TREA

Method and apparatus for aseptic packaging

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Information

  • Patent Grant
  • 6536188
  • Patent Number
    6,536,188
  • Date Filed
    Thursday, May 6, 1999
    25 years ago
  • Date Issued
    Tuesday, March 25, 2003
    21 years ago
Information
Abstract
A method and apparatus for providing aseptically processed low acid products in a container having a small opening, such as a glass or plastic bottle or jar, at a high output processing speed.
Description




FIELD OF THE INVENTION




The present invention relates generally to systems for the aseptic packaging of food products. More particularly, the present invention relates to an aseptic packaging system for the aseptic packaging of food products in containers such as bottles or jars.




BACKGROUND OF THE INVENTION




Sterilized packaging systems in which a sterile food product is placed and sealed in a container to preserve the product for later use are well known in the art. Methods of sterilizing incoming containers, filling the containers with pasteurized product, and sealing the containers in an aseptic tunnel are also known.




Packaged food products can generally be categorized as high acid products (Ph below 4.5) or low acid products (Ph of 4.5 and above). The high acid content of a high acid product helps to reduce bacteria growth in the product, thereby increasing the shelf life of the product. The low acid content of a low acid product, however, necessitates the use of more stringent packaging techniques, and often requires refrigeration of the product at the point of sale.




Several packaging techniques, including extended shelf life (ESL) and aseptic packaging, have been developed to increase the shelf life of low acid products. During ESL packaging, for example, the packaging material is commonly sanitized and filled with a product in a presterilized tunnel under “ultra-clean” conditions. By using such ESL packaging techniques, the shelf life of an ESL packaged product is commonly extended from about 10 to 15 days to about 90 days. Aseptic packaging techniques, however, which require that the packaging take place in a sterile environment, using presterilized containers, etc., are capable of providing a packaged product having an even longer shelf life of 150 days or more. In fact, with aseptic packaging, the shelf life limitation is often determined by the quality of the taste of the packaged product, rather than by a limitation caused by bacterial growth.




For the aseptic packaging of food products, an aseptic filler must, for example, use an FDA (Food and Drug Administration) approved sterilant, meet FDA quality control standards, use a sterile tunnel or clean room, and must aseptically treat all packaging material. The food product must also be processed using an “Ultra High Temperature” (UHT) pasteurization process to meet FDA aseptic standards. The packaging material must remain in a sterile environment during filling, closure, and sealing operations.




Many attempts have been made, albeit unsuccessfully, to aseptically fill containers, such as bottles or jars having small openings, at a high output processing speed. In addition, previous attempts for aseptically packaging a low acid product in plastic bottles or jars (e.g., formed of polyethylene terepthalate (PET) or high density polyethylene (HDPE)), at a high output processing speed, have also failed. Furthermore, the prior art has not been successful in providing a high output aseptic filler that complies with the stringent United States FDA standards for labeling a packaged product as “aseptic.” In the following description of the present invention, the term “aseptic” denotes the United States FDA level of aseptic.




SUMMARY OF THE INVENTION




In order to overcome the above deficiencies, the present invention provides a method and apparatus for providing aseptically processed low acid products in a container having a small opening, such as a glass or plastic bottle or jar, at a high output processing speed.




Many features are incorporated into the aseptic processing apparatus of the present invention in order to meet the various United States FDA aseptic standards and the


3


A Sanitary Standards and Accepted Practices.




The aseptic processing apparatus of the present invention uses filtered air to maintain a positive pressure within a filler apparatus. The filler apparatus includes a sterile tunnel that is pressurized to a level greater than atomospheric pressure using filtered sterile air. The filler apparatus includes three interfaces with the ambient environment, each of which eliminates the possibility of external contamination. The first interface is where containers first enter the sterile tunnel through a bottle infeed and sterilization apparatus. In accordance with the present invention, there is always an outflow of aseptic sterilant (e.g., hydrogen peroxide) enriched sterile air from the first interface to prevent contaminants from entering the sterile tunnel. The second interface with the sterile tunnel is the path where incoming lid stock enters a lid sealing and heat sealing apparatus. To prevent contamination, the lid stock passes through a hydrogen peroxide bath that provides an aseptic barrier for any contaminants that enter the sterile tunnel through the second interface. The third interface with the sterile tunnel is at an exit opening of a discharge apparatus where sealed containers leave the sterile tunnel. Positive sterile air pressure within the sterile tunnel ensures that sterile air is continuously flowing out of the exit opening of the discharge apparatus, thereby preventing contaminants from entering the sterile tunnel through this interface.




The aseptic processing apparatus includes a conveying apparatus for transporting the containers through a plurality of processing stations located within the sterile tunnel. The entire conveying apparatus is enclosed within the sterile tunnel, and is never is exposed to unsterile conditions.




The interior surface of a container such as a bottle or jar is much more difficult to aseptically sterilize than the interior surface of a cup. A cup generally has a large opening compared to its height, whereas a bottle or jar generally has a small opening compared to its height and its greatest width (e.g., the ratio of the opening diameter to the height of the container is less than 1.0). A sterilant can be introduced, activated, and removed in a cup much more rapidly than in a bottle or jar. The processing speed when using a bottle or jar is limited, in part, by the time required to aseptically sterilize the interior surface of the bottle or jar. The aseptic processing apparatus of the present invention overcomes the processing speed limitations associated with the use of containers such as bottles or jars.




A high output processing speed is achieved in the present invention by applying a hot atomized sterilant, such as a hydrogen peroxide spray onto the interior surface of each container, and by subsequently activating and removing the sterilant in a plurality of drying stations using hot sterile air. For example hydrogen peroxide breaks down into water and oxygen, and thus oxidizes and kills bacteria within the container. To achieve aseptic sterilization, a minimum container temperature is developed and held for a predetermined period of time (e.g., 131° F. for 5 seconds) after application of the sterilant. Hot sterile air is delivered at a high volume and a relatively low temperature to dry the container and to prevent the container (if formed of plastic) from being heated to its softening temperature. After container drying, the residual hydrogen peroxide in the container is below a predetermined level (e.g., about 0.5 PPM (parts per million)).




The present invention generally provides a method for aseptically bottling aseptically sterilized foodstuffs comprising the steps of:




providing a plurality of bottles;




aseptically disinfecting the plurality of bottles;




aseptically filling the aseptically disinfected plurality of bottles with the aseptically sterilized foodstuffs; and




filling the aseptically disinfected plurality of bottles at a rate greater than 100 bottles per minute.




