completeness:

In March 2, 2017 testimony Pre-ANDA program is suggested. I believe that is the most brilliant idea for filing application and reducing time. It is a step QbD implementation of the application filing process.

“About four reviews” needed for FDA application is equal to FDA using four iterations to have a quality application. Current method to get to an acceptable product (application) is a QbA (Quality by Analysis) practice. I equate QbA to “Quality by Aggravation”.

FDA also has to practice what it is suggesting companies to follow. Quoting FDA “This guidance ⁽³⁾ describes the concept that quality cannot be tested into products; (ANDA application, to me is a product of FDA’s work), in other words, it should be built-in or should be present by design.”

Yes like manufacturing processes, applications for every product are going to be different when it comes to content but the information filing requirements are essentially going to be same. I believe a template application that covers better than 90% of the filing requirements can be designed. A standard application format could pare down four reviews to a single review and completeness. This would be a monumental accomplishment. If accomplished, we will automatically see the approval time reduction.

Currently it can take up to 45 days for the FDA reviewing team to determine completeness of the application. FDA would have to figure out how this time can be reduced to 15 days. Current review practices would have to be modified. Long delays suggest that the filing team does not understand FDA’s QbD expectations or FDA has not relayed them to applicants.

FDA has to create applications that clearly state what it expects from the companies. A standard template has to be created. It's possible that the current templates do not relay FDA expectations. A redesign may be necessary. Once these applications are designed, companies and FDA staff can be trained to follow the process. Workshops could be held on a regular basis to train industry to what is needed.

I know such processes work. We had similar processes at Illinois EPA in 1972 for various industry segments. We had timelines from submission to approval of equipment design and operating permits. Based on our questions, every industry submitted relevant information that facilitated review and approval. FDA may have to benchmark to see which government agency has the best application review and approval process. Elements can be incorporated.

Another important aspect of the filing process would be to involve the engineers and chemists who have created and commercialized the process so the filled application is complete and represents a quality (QbD) filing. It means that the companies have to do their homework. They know their processes the best.

Every effort has to be made to pare ten months to 90 days. It is a doable challenge.

Volume of Applications:

FDA can go with best basis planning scenario and deal with ups and downs of the numbers. Ability to deal with such changes will be its operational finesse strategy. Many businesses deal with such scenarios. Most likely I have oversimplified the situation.

Other Factors:

*    Risk Evaluation and Mitigation Strategies are used by Brand companies to delay generic entry. 



FDA has to develop a program or strategy to prevent such harassment. Roadblock could be set but there has to be a resolution that is acceptable to each side. Generics have to be on top of their game to counter such delay tactics. Legislatorial changes might have to be incorporated. In our political system that could be a challenge.

*       Delaying or denying generic companies’ access to reference listed drug products, thereby preventing the companies from conducting studies required for approval.

Congressional intervention might be needed. USP or others who have information should be able to share the information. Congress can create a scenario to assure necessary samples are available for the generics. This would be good for their constituents. I believe FDA can intervene also.

*       Misuse of FDA’s citizen petition process as a means to block generic approvals. 



If the brand companies are abusing citizen’s petition process, there has to be a counter strategy from the generics. I have not looked at this in detail but I am sure that there are ways and means to counter this challenge.

*      FDA generally cannot approve generics until patent and exclusivity on the innovator product expire. Patent litigation and other legal challenges can frustrate timely approval. 



Generic filers have to develop their strategies. I believe if the approval time is lowered from ten months to 90 days, companies could develop workable measures. Filing company has to have a complete grasp of the situation and strategies.

If the approval process is lowered from ten months to 90 days, need for priority review most likely could disappear.

Breakdown of 90 Day Time:

I would break the 90 days in three segments. Initial review has to be completed by FDA in 15 days from acceptance of the initial application. FDA has to provide the company deficiencies of the application. Incomplete application could be rejected. Companies will have 30 days to respond FDA’s requirements. FDA would have 45 days after corrections, more than sufficient time, to review and interact with the company and act on the application.

If for some reasons the company is not able to fulfill its obligation after the initial 15 day FDA review and complete its deficiencies 30 days, they could stand to loose its application and would have to start over again. With such a possibility, it would be in the best interest of all parties to have quality application from the get go. It will be a QbD win for all.

It is very possible that facility inspections could be an encumbrance in the approval process. However, having command of the designed process would be reflected in the application. If it were not that would mean that the designed and operating process is different from the filled information. It would be tantamount to falsification of information and it should be used to ban the company from shipping products to the US market. 

What I am suggesting might be a challenge but until we take on challenges progress is never made. By posting this blog I am not questioning authority of FDA or any other government body but just presenting an alternate perspective that would bring generics to the market quicker and lower healthcare costs. I might also be incorrect in my conjectures and expectations but it would be worth if we can make an improvement and lower drug costs.

Girish Malhotra, PE

President

EPCOT International 


1.  Generic Drug User Fee Act Reauthorization (GDUFA II) Accessed March 16, 2017
2. Testimony of Drs. Woodcock, Marks and Shuren Accessed March 23, 2017
3. Advancement of Emerging Technology Applications to Modernize the Pharmaceutical Manufacturing Base Guidance for Industry Accessed March 24, 2017