The present invention additionally provides a method for aseptically bottling aseptically sterilized foodstuffs comprising the steps of:




providing a plurality of bottles;




aseptically disinfecting the bottles at a rate greater than 100 bottles per minute; and




aseptically filling the bottles with aseptically sterilized foodstuffs.











BRIEF DESCRIPTION OF THE DRAWINGS




The features of the present invention will best be understood from a detailed description of the invention and a preferred embodiment, thereof selected for the purposes of illustration, and shown in the accompanying drawings in which:





FIG. 1

is a plan view of an aseptic processing apparatus in accordance with a preferred embodiment of the present invention;





FIG. 2

is a side view of the aseptic processing apparatus of

FIG. 1

;





FIG. 3

is a partial cross-sectional side view of the aseptic processing apparatus of

FIG. 1

;





FIG. 4

is a cross-sectional side view of a bottle infeed and sterilization apparatus;





FIG. 5

illustrates a cross-sectional top view of the bottle infeed and sterilization apparatus taken along line


5





5


of

FIG. 4

;





FIG. 6

is an interior sectional view of an interior wall taken along line


6





6


of

FIG. 4

;





FIG. 7

is a cross-sectional view of the bottle infeed and sterilization apparatus taken along line


7





7


of

FIG. 4

;





FIG. 8

is a perspective view of a conveying plate for use in the aseptic processing apparatus of the present invention;





FIG. 9

is a perspective view of a partition in a sterile tunnel;





FIG. 10

is a cross-sectional side view of an interior bottle sterilization apparatus and the partition located between stations


8


and


9


;





FIG. 11

is a cross-sectional side view of the partition located between stations


22


and


23


;.





FIG. 12

is a cross-sectional side view of the partition located between stations


35


and


36


;





FIG. 13

is a cross-sectional side view of a lid sterilization and heat sealing apparatus;





FIG. 14

is a side view of a lifting apparatus with a gripper mechanism for lifting the bottles from the sterile tunnel;





FIG. 15

is a top view of the aseptic processing apparatus; and





FIG. 16

is a side view of the aseptic processing apparatus indicating the control and monitoring locations that are interfaced with a control system.











DETAILED DESCRIPTION OF THE INVENTION




Although certain preferred embodiments of the present invention will be shown and described in detail, it should be understood that various changes and modifications may be made without departing from the scope of the appended claims. The scope of the present invention will in no way be limited to the number of constituting components, the materials thereof, the shapes thereof, the relative arrangement thereof, etc., and are disclosed simply as an example of the preferred embodiment. The features and advantages of the present invention are illustrated in detail in the accompanying drawings, wherein like reference numerals refer to like elements throughout the drawings. Although the drawings are intended to illustrate the present invention, the drawings are not necessarily drawn to scale.




The present invention provides an aseptic processing apparatus


10


that will meet the stringent FDA (Food and Drug Administration) requirements and


3


A Sanitary Standards and Accepted Practices required to label a food product (foodstuffs) as “aseptic”. Hereafter, “aseptic” will refer to the FDA level of aseptic. The present invention provides a method and apparatus for producing at least about a 12 log reduction of


Clostridium botulinum


in food products. In addition, the present invention produces packaging material with at least about a 6 log reduction of spores. Actual testing of the aseptic processing apparatus is accomplished with spore test organisms. These test organisms are selected on their resistance to the media selected used to achieve sterility. For example, when steam is the media, the test organism is


Bacillus stearothermophilus.


When hydrogen peroxide is the media, then the test organism is


Bacillus subtilis


var.


globigii.






The present invention processes containers such as bottles or jars that have a small opening compared to its height and its greatest width (e.g., the ratio of the opening diameter to the height of the container is less than 1.0). In the preferred embodiment, a bottle


12


(see, e.g.,

FIG. 8

) is illustrated as the container. The container may alternately comprise a jar. The bottle


12


is preferably formed of a plastic such as polyethylene terepthalate (PET) or high density polyethylene (HDPE), although other materials such as glass may also be used. The present invention uses an aseptic sterilant such as hydrogen peroxide (H


2


O


2


) or oxonia to sterilize the bottles


12


. In the preferred embodiment of the present invention, hydrogen peroxide is used as the sterilant. The present invention uses hydrogen peroxide with a concentration of less than about 35% and ensures that the bottles


12


have less than about 0.5 ppm of residual hydrogen peroxide after each bottle


12


is sterilized.





FIGS. 1-3

illustrate several views of an aseptic processing apparatus


10


in accordance with a preferred embodiment of the present invention. As shown, the aseptic processing apparatus


10


includes a first bottle unscrambler


20


, a second bottle unscramble


30


, and a bottle lifter


40


for providing a supply of properly oriented empty bottles. The empty bottles are delivered to a filler apparatus


50


after passing through a bottle infeed and sterilization apparatus


60


for aseptic sterilization. The filled bottles are sealed at a first capping apparatus


400


or a second capping apparatus


410


. A control system


550


monitors and controls the operation of the aseptic processing apparatus


10


. The filled and sealed bottles are packed and palletized using a first case packing apparatus


480


, a second case packing apparatus


490


, a first palletizer


500


, and a second palletizer


510


.




The bottles


12


arrive at a first bottle unscrambler


20


with a random orientation, such that an opening


16


(see

FIG. 8

) of each bottle


12


can be oriented in any direction. The first bottle unscrambler


20


manipulates the bottles


12


until the opening


16


of each bottle


12


is in a top vertical position. The bottles


12


leave the first bottle unscrambler


20


in a series formation with the opening


16


of each bottle


12


oriented vertically. The bottles


12


travel in single file in a first lane


18


to a first bottle lifter


40


. The first bottle lifter


40


lifts and transports the bottles


12


to a bottle infeed and sterilization apparatus


60


. A second bottle unscrambler


30


may also used to provide a supply of vertically oriented bottles


12


. The bottles


12


output from the second bottle unscrambler


30


travel in single file in a second lane


22


to a second bottle lifter


42


, which lifts and transports the bottles


12


to the bottle infeed and sterilization apparatus


60


.





FIG. 3

illustrates the bottle infeed, sterilization, and conveying apparatus


60


attached to the filler apparatus


50


.

FIG. 4

illustrates a cross-sectional side view of the bottle infeed, sterilization, and conveying apparatus


60


.

FIG. 5

illustrates a cross-sectional top view of the bottle infeed, sterilization, and conveying apparatus


60


taken along line


5





5


of FIG.


4


. The bottle infeed and sterilization apparatus


60


preferably inputs six bottles


12


in a horizontal direction from the first lane


18


and six bottles in a horizontal direction from the second lane


22


(FIG.


5


). A gate


76


in the first lane


18


selectively groups six bottles


12


at a time in first horizontal row


24


. A gate


78


in the second lane


22


selectively groups six bottles


12


at a time in a second horizontal row


28


. An infeed apparatus


80


includes a pushing element


84


for pushing the bottles


12


in the first horizontal row


24


into a first vertical lane


26


. A corresponding infeed apparatus


80


includes a pushing element


86


for pushing the bottles


12


in the second horizontal row


28


into a second vertical lane


32


. The six bottles


12


in the first vertical lane


26


and the six bottles


12


in the second vertical lane


32


are directed downward into the bottle infeed and sterilization apparatus


60


.




Referring to

FIG. 4

, as the bottles


12


move downward in the first vertical lane


26


and the second vertical lane


32


, a sterilant


14


, such as heated hydrogen peroxide, oxonia, or other aseptic sterilant, is applied to an outside surface


34


of each bottle


12


by a sterilant application apparatus


36


. The outside surface


34


of a bottle


12


is illustrated in greater detail in FIG.


8


. The bottles


12


may move downward in the first vertical lane


26


and the second vertical lane


32


by the force of gravity. Alternatively, controlled downward movement of the bottles


12


can be created by the use of a conveying device such as a moving conveying chain. A plurality of pins are attached to the conveying chain. Each bottle


12


rests on one of the pins attached to the conveying chain. Therefore, the motion of each bottle is controlled by the speed of the moving conveying chain.




A sterilant such as hydrogen peroxide may be provided to the sterilant application apparatus


36


in many ways. For example, liquid hydrogen peroxide may be provided in a reservoir at a level maintained by a pump and overflow pipe. A plurality of measuring cups (e.g., approximately 0.5 ml each) connected by an air cylinder are submerged into the reservoir and are lifted above the liquid level. Thus, a measured volume of liquid hydrogen peroxide is contained in each measuring cup.




Each measuring cup may include a conductivity probe that is configured to send a signal to the control system


550


indicating that the measuring cup is full. A tube (e.g., having a diameter of about {fraction (1/16)}″) is positioned in the center of the measuring cup. A first end of the tube is positioned near the bottom of the measuring cup. A second end of the tube is connected to the sterilant application apparatus


36


. The sterilant application apparatus


36


includes a venturi and a heated double tube heat exchanger. When the measuring cup is full, and a signal is received from the control system


550


, a valve is opened allowing pressurized sterile air to enter the venturi. The pressurized air flow causes a vacuum to be generated in second end of the tube causing liquid hydrogen peroxide to be pulled out of the measuring cup. The liquid hydrogen peroxide is sprayed into a sterile air stream which atomizes the hydrogen peroxide into a spray. The atomized hydrogen peroxide enters the double tube heat exchanger in order to heat the atomized hydrogen peroxide to its vaporization phase. The double tube heat exchanger is heated with steam and the temperature is monitored and controlled by the control system


550


. In

FIG. 4

, the application of the sterilant


14


by the sterilant application apparatus


36


is accomplished through the use of spray nozzles


64


that produce a sterilant fog which is directed to the outside surface


34


of each bottle


12


.




Alternatively, a direct spray of heated hydrogen peroxide may be continuously applied to the outside surface


34


of each bottle


12


. For producing the direct spray, a metering pump regulates the amount of hydrogen peroxide, a flow meter continuously measures and records the quantity of hydrogen peroxide being dispensed, a spray nozzle produces a fine mist, and a heat exchanger heats the hydrogen peroxide above the vaporization point.





FIGS. 3 and 4

illustrate the sterilization chamber


38


for activation and drying of bottles


12


which is included in the bottle infeed, sterilization, and conveying apparatus


60


. The sterilization chamber


38


sterilizes the outside surface


34


of each bottle


12


. The sterilization chamber


38


encloses a conduit


39


. Sterile heated air, which is generated by a sterile air supply system


146


(FIG.


3


), enters the conduit


39


of the sterilization chamber


38


through ports


64


and


68


located at the bottom of the sterilization chamber


38


. The sterile heated air also enters through a bottom opening


62


of the bottle infeed and sterilization apparatus


60


. The sterile heated air travels up through the conduit


39


of the sterilization chamber


38


, and exits the top of the sterilization chamber


38


through an exhaust conduit


70


. The sterile heated air continuously flows in an upward direction through the sterilization chamber


38


, thus preventing any contaminants from entering the bottle infeed and sterilization apparatus


60


. To create the sterile heated air, the air is first passed through a filtering system (e.g., a group of double sterile air filters) to sterilize the air. The air is then heated in a heating system (e.g., an electric heater) to about 230° F. The air temperature is regulated by the control system


550


. Other techniques for providing the sterile heated air may also be used. The control system


550


monitors the air pressure and flow rate of the sterile heated air to ensure that an adequate flow of the hot sterile air is maintained in the bottle sterilization chamber


38


of the bottle infeed and sterilization apparatus


60


.




As illustrated in

FIGS. 4

,


6


, and


7


, the sterilization chamber


38


includes two opposing, interior, perforated walls


72


A,


72


B. The perforated walls


72


A and


72


B guide the bottles


12


downward in the first vertical lane


26


and the second vertical lane


32


, respectively. The perforated walls


72


A,


72


B also allow the complete circulation of hot sterile air around the outside surface


34


of each bottle


12


in the sterilization chamber


38


. The sterilization chamber


38


supplies hot sterile air to the outside surface


34


of each bottle


12


between the sterilant application apparatus


36


and the bottom opening


62


of the bottle infeed and sterilization apparatus


60


. This sterilant may be hydrogen peroxide or oxonia (hydrogen peroxide and peroxyacetic acid).




In accordance with the preferred embodiment of the present invention, twelve drying positions are provided in the sterilization chamber


38


. Each bottle


12


is exposed to the hot sterile air in the sterilization chamber


38


for about at least 24 seconds. This provides time sufficient time for the hydrogen peroxide sterilant to break down into water and oxygen, to kill any bacteria on the bottles


12


, and to evaporate from the outside surface


34


of the bottles


12


.




An exhaust fan


73


is located at a top of the exhaust conduit


70


to provide an outlet from a sterile tunnel


90


, and to control the sterile air flow rate through the sterilization chamber


38


. The exhaust fan


73


is controlled by the control system


550


. The control system


550


controls the sterile air temperature preferably to about 230° F., and controls the sterile air flow rate through the sterilization chamber


38


. The flow rate is preferably about 1800 scfm through the sterilization chamber


38


. The bottles


12


leave the sterilization chamber


38


with a hydrogen peroxide concentration of less than 0.5 PPM.




As shown in

FIGS. 3 and 4

, a plurality of proximity sensors


71


located along the sides of the vertical lanes


26


,


32


detect any bottle


12


jams that occur within the sterilization chamber


38


. The proximity sensors


71


transmit an alarm signal to the control system


550


. The bottles


12


leave the bottle infeed and sterilization apparatus


60


through the bottom opening


62


, and enter the sterile tunnel


90


of the filler apparatus


50


.




In the preferred embodiment of the present invention, the filler apparatus


50


includes forty-one (41) index stations


92


, hereafter referred to as “stations.” Various index stations


92


are illustrated in

FIGS. 3

,


4


, and


11


-


15


. The conveying motion of the bottles


12


to the various stations


92


through the filler apparatus


50


is based on an indexing motion. The filler apparatus


50


is designed to convey the bottles


12


through the various operations of the filler


50


in a two by six matrix. The twelve bottles


12


in the two by six matrix are positioned in, and displaced by, a conveying plate


94


as illustrated in FIG.


8


. Therefore, twelve bottles


12


are exposed to a particular station


92


at the same time. A conveying apparatus


100


moves the set of twelve bottles


12


in each conveying plate


94


sequentially through each station


92


.




Referring to

FIGS. 3 and 4

, the bottles


12


are supplied from an infeed chamber


102


to station


2


of the filler apparatus


50


through the bottom opening


62


of the bottle infeed and sterilization apparatus


60


. The infeed chamber


102


is enclosed to direct heated hydrogen peroxide laden air completely around the outer surface


34


of the bottles


12


. A mechanical scissors mechanism and a vacuum “pick and place” apparatus


104


position twelve bottles


12


at a time (in a two by six matrix,

FIG. 8

) into one of the conveying plates


94


.




A plurality of conveying plates


94


are attached to a main conveyor


106


. The main conveyor


106


forms a continuous element around conveyor pulleys


108


and


110


as illustrated in

FIG. 3. A

bottle support plate


107


supports a bottom


120


of each bottle


12


as the bottles


12


are conveyed from station to station through the filler apparatus


50


. Each conveying plate


94


passes through stations


1


through


41


, around pulley


108


, and returns around pulley


110


to repeat the process. The main conveyor


106


, conveying plates


94


, and pulleys


108


and


110


are enclosed in the sterile tunnel


90


.




At station


4


, the bottles


12


in the conveying plate


94


enter a bottle detection apparatus


112


. The bottle detection apparatus


112


determines whether all twelve bottles


12


are actually present and correctly positioned in the conveying plate


94


. Proximity sensors


114


detect the presence and the alignment of each bottle


12


. In the present invention, a bottle


12


with correct alignment is in an upright position with the opening


16


of the bottle


12


located in an upward position. Information regarding the location of any misaligned or missing bottles


12


is relayed to the control system


550


. The control system


550


uses this location information to ensure that, at future stations


92


, bottle filling or sealing will not occur at the locations corresponding to the misaligned or missing bottles


12


.




At station


7


, as illustrated in

FIGS. 3 and 10

, the bottles


12


in the conveying plate


94


enter an interior bottle sterilization apparatus


116


. A sterilant, such as hydrogen peroxide, oxonia, or any other suitable aseptic sterilant is applied as a heated vapor fog into the interior


118


of each bottle


12


. Preferably, hydrogen peroxide is used as the sterilant in the present invention. The application of sterilant is accomplished with the use of a plurality of sterilant measuring devices


120


and applicator spray nozzles


122


. A separate measuring device


120


and applicator spray nozzle


122


are used for each of the twelve bottle


12


locations in the conveying plate


94


. Each bottle


12


is supplied with the same measured quantity of sterilant, preferably in the form of a hot vapor fog. The measured quantity of sterilant may be drawn from a reservoir


124


of sterilant, heated, vaporized, etc., in a manner similar to that described above with regard to the sterilant application apparatus


36


.




The control system


550


monitors and controls a spray apparatus


126


that includes the applicator spray nozzles


122


. Each applicator spray nozzle


122


sprays the sterilant into the interior


118


of a corresponding bottle


12


as a hot vapor fog. The applicator spray nozzles


122


are designed to extend through the bottle openings


16


. The applicator spray nozzles


122


descends into the interior


118


and toward the bottom of the bottles


12


. This ensures the complete application of sterilant to the entire interior


118


and interior surface


119


of each bottle


12


. Alternately, the applicator spray nozzles


122


may be positioned immediately above the bottle openings


16


prior to the application of sterilant.





FIG. 9

illustrates a perspective view of a partition


130


that provides control of sterile air flow within the sterile tunnel


90


of the filler apparatus


50


. The partition


130


includes a top baffle plate


132


, a middle baffle plate


134


, and a bottom baffle plate


136


. The top baffle plate


132


and the middle baffle plate


134


are provided with cut-outs


133


which correspond to the outer shape of each bottle


12


and to the outer shape of the conveyor plate


94


. The cut-outs


133


allow each bottle


12


and each conveyor plate


94


to pass through the partition


130


. A space


138


between the middle baffle plate


134


and the bottom baffle plate


136


allows each empty conveyor plate


94


to pass through the partition


130


as it travels on its return trip from the pulley


108


toward the pulley


110


.




As illustrated in

FIG. 3

, partitions


130


A,


130


B, and


130


C, are located within the sterile tunnel


90


.

FIG. 10

illustrates a cross-sectional view of partition


130


A including baffle plates


132


A,


134


A, and


136


A. The partition


130


A is located between stations


8


and


9


.

FIG. 11

illustrates a cross-sectional view of partition


130


B including baffle plates


132


B,


134


B, and


136


B. The partition


130


B is located between stations


22


and


23


.

FIG. 12

illustrates a cross-sectional view of partition


130


C including baffles


132


C,


134


C, and


136


C. The partition


130


C is located between stations


35


and


36


. As illustrated in

FIG. 3

, sterile air is introduced through sterile air conduits


140


,


142


, and


144


into the sterile tunnel


90


. The sterile air conduit


140


is located at station


23


(FIG.


11


), the sterile air conduit


142


is located at station


27


(FIG.


3


), and the sterile air conduit


144


is located at station


35


(FIG.


12


).




The partition


130


A separates an activation and drying apparatus


152


from the interior bottle sterilization apparatus


116


. The partition


130


B separates the activation and drying apparatus


152


from a main product filler apparatus


160


and a lid sterilization and heat sealing apparatus


162


. Thus, a first sterilization zone


164


is created that includes the activation and drying apparatus


152


. Partition


130


C separates the main product filler apparatus


160


and the lid sterilization and heat sealing apparatus


162


from a bottle discharge apparatus


280


. Thus, partitions


130


B and


130


C create a second sterilization zone


166


that includes the main product filler apparatus


160


and the lid sterilization and heat sealing apparatus


162


. A third sterilization zone


172


includes the bottle discharge apparatus


280


. A fourth sterilization zone


165


includes the interior bottle sterilization apparatus


116


. The second sterilization zone


166


provides a highly sterile area where the bottles


12


are filled with a product and sealed. The second sterilization zone


166


is at a higher pressure than the first sterilization zone


164


and the third sterilization zone


172


. Therefore, any gas flow leakage is in the direction from the second sterilization zone


166


out to the first sterilization zone


164


and the third sterilization zone


172


. The first sterilization zone


164


is at a higher pressure than the fourth sterilization zone


165


. Therefore, gas flow is in the direction from the first sterilization zone


164


to the fourth sterilization zone


165


.




The partitions


130


A,


130


B, and


130


C create sterilization zones


164


,


165


,


166


, and


172


with different concentration levels of gas laden sterilant (e.g., hydrogen peroxide in air). The highest concentration level of sterilant is in the fourth sterilization zone


165


. An intermediate concentration level of sterilant is in the first sterilization zone


164


. The lowest concentration level of sterilant is in the second sterilization zone


166


. Advantageously, this helps to maintain the main product filler apparatus


160


and the lid sterilization and heat sealing apparatus


162


at a low sterilant concentration level. This prevents unwanted high levels of sterilant to enter the food product during the filling and lidding process.




Stations


10


through


21


include twelve stations for directing hot sterile air into each bottle


12


for the activation and removal of the sterilant from the interior of the bottle


12


. The sterile air supply system


146


supplies hot sterile air to a plurality of nozzles


150


in the activation and drying apparatus


152


. Hot sterile air is supplied to the sterile air supply system


146


through conduit


148


. The air is first passed through a filtration system to sterilize the air. The air is then heated in a heating system to about


230


° F. The air temperature is regulated by the control system


550


. Also, the control system


550


monitors the air pressure and flow rate to ensure that an adequate flow of hot sterile air is maintained in the sterile tunnel


90


of the application and drying apparatus


152


.




As shown in

FIG. 8

, each bottle


12


generally has a small opening


16


compared to its height “H.” A ratio of a diameter “D” of the bottle


12


to the height “H” of the bottle


12


is generally less than 1.0. The small bottle opening


16


combined with a larger height “H” restricts the flow of hot gas into the interior


118


of the bottle


12


. Also, PET and HDPE bottle materials have low heat resistance temperatures. These temperatures commonly are about 55° C. for PET and about 121° C. for HDPE. Typically, in the aseptic packaging industry, a low volume of air at a high temperature is applied to the packaging materials. This often results in deformation and softening of packaging materials formed of PET and HDPE. In order to prevent softening and deformation of the bottles


12


, when formed from these types of materials, the present invention applies high volumes of air at relatively low temperatures over an extended period of time in the activation and drying apparatus


152


. The plurality of nozzles


150


of the activation and drying apparatus


152


direct hot sterile air into the interior


118


of each bottle


12


(FIG.


11


). A long exposure time is predicated by the geometry of the bottle


12


and the softening temperature of the material used to form the bottle


12


. In the present invention, about 24 seconds are allowed for directing hot sterile air from the plurality of nozzles


150


into each bottle for the activation and removal of sterilant from the interior surface


119


of the bottle


12


. To achieve aseptic sterilization, a minimum bottle temperature of about 131° F. should be held for at least 5 seconds. To achieve this bottle temperature and time requirements, including the time required to heat the bottle, the sterilant is applied for about 1 second and the hot sterile air is introduced for about 24 seconds. The hot sterile air leaves the nozzles


150


at about 230° F. and cools to about 131° F. when it enters the bottle


12


. The hot sterile air is delivered at a high volume so that the bottle


12


is maintained at about 131° F. for at least 5 seconds. The about 24 seconds provides adequate time for the bottle


12


to heat up to about 131° F. and to maintain this temperature for at least 5 seconds. After bottle


12


has dried, the residual hydrogen peroxide remaining on the bottle


12


surface is less than 0.5 PPM.




A foodstuff product is first sterilized to eliminate bacteria in the product. An “Ultra High Temperature” (UHT) pasteurization process is required to meet the aseptic FDA standard. The time and temperature required to meet the aseptic FDA standard depends on the type of foodstuff. For example, milk must be heated to 282° F. for not less than 2 seconds in order to meet the aseptic standards.




After UHT pasteurization, the product is delivered to a main product filler apparatus


160


. The main product filler apparatus is illustrated in

FIGS. 3 and 13

. The main product filler


160


can be sterilized and cleaned in place to maintain aseptic FDA and


3


A standards. A pressurized reservoir apparatus


180


that can be steam sterilized is included in the main product filler apparatus


160


. As illustrated in

FIG. 13

, the pressurized reservoir apparatus


180


includes an enclosed product tank


182


with a large capacity (e.g., 15 gallons). The product tank


182


is able to withstand elevated pressures of about 60 psig or more. The pressurized reservoir apparatus


180


also includes a level sensor


184


, a pressure sensor


186


, a volumetric measuring device


188


, and a filling nozzle


190


. The product tank


182


includes a single inlet with a valve cluster including a sterile barrier to separate the product process system from aseptic surge tanks and the main product filler apparatus


160


. The product tank


182


has an outlet with twelve connections. At each connections is a volumetric measuring device


188


such as a mass or volumetric flow meter. A plurality of filling nozzles


190


A,


190


B are provided at stations


23


,


25


, respectively. In addition, there are a plurality of volumetric measuring devices


188


A and


188


B to measure the volume of product entering each bottle


12


at stations


23


and


25


, respectively. The control system


550


calculates the desired volume of product to be inserted into each bottle


12


, and controls the product volume by opening or closing a plurality of valves


194


A and


194


B. The activation mechanisms for valves


194


A and


194


B have a sterile barrier to prevent contamination of the product. The plurality of valves


194


A control the volume of product flowing through a corresponding plurality of nozzles


196


A into the bottles


12


at station


23


. The plurality of valves


194


B control the volume of product flowing through a corresponding plurality of nozzles


196


B into the bottles


12


at station


25


. The control system


550


uses the previously stored information provided by the bottle detection apparatus


112


to only allow filling to occur at the locations where bottles


12


are actually present and correctly aligned.




The initial sterilization process for the pressurized reservoir apparatus


180


includes the step of exposing all of the surfaces of the pressurized reservoir apparatus


180


that come in contact with the product to steam at temperatures above about 250° F. for a minimum of about 30 minutes. Elements such as cups


198


A and


198


B are used to block off nozzle outlets


196


A and


196


B respectively, to allow a build-up of steam pressure to about 50 psig inside the pressurized reservoir apparatus


180


. Condensate generated as the steam heats the interior surfaces of the pressurized reservoir apparatus


180


is collected and released from the nozzles


198


A and


198


B. This condensate is released when the cups


198


A and


198


B are removed from the nozzle outlets


196


A and


196


B. Once the interior surfaces of the pressurized reservoir apparatus


180


are sterilized, the steam is shut off, and sterile air is used to replace the steam. The sterile air reduces the interior temperature of the pressurized reservoir apparatus


180


to the temperature of the product before the product is allowed to enter the enclosed product tank


182


. Sterile air is directed through sterile air conduits


142


and


144


into the second sterilization zone


166


at a volume rate of about 800 scfm (FIG.


13


). The sterile air flow entering the second sterilization zone


166


provides sterile air to the main product filler apparatus


160


and to the lid sterilization and heat sealing apparatus


162


.




The main product filler apparatus


160


includes a separate filling position for each bottle. The bottle


12


filling operation is completed for six bottles at station


23


and for six bottles at station


25


.





FIGS. 3 and 13

illustrate the lid sterilization and heat sealing apparatus


162


. A lid


200


is applied to each of the twelve bottles


12


at station


31


. For a fully aseptic bottle filler, complete lid


200


sterilization is necessary, and therefore a sterilant such as hydrogen peroxide is typically used. In the present invention, the lids are formed of a material such as foil or plastic. The lids


200


are joined together by a small interconnecting band that holds them together to form a long connected chain of lids


200


, hereinafter referred to as a “daisy chain”


202


. A daisy chain


202


of lids


200


is placed on each of a plurality of reels


210


. For the twelve bottle configuration of the present invention, six of the reels


210


, each holding a daisy chain


202


of lids


200


, are located on each side of a heat sealing apparatus


214


. Each daisy chain


202


of lids


200


winds off of a corresponding reel


210


and is sterilized, preferably using a hydrogen peroxide bath


204


. A plurality of hot sterile air knives


208


, which are formed by jets of hot sterile air, activate the hydrogen peroxide to sterilize the lids


200


on the daisy chain


202


. The hot sterile air knives


208


also remove the hydrogen peroxide from the lids


200


so that the residual concentration of hydrogen peroxide is less than 0.5 PPM. The hydrogen peroxide bath


204


prevents any contaminants from entering the sterile tunnel


90


via the lidding operation. Once sterilized, the lids


200


enter the sterile tunnel


90


where they are separated from the daisy chain


202


and placed on a bottle


12


. Each lid is slightly larger in diameter then that of the opening


16


of a bottle


12


. During the placement of the lid


200


on the bottle


12


, a slight mechanical crimp of the lid


200


is formed to locate and hold the lid


200


on the bottle


12


. The crimp holds the lid


200


in place on the bottle


12


until the bottle


12


reaches a station


33


for sealing.




At station


33


, the lids


200


are applied to the bottles


12


. The heat sealing apparatus


214


includes a heated platen


216


that applies heat and pressure against each lid


200


for a predetermined length of time, to form a seal between the lid


200


and the bottle


12


. The heated platen


216


is in a two by six configuration to seal twelve of the bottles


12


at a time.




At station


37


, the lid


200


seal and bottle


12


integrity are checked in a known manner by a seal integrity apparatus (not shown) comprising, for example, a bottle squeezing mechanism and a proximity sensor. Each bottle


12


is squeezed by the bottle squeezing mechanism which causes the lid


200


on the bottle


12


to extend upward. The proximity sensor detects if the lid


200


has extended upward, which indicates an acceptable seal, or whether the seal remains flat, which indicates a leaking seal or bottle


12


. The location of the defective bottles


12


are recorded by the control system


550


so that the defective bottles will not be packed.




Bottle discharge from the sterile tunnel


90


of the filler apparatus


50


occurs at stations


38


and


40


as illustrated in

FIGS. 3

,


13


and


14


. A bottle discharge apparatus


280


is located at stations


38


and


40


. At this point in the filler apparatus


50


, the filled and sealed bottles


12


are forced in an upward direction such that a top portion


284


of each bottle


12


protrudes through an opening


282


in the sterile tunnel


90


(FIG.


14


). A rotating cam


290


or other suitable means (e.g., an inflatable diaphragm, etc.) may be used to apply a force against the bottom


120


of each bottle


12


to force the bottle


12


in an upward direction.




As illustrated in

FIG. 14

, the bottle discharge apparatus


280


comprises a lifting apparatus


286


that includes a gripper


288


that grasps the top portion


284


of each bottle


12


and lifts the bottle


12


out through the opening


282


in the sterile tunnel


90


. In order to ensure that contaminated air cannot enter the sterile tunnel


90


, the sterile air in the sterile tunnel


90


is maintained at a higher pressure than the air outside the sterile tunnel


90


. Thus, sterile air is always flowing out of the sterile tunnel


90


through the opening


282


. In addition, the gripper


288


never enters the sterile tunnel


90


, because the top portion


284


of the bottle


12


is first lifted out of the sterile tunnel


90


by the action of the rotating cam


290


before being grabbed by the gripper


288


.





FIG. 15

illustrates a top view of the filler apparatus


50


including the bottle infeed and sterilization apparatus


60


, the interior bottle sterilization apparatus


116


, and the activation and drying apparatus


152


.

FIG. 15

additionally illustrates the main filler apparatus


160


, the lid sterilization and heat sealing apparatus


162


, and the bottle discharge apparatus


280


.




Referring again to

FIGS. 1 and 14

, the lifting apparatus


286


lifts the bottles


12


at station


38


and places the bottles


12


in a first lane


292


that transports the bottles


12


to a first capping apparatus


410


. In addition, the lifting apparatus


286


lifts the bottles


12


at station


40


and places the bottles


12


in a second lane


294


that transports the bottles


12


to a second capping apparatus


400


.




The first capping apparatus


410


secures a cap (not shown) on the top of each bottle


12


in the first lane


292


. The second capping apparatus


400


secures a cap on the top of each bottle


12


in the second lane


294


. The caps are secured to the bottles


12


in a manner known in the art. It should be noted that the capping process may be performed outside of the sterile tunnel


90


because each of the bottles


12


have previously been sealed within the sterile tunnel


90


by the lid sterilization and heat sealing apparatus


162


using a sterile lid


200


.




After capping, the bottles


12


are transported via the first and second lanes


292


,


294


to labelers


460


and


470


. The first labeling apparatus


470


applies a label to each bottle


12


in the first lane


292


. The second labeling apparatus


460


applies a label to each bottle


12


in the second lane


294


.




From the first labeling apparatus


470


, the bottles


12


are transported along a first set of multiple lanes (e.g.,


4


) to a first case packing apparatus


490


. From the second labeling apparatus


460


, the bottles


12


are transported along a second set of multiple lanes to a second case packing apparatus


480


. Each case packing apparatus


480


,


490


gathers and packs a plurality of the bottles


12


(e.g., twelve) in each case in a suitable (e.g., three by four) matrix.




A first conveyor


296


transports the cases output by the first case packer


490


to a first palletizer


510


. A second conveyor


298


transports the cases output by the second case packer


480


to a second palletizer


500


. A vehicle, such as a fork lift truck, then transports the pallets loaded with the cases of bottles


12


to a storage warehouse.




Referring again to

FIG. 3

, the main conveyor


106


and each conveying plate


94


are cleaned and sanitized once during each revolution of the main conveyor


106


. Specifically, after each empty conveying plate


94


passes around the pulley


108


, the conveying plate


94


is passed through a liquid sanitizing apparatus


300


and a drying apparatus


302


. The liquid sanitizing apparatus


300


sprays a mixture of a sterilizing agent (e.g., oxonia, (hydrogen peroxide and peroxyacetic acid)) over the entire surface of each conveying plate


94


and associated components of the main conveyor


106


. In the drying apparatus


302


, heated air is used to dry the main conveyor


106


and conveying plates


94


.




Stations


1


through


40


are enclosed in the sterile tunnel


90


. The sterile tunnel


90


is supplied with air that is pressurized and sterilized. The interior of the sterile tunnel


90


is maintained at a pressure higher than the outside environment in order to eliminate contamination during the bottle processing. In addition, to further ensure a sterile environment within the sterile tunnel


90


, the sterile air supply provides a predetermined number of air changes (e.g., 2.5 changes of air per minute) in the sterile tunnel


90


.




The bottle infeed and sterilization apparatus


60


and the filler apparatus


50


meet the 3A Sanitary Standards of the Sanitary Standards Symbol Administrative Council. The 3A Sanitary Standards ensure that all product contact surfaces can be cleaned and sterilized on a regular basis such as daily. The present invention allows the product contact surfaces to be cleaned-in-place without dismantling the bottle infeed and sterilization apparatus


60


or the filler apparatus


50


. The 3A Sanitary Standards includes requirements such as the material type, the material surface finish, the elastomer selection, the radius of machined parts and the ability of all surfaces to be free draining. For example, the material type is selected from the 300 series of stainless steel and all product contact surfaces have a finish at least as smooth as No.


4


ground finish on stainless steel sheets.




Before bottle production is initiated, the bottle infeed and sterilization apparatus


60


and the filler apparatus


50


are preferably sterilized with an aseptic sterilant. For example, a sterilant such as a hot hydrogen peroxide mist may be applied to all interior surfaces of the bottle infeed and sterilization apparatus


60


and the filler apparatus


50


. Then, hot sterile air is supplied to activate and remove the hydrogen peroxide, and to dry the interior surfaces of the bottle infeed and sterilization apparatus


60


and the filler apparatus


50


.





FIG. 16

is a side view of the aseptic processing apparatus


10


of the present invention indicating the location of the control and monitoring devices that are interfaced with the control system


550


. The control system


550


gathers information and controls process functions in the aseptic processing apparatus


10


. A preferred arrangement of the control and monitoring devices are indicated by encircled letters in

FIG. 16. A

functional description of each of the control and monitoring devices is listed below. It should be noted that these control and monitoring devices are only representative of the types of devices that may be used in the aseptic processing apparatus


10


of the present invention. Other types and combinations of control and monitoring devices may be used without departing from the intended scope of the present invention. Further, control system


550


may respond in different ways to the outputs of the control and monitoring devices. For example, the control system


550


may automatically adjust the operational parameters of the various components of the aseptic processing apparatus


10


, may generate and/or log error messages, or may even shut down the entire aseptic processing apparatus


10


. In the preferred embodiment of the present invention, the control and monitoring devices include:




A. A bottle counter to ensure that a predetermined number of the bottles


12


(e.g., six bottles) on each upper horizontal row


24


,


28


enter the loading area of the bottle infeed and sterilization apparatus


60


.




B. A proximity sensor to ensure that the first group of bottles


12


has dropped into the first bottle position in the bottle infeed and sterilization apparatus


60


.




C


1


. A conductivity sensor to ensure that the measuring cup used by the sterilant application apparatus


36


is full.




C


2


. A conductivity sensor to ensure that the measuring cup used by the sterilant application apparatus


36


is emptied in a predetermined time.




C


3


. A pressure sensor to ensure that the pressure of the air used by the sterilant application apparatus


36


is within predetermined atomization requirements.




C


4


. A temperature sensor to ensure that each heat heating element used by the sterilant application apparatus


36


is heated to the correct temperature.




D. A proximity sensor (e.g., proximity sensor


71


,

FIG. 3

) to ensure that a bottle jam has not occurred within the bottle infeed and sterilization apparatus


60


.




E. A temperature sensor to ensure that the temperature of the heated sterile air entering the bottle infeed and sterilization apparatus


60


is correct.




F. A proximity sensor that to ensure that each conveying plate


94


is fully loaded with bottles


12


.




G


1


. A conductivity sensor to ensure that the measuring cup used by the interior bottle sterilization apparatus


116


is full.




G


2


. A conductivity sensor to ensure that the measuring cup used by the interior bottle sterilization apparatus


116


is emptied in a predetermined time.




G


3


. A pressure sensor to ensure that the pressure of the air used by the interior bottle sterilization apparatus


116


is within predetermined atomization requirements.




G


4


. A temperature sensor to ensure that each heat heating element used by the interior bottle sterilization apparatus.


116


is heated to the correct temperature.




H. A temperature sensor to ensure that the air drying temperature within the activation and drying apparatus


152


is correct.




I. A plurality of flow sensors to ensure that the airflow rate of the sterile air entering the sterile tunnel


90


is correct.




J. A pressure sensor to ensure that the pressure of the sterile air entering the activation and drying apparatus


152


is correct.




K. A measuring device (e.g., volumetric measuring device


188


,

FIG. 3

) to ensure that each bottle


12


is filled to a predetermined level.




L. A pressure sensor to ensure that the pressure in the product tank


182


is above a predetermined level.




M. A level sensor to ensure that the level of product in the product tank


182


is maintained at a predetermined level.




N. Proximity sensors to ensure that the daisy chains


202


of lids


200


are present in the lid sterilization and heat sealing apparatus


162


.




O. A level sensor to ensure that the hydrogen peroxide level in the hydrogen peroxide bath


204


in the lid sterilization and heat sealing apparatus


162


is above a predetermined level.




P. A temperature sensor to ensure that the temperature of the hot sterile air knives


208


of the lid sterilization and heat sealing apparatus


162


is correct.




Q. A temperature sensor to ensure that the heat sealing apparatus


214


is operating at the correct temperature.




R. Proximity sensors to ensure that the bottles


12


are discharged from the filler.




S. A speed sensor to measure the speed of the conveying apparatus


100


.




T. A concentration sensor to ensure that the concentration of oxonia is maintained at a predetermined level in the sanitizing apparatus


300


.




U. A pressure sensor to ensure that the pressure of the oxonia is maintained above a predetermined level in the sanitizing apparatus


300


.




V. A temperature sensor to ensure that the drying temperature of the drying apparatus


302


is correct.




The foregoing description of the present invention has been presented for purposes of illustration and description. It is not intended to be exhaustive or to limit the invention to the precise form disclosed, and many modifications and variations are possible in light of the above teaching. Such modifications and variations that may be apparent to a person skilled in the art are intended to be included within the scope of this invention defined by the accompanying claims.



Claims
  • 1. A method for aseptically bottling aseptically sterilized foodstuffs comprising the steps of:providing a plurality of bottles; aseptically disinfecting the plurality of bottles to a level producing at least about a 6 log reduction in spore organisms; filling the aseptically disinfected plurality of bottles with the aseptically sterilized foodstuffs; and filling the aseptically disinfected plurality of bottles at a rate greater than 100 bottles per minute.
  • 2. The method according to claim 1, wherein the plurality of bottles are made from a glass.
  • 3. The method according to claim 1, wherein the plurality of bottles are made from a plastic.
  • 4. The method according to claim 3, wherein the plastic is polyethylene terepthalate.
  • 5. The method according to claim 3, wherein the plastic is high density polyethylene.
  • 6. The method according to claim 1, further including capping the bottle with an aseptically disinfected lid.
  • 7. The method according to claim 1, wherein the plurality of bottles has an opening size to height ratio of less than one.
  • 8. The method according to claim 1, further including disinfecting the interior of the plurality of bottles with a hot hydrogen peroxide spray.
  • 9. The method according to claim 8, wherein disinfecting the interior of the plurality of bottles includes the application of the hot hydrogen peroxide spray for about 1 second and the activation and removal of the hot hydrogen peroxide using hot aseptically sterilized air for about 24 seconds.
  • 10. The method according to claim 1, further including a feedback control system for maintaining aseptic bottling conditions.
  • 11. The method according to claim 1, wherein disinfecting is provided by hydrogen peroxide.
  • 12. The method according to claim 1, wherein disinfecting is provided by oxonia.
  • 13. The method according to claim 1, wherein disinfecting the outside surfaces of the plurality of bottles is provided by oxonia.
  • 14. The method according to claim 1, wherein the step of filling the aseptically disinfected bottling further comprises: filling the aseptically disinfected bottling at a rate greater than 360 bottles per minute.
  • 15. The method for aseptically bottling aseptically sterilized foodstuffs comprising the steps of:providing a plurality of bottles; aseptically disinfecting the plurality of bottles; filling the aseptically disinfected plurality of bottles with the aseptically sterilized foodstuffs; and filling the aseptically disinfected plurality of bottles at a rate greater than 100 bottles per minute wherein disinfecting the outside surfaces of the plurality of bottles is provided by hydrogen peroxide.
  • 16. The method according to claim 15, wherein disinfecting the outside surface of the plurality of bottles includes about 1 second for the application of the hot hydrogen peroxide spray and about 24 seconds for the activation and removal of the hot hydrogen peroxide using hot aseptically sterilized air.
  • 17. The method for asepctically bottling aseptically sterilized foodstuffs comprising the steps of:providing a plurality of bottles; filling the aseptically disinfected plurality of bottles with the aseptically sterilized foodstuffs wherein the aseptically sterilized foodstuffs are sterilized to a level producing at least about 12 log reduction in Clostridium botulinum; and filling the aseptically disinfected plurality of bottles at a rate greater than 100 bottles per minute.
  • 18. The method for aseptically bottling aseptically sterilized foodstuffs comprising the steps of:providing a plurality of bottles; filling the aseptically disinfected plurality of bottles with the aseptically sterilized foodstuffs; and filling the aseptically disinfected plurality of bottles at a rate greater than 100 bottles per minute, further including disinfecting the interior of the plurality of bottles with a hot hydrogen peroxide spray wherein the residual level of hydrogen peroxide is less than about 0.5 ppm.
  • 19. A device for aseptically bottling aseptically sterilized foodstuffs having at least about a 12 log reduction in Clostridium botulinum comprising:means for providing a plurality of bottles; means for aseptically disinfecting the plurality of bottles; means for aseptically filling the aseptically disinfected plurality of bottles with the aseptically sterilized foodstuffs; and means for filling the aseptically disinfected plurality of bottles at a rate greater than 100 bottles per minute.
  • 20. A method for aseptically bottling aseptically sterilized foodstuffs comprising the steps of:providing a plurality of bottles; aseptically disinfecting the plurality of bottles to a level producing at least about a 6 log reduction in spore organisms; filling the aseptically disinfected plurality of bottles with the aseptically sterilized foodstuffs wherein the aseptically sterilized foodstuffs are sterilized to a level producing at least about a 12 log reduction in Clostridium botulinum; and filling the aseptically disinfected plurality of bottles at a rate greater than 100 bottles per minute, further including disinfecting the interior of the plurality of bottles with a hot hydrogen peroxide spray wherein the residual level of hydrogen peroxide is less than about 0.5 ppm.
Parent Case Info

This application claims the benefit of Provisional Application No. 60/118,404, filed Feb. 2, 1999.

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Provisional Applications (1)
Number Date Country
60/118404 Feb 1999 US